US20090092654A1 - Drug Delivery Methods, Structures, and Compositions for Nasolacrimal System - Google Patents
Drug Delivery Methods, Structures, and Compositions for Nasolacrimal System Download PDFInfo
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- US20090092654A1 US20090092654A1 US12/332,219 US33221908A US2009092654A1 US 20090092654 A1 US20090092654 A1 US 20090092654A1 US 33221908 A US33221908 A US 33221908A US 2009092654 A1 US2009092654 A1 US 2009092654A1
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61F—FILTERS IMPLANTABLE INTO BLOOD VESSELS; PROSTHESES; DEVICES PROVIDING PATENCY TO, OR PREVENTING COLLAPSING OF, TUBULAR STRUCTURES OF THE BODY, e.g. STENTS; ORTHOPAEDIC, NURSING OR CONTRACEPTIVE DEVICES; FOMENTATION; TREATMENT OR PROTECTION OF EYES OR EARS; BANDAGES, DRESSINGS OR ABSORBENT PADS; FIRST-AID KITS
- A61F2/00—Filters implantable into blood vessels; Prostheses, i.e. artificial substitutes or replacements for parts of the body; Appliances for connecting them with the body; Devices providing patency to, or preventing collapsing of, tubular structures of the body, e.g. stents
- A61F2/02—Prostheses implantable into the body
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- A61F9/00—Methods or devices for treatment of the eyes; Devices for putting-in contact lenses; Devices to correct squinting; Apparatus to guide the blind; Protective devices for the eyes, carried on the body or in the hand
- A61F9/0008—Introducing ophthalmic products into the ocular cavity or retaining products therein
- A61F9/0017—Introducing ophthalmic products into the ocular cavity or retaining products therein implantable in, or in contact with, the eye, e.g. ocular inserts
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- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
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Definitions
- the present application is related to implants for use in or near the nasolacrimal drainage system, with embodiments providing canalicular implants, lacrimal sac implants, punctal plugs and punctal plugs with drug delivery capabilities.
- Patient compliance in taking the medications can be erratic, and in some cases, patients may not follow the directed treatment regime. Lack of compliance can include, failure to instill the drops, ineffective technique (instilling less than required), excessive use of the drops (leading to systemic side effects), and use of non-prescribed drops or failure to follow the treatment regime requiring multiple types of drops. Many of the medications may require the patient to instill them up to 4 times a day.
- topically applied medications have a peak ocular effect within about two hours, after which additional applications of the medications should be performed to maintain the therapeutic benefit.
- inconsistency in self-administered or ingested medication regimes can result in a suboptimal therapy.
- PCT Publication WO 06/014434 (Lazar), which is incorporated herein by reference in its entirety, may be relevant to these and/or other issues associated with eye drops.
- One promising approach to ocular drug delivery is to place an implant that releases a drug in tissue near the eye.
- this approach can offer some improvement over eye drops, some potential problems of this approach may include implantation of the implant at the desire tissue location, retention of the implant at the desired tissue location, and sustaining release of the drug at the desired therapeutic level for an extended period of time.
- implantation of the implant at the desire tissue location may include implantation of the implant at the desire tissue location, retention of the implant at the desired tissue location, and sustaining release of the drug at the desired therapeutic level for an extended period of time.
- undetected and premature loss of an implant can result in no drug being delivered, and the patient can potentially suffer a reduction in vision, possibly even blindness.
- the present invention provides implant devices, systems and methods for delivery of a therapeutic agent from a punctuin of a patient ocular tissues.
- embodiments of the present invention provide an implant for insertion into a punctum of a patient.
- the punctum provides a flow path for a tear fluid from an eye to a canalicular lumen.
- the implant comprises a body.
- the body has a distal end, a proximal end, and an axis therebetween.
- the distal end of the body is insertable distally through the punctum into the canalicular lumen.
- the body comprises a therapeutic agent included within an agent matrix drug core. Exposure of the agent matrix to the tear fluid effects an effective therapeutic agent release into the tear fluid over a sustained period.
- the body has a sheath disposed over the agent matrix to inhibit release of the agent away from the proximal end.
- the body also has an outer surface configured to engage luminal wall tissues so as to inhibit expulsion when disposed therein.
- the agent matrix comprises a non-bioabsorbable polymer, for example silicone in a non-homogenous mixture with the agent.
- the non-homogeneous mixture may comprise a silicone matrix saturated with the therapeutic agent and inclusions of the therapeutic agent.
- the outer surface of the body can be disposed on the sheath, and the outer surface may define a body shape that inhibits expulsion of the body from the punctum.
- the body may further comprise a support structure over the agent matrix.
- the support structure may define the outer surface and be configured to inhibit expulsion of the body from the punctum.
- the support structure receives the sheath and agent matrix drug core therein, and inhibits inadvertent expulsion of the agent matrix in use.
- the support structure can comprise a helical coil.
- the support structure may have a receptacle therein, and the receptacle may fittingly receive the sheath and agent matrix therein so as to allow unrestricted fluid communication between the proximal end and the tear film in use.
- the outer surface may expand radially when released within the punctum, and the radial expansion may inhibits the expulsion from the punctum.
- the agent comprises a prostaglandin analogue
- the extended period comprises at least 3 months.
- an implant for insertion into a patient comprising a body.
- the body can comprise a therapeutic agent and a support structure.
- the body can be configured to, when implanted at a target location along the tear fluid path, release a quantity of the therapeutic agent into the tear fluid each day for a sustained release period of days.
- the quantity can be significantly less than a recommended daily drop-administered quantity of the therapeutic agent.
- the quantity can be less than 10% of the recommended drop-administered quantity.
- the quantity can be less than 5% of the recommended drop-administered quantity.
- the period comprises at least three weeks and may comprise at least three months.
- the therapeutic agent may comprise Timolol maleate.
- the body may comprise in a range from about 270 ⁇ g to about 1350 ⁇ g of the therapeutic agent.
- the quantity released each day can be in a range from about 20 ⁇ g to about 135 ⁇ g.
- the therapeutic agent may comprise a prostaglandin analogue, for example Latanoprost and/or Bimatoprost, and the body can comprise therapeutic agent in a range from about 3 ⁇ g to about 135 ⁇ g.
- the quantity can be in a range from about 5 ng to about 500 ng.
- the body may comprise therapeutic agent in a range from about 5 ⁇ g to about 30 ⁇ g, and the quantity can be in a range from about 10 ng to 150 ng.
- embodiments of the present invention provide a method of delivering a therapeutic agent to an eye having associated tear fluid.
- the method comprises placing a drug core in a canaliculus of the eye.
- the drug core comprises a matrix and inclusions of the therapeutic agent within the matrix.
- a portion of the drug core is exposed to the tear.
- the therapeutic agent is released to the tear of the eye.
- the therapeutic agent dissolves into the matrix such that the matrix remains substantially saturated with the therapeutic agent while the therapeutic agent is released through the exposed portion at therapeutic levels over a sustained period.
- a rate of release is substantially determined by solubility of the agent in the core, the solubility of the agent in the tear and an area of the exposed portion.
- the drug can be released through the exposed portion at therapeutic levels for about 90 days.
- the therapeutic agent may comprise a prostaglandin analogue, and the inclusions of the therapeutic agent comprise an oil.
- the therapeutic agent can be encapsulated within the matrix, and the matrix may comprise a non-bioabsorbable polymer.
- the therapeutic agent has a solubility in water of less than about 0.03% percent by weight.
- the therapeutic agent can be released at therapeutic levels in response to a surfactant of the tear.
- a sheath may be disposed over the core to define the exposed portion, and the exposed portion oriented toward the eye on a proximal end of the core.
- a punctal plug to treat glaucoma comprises a body no more than about 2.0 mm across. When inserted in the punctum for 35 days the body delivers at least a therapeutic quantity of therapeutic agent each day of the 35 days.
- the body no more than about 2.0 mm across comprises a cross sectional size no more than about 1.0 mm across while inserted into the patient.
- the body comprises a drug core and the therapeutic agent is delivered from the drug core.
- the drug core may be no more than about 1 mm across, and the body may be no more than about 2 mm in length.
- a method of treating glaucoma comprises eluting at least 10 ng per day of a therapeutic agent from the punctal plug for at least 90 days.
- the therapeutic agent comprises at least one of Bimatoprost or Latanoprost.
- the therapeutic agent may have a solubility in water no more than about 0.03% by weight.
- a punctal plug to treat glaucoma comprises a body.
- the body comprises a therapeutic agent, and the body is adapted to release the therapeutic agent at therapeutic levels in response to a surfactant of the eye.
- the therapeutic agent has a solubility in water no more than about 0.03% by weight.
- the therapeutic agent may comprise cyclosporin.
- a punctal plug to treat glaucoma comprises a plug body.
- the body comprises a therapeutic agent.
- the body is adapted to release from about 80 to 120 ng of the therapeutic agent into a tear of the eye for at least about 20 days.
- the therapeutic agent may comprise at least one of Bimatoprost or Latanoprost.
- a punctal plug to treat glaucoma comprises a body.
- the body comprises therapeutic agent stored within a volume no more than about 0.02 cm 3 .
- the body is adapted to deliver therapeutic levels of the therapeutic agent for at least about 1 month.
- the body is adapted to deliver the therapeutic agent at therapeutic levels for at least about 3 months.
- the body can be adapted to deliver the therapeutic agent with a substantially zero order release rate for the at least one month.
- composition of matter to treat glaucoma of an eye having an associated tear comprises inclusions.
- the inclusions comprise a concentrated form of a therapeutic agent.
- the therapeutic agent comprises a solubility in water no more than about 0.03% by weight.
- a silicone matrix encapsulates the inclusions.
- the therapeutic agent is soluble in the silicone matrix to release the therapeutic agent from the silicon matrix into the tear at therapeutic levels.
- the therapeutic agent inclusions are encapsulated within the silicon matrix comprise an inhomogeneous mixture of the inclusions encapsulated within the silicon matrix.
- the inclusions can comprise Latanoprost oil.
- FIGS. 1-1 and 1 - 2 show anatomical tissue structures of the eye suitable for use with implants, according to embodiments of the present invention
- FIG. 1A shows a top cross sectional view of a sustained release implant to treat an optical defect of an eye, according to an embodiment of the present invention
- FIG. 1B shows a side cross sectional view of the sustained release implant of FIG. 1A ;
- FIG. 1C shows a perspective view of a sustained release implant with a coil retention structure, according to an embodiment of the present invention
- FIG. 1D shows a perspective view of a sustained release implant with a retention structure comprising struts, according to an embodiment of the present invention
- FIG. 1E shows a perspective view of a sustained release implant with a cage retention structure, according to an embodiment of the present invention
- FIG. 1F shows a perspective view of a sustained release implant comprising a core and sheath, according to an embodiment of the present invention
- FIG. 1G schematically illustrates a sustained release implant comprising a flow restricting retention element, a core and a sheath, according to an embodiment of the present invention
- FIG. 2A shows a cross sectional view of a sustained release implant with core comprising an enlarged exposed surface area, according to an embodiment of the present invention
- FIG. 2B shows a cross sectional view of a sustained release implant with a core comprising an enlarged exposed surface area, according to an embodiment of the present invention
- FIGS. 2C and 2D show perspective view and cross sectional views, respectively, of a sustained release implant with a core comprising a reduced exposed surface area, according to an embodiment of the present invention:
- FIG. 2E shows a cross sectional view of a sustained release implant with a core comprising an enlarged exposed surface area with an indentation and castellation, according to an embodiment of the present invention
- FIG. 2F shows a perspective view of a sustained release implant comprising a core with folds, according to an embodiment of the present invention
- FIG. 2G shows a perspective view of a sustained release implant with a core comprising a channel with an internal porous surface, according to an embodiment of the present invention
- FIG. 2H shows a perspective view of a sustained release implant with a core comprising porous channels to increase drug migration, according to an embodiment of the invention
- FIG. 2I shows a perspective view of a sustained release implant with a convex exposed drug core surface, according to an embodiment of the present invention
- FIG. 2J shows a side view of a sustained release implant with a core comprising an exposed surface area with several soft brush-like members extending therefrom, according to an embodiment of the present invention
- FIG. 2K shows a side view of a sustained release implant with a drug core comprising a convex exposed surface and a retention structure, according to an embodiment of the present invention
- FIG. 2L shows a side view of a sustained release implant with a drug core comprising a concave indented surface to increase exposed surface area of the core, according to an embodiment of the present invention
- FIG. 2M shows a side view of a sustained release implant with a drug core comprising a concave surface with a channel formed therein to increase an exposed surface area of the core, according to an embodiment of the present invention
- FIG. 3A shows an implant with a sheath body with extensions that attach the sheath body and core to the retention element, according to an embodiment of the present invention
- FIG. 3B shows an implant with a retention element with an extension that retains a sheath body and a core, according to an embodiment of the present invention
- FIGS. 4A and 4B show a cross-sectional view of an implant with a retention structure that is shorter in length while in a large cross-sectional profile configuration than a small cross-sectional profile configuration, according to an embodiment of the present invention
- FIGS. 5A to 5C schematically illustrate replacement of a drug core and a sheath body, according to an embodiment of the present invention
- FIGS. 6A to 6C show deployment of a sustained release implant, according to an embodiment of the present invention.
- FIGS. 7A and 7B show elution data of Latanoprost at day 1 and day 14, respectively, for the three core diameters of 0.006, 0.012 and 0.025 inches and three Latanoprost concentrations of approximately 5%, 11% and 18%, according to embodiments of the present invention
- FIG. 7C shows elution data for Latanoprost from 0.32 mm diameter, 0.95 mm long drug cores with concentrations of 5, 10 and 20% and drug weights of 3.5, 7 and 14 ⁇ g, respectively, according to embodiments of the present invention
- FIGS. 7D and 7E show dependence of the rate of elution on exposed surface area of the drug core for the three core diameters and the three concentrations as in FIGS. 7A and 7B Latanoprost at day 1 and day 14, respectively, according to embodiments of the present invention
- FIG. 8A shows elution profiles of cyclosporine from drug cores into a buffer solution with surfactant and a buffer solution with surfactant, according to embodiments of the present invention
- FIG. 9A shows normalized elution profiles in nano-grams per device per day over 100 days for bulk sample of silicone with 1% Bimatoprost, according to embodiments of the present invention.
- FIG. 10A shows profiles of elution of Latanoprost from the cores for four formulations of Latanoprost according to embodiments of the present invention.
- FIGS. 1-1 and 1 - 2 show anatomical tissue structures of an eye 2 suitable for treatment with implants, according to an embodiment of the present invention.
- Eye 2 includes a cornea 4 and an iris 6 .
- a sclera 8 surrounds cornea 4 and iris 6 and appears white.
- a conjunctival layer 9 is substantially transparent and disposed over sclera 8 .
- a crystalline lens 5 is located within the eye.
- a retina 7 is located near the back of eye 2 and is generally sensitive to light.
- Retina 7 includes a fovea 7 F that provides high visual acuity and color vision. Cornea 4 and lens 5 refract light to form an image on fovea 7 F and retina 7 .
- the optical power of cornea 4 and lens 5 contribute to the formation of images on fovea 7 F and retina 7 .
- the relative locations of cornea 4 , lens 5 and fovea 7 F are also important to image quality. For example, if the axial length of eye 2 from cornea 4 to retina 7 F is large, eye 2 can be myopic. Also, during accommodation, lens 5 moves toward cornea 4 to provide good near vision of objects proximal to the eye.
- the anatomical tissue structures shown in FIG. 1-1 also include the lacrimal system, which includes an upper canaliculus 10 and a lower canaliculus 12 , collectively the canaliculae, and the naso-lacrimal duct or sac 14 .
- the upper and lower canaliculae terminate in an upper punctum 11 and a lower punctum 13 , also referred to as punctal apertures.
- the punctal apertures are situated on a slight elevation at the medial end of the lid margin at the junction 15 of the ciliary and lacrimal portions near the medial canthus 17 .
- the punctal apertures are round or slightly ovoid openings surrounded by a connective ring of tissue.
- Each of the punctal openings 11 , 13 leads into a vertical portion 10 a , 12 a of the respective canaliculus before turning horizontally to join its other canaliculus at the entrance of a lacrimal sac 14 .
- the canaliculae are tubular and lined by stratified squamous epithelium surrounded by elastic tissue which permits the canaliculus to be dilated.
- FIG. 1A shows a top cross sectional view of a sustained release implant 100 to treat an optical defect of an eye, according to embodiments of the present invention.
- Implant 100 includes a drug core 110 .
- Drug core 110 is an implantable structure that retains a therapeutic agent.
- Drug core 110 comprises a matrix 170 that contains inclusions 160 of therapeutic agent.
- Inclusions 160 will often comprise a concentrated form of the therapeutic agent, for example a crystalline form of the therapeutic agent, and the therapeutic agent may over time dissolve into matrix 170 of drug core 110 .
- Matrix 170 can comprise a silicone matrix or the like, and the mixture of therapeutic agent within matrix 170 can be non-homogeneous.
- the non-homogenous mixture comprises a silicone matrix portion that is saturated with the therapeutic agent and an inclusions portion comprising inclusions of the therapeutic agent, such that the non-homogenous mixture comprises a multiphase non-homogenous mixture.
- inclusions 160 comprise droplets of an oil of the therapeutic agent, for example Latanoprost oil.
- inclusions 160 may comprise particles of the therapeutic agent, for example solid Bimatoprost particles in crystalline form.
- matrix 170 encapsulates inclusions 160
- inclusions 160 may comprise microparticles have dimensions from about 1 ⁇ m to about 100 ⁇ m. The encapsulated inclusions dissolve into the surrounding solid matrix, for example silicone, that encapsulates the micro particles such that matrix 170 is substantially saturated with the therapeutic agent while the therapeutic agent is released from the core.
- Drug core 110 is surrounded by a sheath body 120 .
- Sheath body 120 is can be substantially impermeable to the therapeutic agent, so that the therapeutic agent is often released from an exposed surface on an end of drug core 110 that is not covered with sheath body 120 .
- a retention structure 130 is connected to drug core 110 and sheath body 120 .
- Retention structure 130 is shaped to retain the implant in a hollow tissue structure, for example, a punctum of a canaliculus as described above.
- An occlusive element 140 is disposed on and around retention structure 130 .
- Occlusive element 140 is impermeable to tear flow and occludes the hollow tissue structure and may also serve to protect tissues of the tissue structure from retention structure 130 by providing a more benign tissue-engaging surface.
- Sheath body 120 includes a sheath body portion 150 that connects to retention structure 130 to retain sheath body 120 and drug core 110 .
- Sheath body portion 150 can include a stop to limit movement of sheath body 120 and drug core 110 .
- sheath body portion 150 can be formed with a bulbous tip 150 B. Bulbous tip 150 B can comprise a convex rounded external portion that provides atraumatic entry upon introduction into the canaliculus.
- sheath body portion 150 B can be integral with occlusive element 140 .
- FIG. 1B shows a side cross sectional view of the sustained release implant of FIG. 1A .
- Drug core 110 is cylindrical and shown with a circular cross-section.
- Sheath body 120 comprises an annular portion disposed on drug core 110 .
- Retention structure 130 comprises several longitudinal struts 131 . Longitudinal struts 131 are connected together near the ends of the retention structure. Although longitudinal struts are shown, circumferential struts can also be used.
- Occlusive element 140 is supported by and disposed over longitudinal struts 131 of retention structure 130 and may comprise a radially expandable membrane or the like.
- FIG. 1C shows a perspective view of a sustained release implant 102 with a coil retention structure 132 , according to an embodiment of the present invention.
- Retention structure 132 comprises a coil and retains a drug core 112 .
- a lumen for example channel 112 C, may extend through the drug core 112 to permit tear flow through the lumen for the delivery of therapeutic agent for nasal and systemic applications of the therapeutic agent.
- retention structure 132 and core 112 can be sized to permit tear flow around the drug core and sheath body while the retention element holds tissue of the canaliculus away from the drug core.
- Drug core 112 may be partially covered.
- the sheath body comprises a first component 122 A that covers a first end of drug cove 112 and a second component 122 B that covers a second end of the drug core.
- An occlusive element can be placed over the retention structure and/or the retention structure can be dip coated as described above.
- FIG. 1D shows a perspective view of a sustained release implant 104 with a retention structure 134 comprising struts, according to an embodiment of the present invention.
- Retention structure 134 comprises longitudinal struts and retains a drug core 114 .
- Drug core 114 is covered with a sheath body 124 over most of drug core 114 .
- the drug core releases therapeutic agent through an exposed end and sheath body 124 is annular over most of the drug core as described above.
- An occlusive element can be placed over the retention structure or the retention structure can be dip coated as described above.
- a protrusion that can be engaged with an instrument can extend from sheath body 124 to permit removal of the drug core and sheath body together so as to facilitate replacement of the sheath body and drug core while the retention structure remains implanted in the canaliculus.
- a protrusion that can be engaged with an instrument comprising hook, a loop, a suture or a ring, can extend from retention structure 134 to permit removal of the sustained release implant by removing the retention structure with the protrusion, drug core and sheath body.
- FIG. 1E shows a perspective view of a sustained release implant 106 with a cage retention structure 136 , according to an embodiment of the present invention.
- Retention structure 136 comprises several connected strands of metal and retains a drug core 116 .
- Drug core 116 is covered with a sheath body 126 over most of drug core 116 .
- the drug core releases therapeutic agent through an exposed end and sheath body 126 is annular over most of the drug core as described above.
- An occlusive element can be placed over the retention structure or the retention structure can be dip coated as described above.
- FIG. 1F shows a perspective view of a sustained release implant comprising a core and sheath, according to an embodiment of the present invention.
- Drug core 118 is covered with a sheath body 128 over most of drug core 118 .
- the drug core releases therapeutic agent through an exposed end and sheath body 128 is annular over most of the drug core as described above.
- the rate of therapeutic agent release is controlled by the surface area of the exposed drug core and materials included within drug core 118 .
- the rate of elution of the therapeutic agent is strongly and substantially related to the exposed surface area of the drug core and weakly dependent on the concentration of drug disposed in the inclusions in the drug core.
- the rate of elution is strongly dependent on the diameter of the exposed surface, for example the diameter of an exposed drug core surface near an end of a cylindrical drug core.
- Such an implant can be implanted in ocular tissues, for example below conjunctival tissue layer 9 of the eye and either above sclera tissue layer 8 , as shown in FIG. 1F , or only partially within the scleral tissue layer so as not to penetrate the scleral tissue.
- drug core 118 can be used with any of the retention structures and occlusive elements as described herein.
- the drug core is implanted between sclera 8 and conjunctiva 9 without sheath body 128 .
- the physical characteristics of the drug core can be adjusted to compensate for the increased exposed surface of drug core, for example by reducing the concentration of dissolved therapeutic agent in the drug core matrix as described herein.
- FIG. 1G schematically illustrates a sustained release implant 180 comprising a flow restricting retention structure 186 , a core 182 and a sheath 184 , according to an embodiment of the present invention.
- Sheath body 184 can at least partially cover drug core 182 .
- Drug core 182 may contain inclusions of the therapeutic agent therein to provide a sustained release of the therapeutic agent.
- Drug core 182 can include an exposed convex surface area 182 A. Exposed convex surface area 182 A may provide an increased surface area to release the therapeutic agent.
- An occlusive element 188 can be disposed over retention structure 186 to block the flow of tear through the canaliculus.
- retention structure 186 can be located within occlusive structure 188 to provide the occlusive element integrated with the retention structure.
- Flow restricting retention structure 186 and occlusive element 188 can be sized to block tear flow through the canaliculus.
- the cores and sheath bodies described herein can be implanted in a variety of tissues in several ways. Many of the cores and sheaths described herein, in particular the structures described with reference to FIGS. 2A to 2J can be implanted alone as punctal plugs.
- cores and sheath bodies described herein can comprise a drug core, sheath body, and/or the like so as to be implanted with the retention structures and occlusive elements described herein.
- FIG. 2A shows a cross sectional view of a sustained release implant 200 with core comprising an enlarged exposed surface area, according to an embodiment of the present invention.
- a drug core 210 is covered with a sheath body 220 .
- Sheath body 220 includes an opening 220 A. Opening 220 has a diameter that approximates the maximum cross sectional diameter of drug core 210 .
- Drug core 210 includes an exposed surface 210 E, also referred to as an active surface.
- Exposed surface 210 E includes 3 surfaces: an annular surface 210 A, a cylindrical surface 210 B and an end surface 210 C.
- Annular surface 210 A has an outer diameter that approximates the maximum cross sectional diameter of core 210 and an inner diameter that approximates the outer diameter of cylindrical surface 210 B.
- End surface 210 C has a diameter that matches the diameter of cylindrical surface 210 B.
- the surface area of exposed surface 210 E is the sum of the areas of annular surface 210 A, cylindrical surface 210 B and end surface 210 C
- the surface area may be increased by the size of cylindrical surface area 210 B that extends longitudinally along an axis of core 210 .
- FIG. 2B shows a cross sectional view of a sustained release implant 202 with a core 212 comprising an enlarged exposed surface area 212 A, according to an embodiment of the present invention.
- a sheath body 222 extends over core 212 .
- the treatment agent can be released from the core as described above.
- Exposed surface area 212 A is approximately conical, can be ellipsoidal or spherical, and extends outward from the sheath body to increase the exposed surface area of drug core 212 .
- FIGS. 2C and 2D show perspective and cross sectional views, respectively, of a sustained release implant 204 with a drug core 214 comprising a reduced exposed surface area 214 A, according to an embodiment of the present invention.
- Drug core 214 is enclosed within a sheath body 224 .
- Sheath body 22 includes an annular end portion 224 A that defines an opening through which drug core 214 extends.
- Drug core 214 includes an exposed surface 214 A that releases the therapeutic agent.
- Exposed surface 214 A has a diameter 214 D that is less than a maximum dimension, for example a maximum diameter, across drug core 214 .
- FIG. 2E shows a cross sectional view of a sustained release implant 206 with a drug core 216 comprising an enlarged exposed surface area 216 A with castellation extending therefrom, according to an embodiment of the present invention.
- the castellation includes several spaced apart fingers 216 F to provide increased surface area of the exposed surface 216 A.
- drug core 216 may also include an indentation 2161 .
- Indentation 2161 may have the shape of an inverted cone.
- Core 216 is covered with a sheath body 226 .
- Sheath body 226 is open on one end to provide an exposed surface 216 A on drug core 216 .
- Sheath body 226 also includes fingers and has a castellation pattern that matches core 216 .
- FIG. 2F shows a perspective view of a sustained release implant 250 comprising a core with folds, according to an embodiment of the present invention.
- Implant 250 includes a core 260 and a sheath body 270 .
- Core 260 has an exposed surface 260 A on the end of the core that permits drug migration to the surrounding tear or tear film fluid.
- Core 260 also includes folds 260 F. Folds 260 F increase the surface area of core that is exposed to the surrounding fluid tear or tear film fluid. With this increase in exposed surface area, folds 260 F increase migration of the therapeutic agent from core 260 into the tear or tear film fluid and target treatment area.
- Folds 260 F are formed so that a channel 260 C is formed in core 260 .
- Channel 260 C connects to the end of the core to an opening in exposed surface 260 A and provides for the migration of treatment agent.
- the total exposed surface area of core 260 includes exposed surface 260 A that is directly exposed to the tear or tear film fluid and the surfaces of folds 260 F that are exposed to the tear or tear film fluids via connection of channel 260 C with exposed surface 260 A and the tear or tear film fluid.
- FIG. 2G shows a perspective view of a sustained release implant with a core comprising a channel with an internal porous surface, according to an embodiment of the present invention.
- Implant 252 includes a core 262 and sheath body 272 .
- Core 262 has an exposed surface 262 A on the end of the core that permits drug migration to the surrounding tear or tear film fluid.
- Core 262 also includes a channel 262 C.
- Channel 262 C increases the surface area of the channel with a porous internal surface 262 P formed on the inside of the channel against the core.
- Channel 262 C extends to the end of the core near exposed surface 262 A of the core.
- the surface area of core that is exposed to the surrounding tear or tear film fluid can include the inside of core 262 that is exposed to channel 262 C. This increase in exposed surface area can increase migration of the therapeutic agent from core 262 into the tear or tear film fluid and target treatment area.
- the total exposed surface area of core 262 can include exposed surface 260 A that is directly exposed to the tear or tear film fluid and porous internal surface 262 P that is exposed to the tear or tear film fluids via connection of channel 262 C with exposed surface 262 A and the tear or tear film fluid.
- FIG. 2H shows a perspective view of a sustained release implant 254 with a core 264 comprising channels to increase drug migration, according to an embodiment of the invention.
- Implant 254 includes core 264 and sheath body 274 .
- Exposed surface 264 A is located on the end of core 264 , although the exposed surface can be positioned at other locations. Exposed surface 264 A permits drug migration to the surrounding tear or tear film fluid.
- Core 264 also includes channels 264 C. Channels 264 C extend to exposed surface 264 . Channels 264 C are large enough that tear or tear film fluid can enter the channels and therefore increase the surface area of core 264 that is in contact with tear or tear film fluid.
- the surface area of the core that is exposed to the surrounding fluid tear or tear film fluid includes the inner surfaces 264 P of core 262 that define channels 264 C. With this increase in exposed surface area, channels 264 C increase migration of the therapeutic agent from core 264 into the tear or tear film fluid and target treatment area.
- the total exposed surface area of core 264 includes exposed surface 264 A that is directly exposed to the tear or tear film fluid and internal surface 264 P that is exposed to the tear or tear film fluids via connection of channels 262 C with exposed surface 264 A and the tear or tear film fluid.
- FIG. 2I shows a perspective view of a sustained release implant 256 with a drug core 266 comprising a convex exposed surface 266 A, according to an embodiment of the present invention.
- Drug core 266 is partially covered with a sheath body 276 that extends at least partially over drug core 266 to define convex exposed surface 266 A.
- Sheath body 276 comprises a shaft portion 276 S.
- Convex exposed surface 266 A provides an increased exposed surface area above the sheath body.
- a cross sectional area of convex exposed surface 266 A is larger than a cross sectional area of shaft portion 276 S of sheath body 276 .
- convex exposed surface 266 A has a larger surface area due to the convex shape which extends outward from the core.
- Sheath body 276 comprises several fingers 276 F that support drug core 266 in the sheath body and provide support to the drug core to hold drug core 266 in place in sheath body 276 . Fingers 276 F are spaced apart to permit drug migration from the core to the tear or tear film fluid between the fingers.
- Protrusions 276 P extend outward on sheath body 276 . Protrusions 276 P can be pressed inward to eject drug core 266 from sheath body 276 . Drug core 266 can be replaced with another drug core after an appropriate time, for example after drug core 266 has released most of the therapeutic agent.
- FIG. 2J shows a side view of a sustained release implant 258 with a core 268 comprising an exposed surface area with several soft brush-like members 268 F, according to an embodiment of the present invention.
- Drug core 268 is partially covered with a sheath body 278 that extends at least partially over drug core 268 to define exposed surface 268 A.
- Sheath body 278 comprises a shaft portion 278 S.
- Soft brush-like members 268 F extend outward from drug core 268 and provide an increased exposed surface area to drug core 268 .
- Soft brush-like members 268 F are also soft and resilient and easily deflected such that these members do not cause irritation to neighboring tissue.
- drug core 268 can be made of many materials as explained above, silicone is a suitable material for the manufacture of drug core 268 comprises soft brush like members 268 F. Exposed surface 268 A of drug core 268 also includes an indentation 2681 such that at least a portion of exposed surface 268 A is concave.
- FIG. 2K shows a side view of a sustained release implant 259 with a drug core 269 comprising a convex exposed surface 269 A, according to an embodiment of the present invention.
- Drug core 269 is partially covered with a sheath body 279 that extends at least partially over drug core 269 to define convex exposed surface 269 A.
- Sheath body 279 comprises a shaft portion 279 S.
- Convex exposed surface 269 provides an increased exposed surface area above the sheath body.
- a cross sectional area of convex exposed surface 269 A is larger than a cross sectional area of shaft portion 279 S of sheath body 279 .
- convex exposed surface 269 A has a larger surface area due to the convex shape that extends outward on the core.
- a retention structure 289 can be attached to sheath body 279 .
- Retention structure 289 can comprise any of the retention structures as describe herein, for example a coil comprising a super elastic shape memory alloy such as NitinolTM.
- Retention structure 289 can be dip coated to make retention structure 289 biocompatible.
- FIG. 2L shows a side view of a sustained release implant 230 with a drug core 232 comprising a concave indented surface 232 A to increase exposed surface area of the core, according to an embodiment of the present invention.
- a sheath body 234 extends at least partially over drug core 232 .
- Concave indented surface 232 A is formed on an exposed end of drug core 232 to provide an increased exposed surface area of the drug core.
- FIG. 2M shows a side view of a sustained release implant 240 with a drug core 242 comprising a concave surface 242 A with a channel 242 C formed therein to increase an exposed surface area of the core, according to an embodiment of the present invention.
- a sheath body 244 extends at least partially over drug core 242 .
- Concave indented surface 242 A is formed on an exposed end of drug core 232 to provide an increased exposed surface area of the drug core.
- Channel 242 C formed in drug core 242 to provide an increased exposed surface area of the drug core.
- Channel 242 C can extend to concave indented surface 242 A such that channel 242 C and provide an increase in surface area of the core exposed to the tear or tear film film.
- FIG. 3A shows an implant 310 comprising a sheath body 320 with extensions 322 , according to an embodiment of the present invention.
- Extensions 322 attach sheath body 320 to the retention element to retain the core near the punctum.
- Sheath body 320 extends over core 330 to define an exposed surface 332 of core 330 .
- Extensions 322 can be resilient and engage the retention element and/or occlusive element to attach the sheath body core to the retention element to retain the core near the punctum.
- FIG. 3B shows an implant 350 comprising a retention element 380 with an extension 382 , according to an embodiment of the present invention.
- Extension 382 retains a sheath body 360 and a core 370 .
- Sheath body 360 extends over core 370 to define an exposed surface 372 of core 370 .
- Exposed surface 372 is disposed near the proximal end of core 370 .
- Extension 382 extends downward to retain core 370 and sheath body 370 .
- FIGS. 4A and 4B show a cross-sectional view of an implant 400 with a retention structure 430 that is shorter in length while in a large cross-sectional profile configuration than a small cross-sectional profile configuration, according to an embodiment of the present invention.
- Implant 400 includes a distal end 402 and a proximal end 404 .
- Implant 400 includes a drug core 410 and a sheath body 420 .
- Sheath body 420 at least partially covers drug core 410 and defines an exposed surface 412 of drug core 410 .
- An occlusive element 440 can be attached to and supported by retention structure 430 .
- Occlusive element 440 can move with retention structure 430 , for example when retention element 430 expands from a small profile configuration to a large profile configuration.
- the retention structure and occlusive element are sized to correspond to a diameter of the canaliculus, for example to match a diameter of the canaliculus or slightly larger than the canalicular diameter, so as occlude fluid flow through the canaliculus and/or anchor in the canaliculus.
- retention structure 430 and occlusive element 440 are in a small profile configuration. Such a small profile configuration can occur while the occlusive element and retention structure are placed in a tip of an insertion tool and covered for deployment.
- Retention element 430 and occlusive element 440 extend fully along the length of sheath body 420 and drug core 410 .
- Retention element 430 is attached to sheath body 420 near distal end 402 .
- retention structure 430 and occlusive element 440 have diameters that are sized to fit inside and slide within the canaliculus while in the small profile configuration, and the retention structure and occlusive element can be sized to anchor within the canaliculus while in a second large profile configuration.
- retention structure 430 and occlusive element 440 are in a large profile configuration. Such a large profile configuration can occur when the occlusive element and retention structure are placed in the canaliculus. In the large profile configuration, the length of occlusive element 440 and retention structure 430 is shorter than in the small profile configuration by a distance 450 . The proximal end of retention structure 430 and occlusive element 440 can slide over sheath body 420 when the sheath body and retention structure assume the large profile configuration such that the proximal end of drug core 410 and sheath body 420 extend from the retention structure and occlusive element.
- the sheath body is shorter than drug core 410 by distance 450 so that more of the drug core is exposed while the retention structure and occlusive element are in the large profile configuration than is exposed while the retention structure and occlusive element are in the small profile configuration. In such embodiments, the retention structure and occlusive element retract to expose the drug core.
- FIGS. 5A to 6 show embodiments of tools that can be used to insert many of the implants as describe herein.
- FIG. 5A shows an insertion tool 500 to insert an implant into the punctum with a plunger 530 that can be depressed, according to an embodiment of the present invention.
- Insertion tool 500 includes a dilator 510 that can be inserted into the punctum to pre-dilate the punctum prior to insertion of an implant.
- An implant 520 can be pre-loaded onto tool 500 prior to dilation of the punctum.
- An internal wire 540 can be connected to implant 520 to retain the implant.
- tool 500 can be used to insert implant 520 into the punctum. While implant 520 is positioned in the punctum, plunger 530 can be depressed to engage wire 540 and release implant 520 from tool 500 .
- FIG. 5B shows an insertion tool 550 to insert an implant 570 into the punctum with a plunger that can slide, according to an embodiment of the present invention.
- Insertion tool 550 includes a dilator 560 with a conical section to dilate the punctum.
- Implant 550 includes a plunger 580 that can slide distally to advance implant 570 into the lumen.
- a shaft 590 is connected to plunger 580 to advance implant 570 distally when plunger 580 is advanced distally.
- plunger 580 can be advanced distally to place implant 570 in the canalicular lumen near the punctum.
- a button can be depressed to advance distally the implant into the lumen, for example a button connected to shaft 590 with an intermediate mechanism.
- FIG. 6 shows an insertion tool 600 to insert an implant into the punctum with a sheath 610 that retracts to position the implant in the canalicular lumen, according to an embodiment of the present invention.
- At least a portion of sheath 610 is shaped to dilate the punctum.
- Sheath 610 is shaped to hold an implant 620 in a small profile configuration.
- Insertion tool 600 includes an annular structure 615 , which can comprise a portion of a body 605 of insertion tool 600 .
- Sheath 610 and annular structure 615 are shaped to dilate the punctum and often comprise proximally inclined surfaces to dilate the punctum.
- Implant 620 , sheath 610 and annular structure 615 can be at least partially inserted into the punctum to place the implant in the canalicular lumen.
- Annular structure 615 is disposed over sheath 610 so that sheath 610 can be retracted and slide under annular structure 615 .
- a stop 625 can be connected to body 605 to retain implant 620 at the desired depth within the canalicular lumen while sheath 610 is retracted proximally to expose implant 620 .
- implant 620 is retracted to expose implant 620 at the desired location in the canalicular lumen.
- a plunger 630 can be used to retract sheath 610 .
- a shaft 640 mechanically couples sheath 610 to plunger 630 .
- retraction of plunger 630 in the proximal direction can retract sheath 610 in the proximal direction to expose implant 620 at the desired location in the canalicular lumen.
- Implant 620 can be any of the implants as described herein. Often, implant 620 will comprise a resilient member that expands to a large profile configuration when sheath 610 is retracted.
- insertion tool 600 can include a dilator to dilate the punctum prior to insertion of the implant, and the dilator can be positioned on an end of the insertion tool that opposes the end loaded with the implant, as described herein above.
- FIGS. 5A to 5C schematically illustrate replacement of a drug core 510 and a sheath body 520 , according to an embodiment of the present invention.
- An implant 700 comprises drug core 510 , sheath body 520 and a retention structure 530 .
- Implant 500 can include an occlusive element support by and movable with retention structure 530 .
- retention structure 530 can assume a first small profile configuration prior to implantation and a second large profile configuration while implanted.
- Retention structure 530 is shown in the large profile configuration and implanted in the canalicular lumen.
- Sheath body 520 includes extension 525 A and extension 525 B to attach the sheath body and drug core to retention structure 530 so that the sheath body and drug core are retained by retention structure 530 .
- Drug core 510 and sheath body 520 can be removed together by drawing drug core 510 proximally as shown by arrow 530 .
- Retention structure 530 can remain implanted in the canalicular tissue after drug core 510 and sheath body 520 have been removed as shown in FIG. 5B .
- a replacement core 560 and replacement sheath body 570 can be inserted together as shown in FIG. 5C . Such replacement can be desirable after drug core 510 has released effective amounts of therapeutic agent such that the supply of therapeutic agent in the drug core has diminished and the rate of therapeutic agent released is near the minimum effective level.
- Replacement sheath body 570 includes extension 575 A and extension 575 B.
- Replacement drug core 560 and replacement sheath body 570 can be advanced distally as shown by arrow 590 to insert replacement drug core 560 and replacement sheath body 570 into retention structure 530 .
- Retention structure 530 remains at substantially the same location while replacement drug core 560 and replacement sheath body 570 are inserted into resilient member 530 .
- FIGS. 6A to 6C show deployment of a sustained release implant, according to an embodiment of the present invention.
- a deployment instrument 610 is inserted into a canaliculus 600 through a punctum 600 A.
- a sustained release implant 620 is loaded into a tip of deployment instrument 610 , and a sheath 612 covers sustained release implant 620 .
- Retention structure 630 assumes a small profile configuration while sheath 612 is positioned over retention structure 630 .
- outer sheath 612 of deployment instrument 610 is withdrawn to expose a retention structure 630 of sustained release implant 620 .
- the exposed portion of retention element 630 assumes a large profile configuration.
- FIG. 6A a deployment instrument 610 is inserted into a canaliculus 600 through a punctum 600 A.
- a sustained release implant 620 is loaded into a tip of deployment instrument 610
- a sheath 612 covers sustained release implant 620 .
- Retention structure 630 assumes a small profile configuration while sheath 6
- deployment instrument 610 has been removed and sustained release implant 620 is implanted in canaliculus 600 .
- a drug core 640 is attached retention structure 630 and retained in the canaliculus.
- An outer body sheath 650 covers at least a portion of drug core 640 and drug core 640 releases a therapeutic agent into a liquid tear or tear film 660 near punctum 600 A of canaliculus 600 .
- the sheath body comprises appropriate shapes and materials to control migration of the therapeutic agent from the drug core.
- the sheath body houses the core and can fit snugly against the core.
- the sheath body is made from a material that is substantially impermeable to the therapeutic agent so that the rate of migration of the therapeutic agent may be largely controlled by the exposed surface area of the drug core that is not covered by the sheath body.
- migration of the therapeutic agent through the sheath body can be about one tenth of the migration of the therapeutic agent through the exposed surface of the drug core, or less, often being one hundredth or less.
- the migration of the therapeutic agent through the sheath body is at least about an order of magnitude less that the migration of the therapeutic agent through the exposed surface of the drug core.
- Suitable sheath body materials include polyimide, polyethylene terephthalate” (hereinafter “PET”).
- PET polyethylene terephthalate
- the sheath body has a thickness, as defined from the sheath surface adjacent the core to the opposing sheath surface away from the core, from about 0.00025′′ to about 0.0015′′.
- the total diameter of the sheath that extends across the core ranges from about 0.2 mm to about 1.2 mm.
- the core may be formed by dip coating the core in the sheath material.
- the sheath body can comprise a tube and the core introduced into the sheath, for example as a liquid or solid that can be slid, injected and/or extruded into the sheath body tube.
- the sheath body can also be dip coated around the core, for example dip coated around a pre-formed core.
- the sheath body can be provided with additional features to facilitate clinical use of the implant.
- the sheath may receive a drug core that is exchangeable while the retention structure and sheath body remain implanted in the patient.
- the sheath body is often rigidly attached to the retention structure as described above, and the core is exchangeable while the retention structure retains the sheath body.
- the sheath body can be provided with external protrusions that apply force to the sheath body when squeezed and eject the core from the sheath body. Another drug core can then be positioned in the sheath body.
- the sheath body and/or retention structure may have a distinguishing feature, for example a distinguishing color, to show placement such that the placement of the sheath body and/or retention structure in the canaliculus or other body tissue structure can be readily detected by the patient.
- the retention element and/or sheath body may comprise at least one mark to indicate the depth of placement in the canaliculus such that the retention element and/or sheath body can be positioned to a desired depth in the canaliculus based on the at least one mark.
- the retention structure comprises an appropriate material that is sized and shaped so that the implant can be easily positioned in the desired tissue location, for example the canaliculus.
- the retention structure is mechanically deployable and typically expands to a desired cross sectional shape, for example with the retention structure comprising a super elastic shape memory alloy such as NitinolTM.
- a super elastic shape memory alloy such as NitinolTM.
- Other materials in addition to NitinolTM can be used, for example resilient metals or polymers, plastically deformable metals or polymers, shape memory polymers, and the like, to provide the desired expansion.
- polymers and coated fibers available from Biogeneral, Inc. of San Diego, Calif. may be used.
- Many metals such as stainless steels and non-shape memory alloys can be used and provide the desired expansion. This expansion capability permits the implant to fit in hollow tissue structures of varying sizes, for example canaliculac ranging from 0.3 mm to 1.2 mm (i.e. one size fits all).
- a single retention structure can be made to fit canaliculae from 0.3 to 1.2 mm across
- a plurality of alternatively selectable retention structures can be used to fit this range if desired, for example a first retention structure for canaliculae from 0.3 to about 0.9 mm and a second retention structure for canaliculae from about 0.9 to 1.2 mm.
- the retention structure has a length appropriate to the anatomical structure to which the retention structure attaches, for example a length of about 3 mm for a retention structure positioned near the punctum of the canaliculus. For different anatomical structures, the length can be appropriate to provide adequate retention force, e.g. 1 mm to 15 mm lengths as appropriate.
- the sheath body and drug core are attached to one end of the retention structure as described above, in many embodiments the other end of retention structure is not attached to drug core and sheath body so that the retention structure can slide over the sheath body and drug core while the retention structure expands.
- This sliding capability on one end is desirable as the retention structure may shrink in length as the retention structure expands in width to assume the desired cross sectional width.
- many embodiments may employ a sheath body that does not slide in relative to the core.
- the retention structure can be retrieved from tissue.
- a protrusion for example a hook, a loop, or a ring, can extend from the retention structure to facilitate removal of the retention structure.
- the occlusive element comprises an appropriate material that is sized and shaped so that the implant can at least partially inhibit, even block, the flow of fluid through the hollow tissue structure, for example lacrimal fluid through the canaliculus.
- the occlusive material shown is a thin walled membrane of a biocompatible material, for example silicone, that can expand and contract with the retention structure.
- the occlusive element is formed as a separate thin tube of material that is slid over the end of the retention structure and anchored to one end of the retention structure as described above.
- the occlusive element can be formed by dip coating the retention structure in a biocompatible polymer, for example silicone polymer.
- the thickness of the occlusive element can be in a range from about 0.01 mm to about 0.15 mm, and often from about 0.05 mm to 0.1 mm.
- a “therapeutic agent” can comprise a drug may be any of the following or their equivalents, derivatives or analogs, including, anti-glaucoma medications, (e.g. adrenergic agonists, adrenergic antagonists (beta blockers), carbonic anhydrase inhibitors (CAIs, systemic and topical), parasympathomimetics, prostaglandins and hypotensive lipids, and combinations thereof), antimicrobial agent (e.g., antibiotic, antiviral, antiparacytic, antifungal, etc.), a coiticosteroid or other anti-inflammatory (e.g., an NSAID), a decongestant (e.g., vasoconstrictor), an agent that prevents of modifies an allergic response (e.g., an antihistamine, cytokine inhibitor, leucotriene inhibitor, IgE inhibitor, immunomodulator), a mast cell stabilizer, cycloplegic or the like.
- the therapeutic agent examples include but are not limited to glaucoma, pre and post surgical treatments, dry eye and allergies.
- the therapeutic agent may be a lubricant or a surfactant, for example a lubricant to treat dry eye.
- Exemplary therapeutic agents include, but are not limited to, thrombin inhibitors; antithrombogenic agents; thrombolytic agents; fibrinolytic agents; vasospasm inhibitors; vasodilators; antihypertensive agents; antimicrobial agents, such as antibiotics (such as tetracycline, chlortetracycline, bacitracin, neomycin, polymyxin, gramicidin, cephalexin, oxytetracycline, chloramphenicol, rifampicin, ciprofloxacin, tobramycin, gentamycin, erythromycin, penicillin, sulfonamides, sulfadiazine, sulfacetamide, sulfamethizole, sulfisoxazole, nitrofurazone, sodium propionate), antifungals (such as amphotericin B and miconazole), and antivirals (such as idoxuridine trifluorothymidine,
- Such anti inflammatory steroids contemplated for use in the methodology of the present invention include triamcinolone acetonide (generic name) and corticosteroids that include, for example, triamcinolone, dexamethasone, fluocinolone, cortisone, prednisolone, flumetholone, and derivatives thereof.); antiallergenics (such as sodium chromoglycate, antazoline, methapyriline, chlorpheniramine, cetrizine, pyrilamine, prophenpyridamine); anti proliferative agents (such as 1,3-cis retinoic acid, 5-fluorouracil, taxol, rapamycin, mitomycin C and cisplatin); decongestants (such as phenylephrine, naphazoline, tetrahydrazoline); miotics and anti-cholinesterase (such as pilocarpine, salicylate, carbachol, acetylcholine chloride, physos
- the amount of drug associated with the drug-delivery device may vary depending on the particular agent, the desired therapeutic benefit and the time during which the device is intended to deliver the therapy. Since the devices of the present invention present a variety of shapes, sizes and delivery mechanisms, the amount of drug associated with the device will depend on the particular disease or condition to be treated, and the dosage and duration that is desired to achieve the therapeutic effect. Generally, the amount of drug is at least the amount of drug that upon release from the device, is effective to achieve the desired physiological or pharmacological local or systemic effects.
- Embodiments of the drug delivery devices of the present invention can be adapted to provide delivery of drug at a daily rate that is substantially below the therapeutically effective drop form of treatment so as to provide a large therapeutic range with a wide safety margin.
- many embodiments treat the eye with therapeutic levels for extended periods that are no more than 5 or 10 percent of the daily drop dosage. Consequently, during an initial bolus or washout period of about one to three days, the implant can elute the therapeutic agent at a rate that is substantially higher than the sustained release levels and well below the daily drop form dosage.
- the amount of drug initially released is less than the 2500 ng of drug that may be present in a drop of drug delivered to the eye.
- This used use of sustained release levels substantially below the amount of drug in a drop and/or drops administered daily allows the device to release a therapeutically beneficial amount of drug to achieve the desired therapeutic benefit with a wide safety margin, while avoiding an inadequate or excessive amount of drug at the intended site or region.
- An extended period of time may mean a relatively short period of time, for example minutes or hours (such as with the use of an anesthetic), through days or weeks (such as the use of pre-surgical or post-surgical antibiotics, steroids, or NSAIDs and the like), or longer (such as in the case of glaucoma treatments), for example months or years (on a recurring basis of use of the device).
- a drug such as Timolol maleate, a beta1 and beta2 (non-selective) adrenergic receptor blocking agent can be used in the device for a release over an extended period of time such as 3 months.
- Three months is a relatively typical elapsed time between physician visits for a glaucoma patient undergoing topical drop therapy with a glaucoma drug, although the device could provide treatment for longer or shorter durations.
- a 0.25% concentration of Timolol translates to from 2.5 to 5 mg/1000 ⁇ L, typically being 2.5 mg/l 000 ⁇ L.
- a drop of Timolol for topical application is usually in the range of 40-60 ⁇ L, typically being 50 ⁇ L.
- a delivery device might contain from 270 to 1350 ⁇ g, for example 720 ⁇ g, of the drug for a 90 day, or 3 month, extended release.
- the drug would be contained within the device and eluted based on the polymer or drug/hydrogel concentration.
- the drug can be similarly contained on the device and eluted for olopatadine hydrochloride (Patanol®) and other drugs in a manner similar to Timolol.
- Timolol maleate Commercially available solutions of Timolol maleate are available in 0.25% and 0.5% preparations, and the initial dosage can be 1 drop twice per day of 0.25% solution.
- a 0.25% concentration of Timolol is equivalent to 2.5 mg per 1000 ⁇ l.
- a sustained release quantity of Timolol released each day from the drug core can be from about 3 to 15 ⁇ g each day. Although the sustained release quantity delivered each day from the device may vary, a sustained release delivery of about 8 ⁇ g per day corresponds to about 3.2% of the 0.250 mg of Timolol applied with two drops of a 0.25% solution.
- this glaucoma medication has concentrations that are about 1/10 th that of Timolol. Therefore, the amount of drug on the implantable device, depending on the bioavailability, would be significantly less—approximately 20-135 ⁇ g and typically 50-100 ⁇ g—for Latanoprost and other prostaglandin analogues. This also translates to a device that can either be smaller than one required for a beta blocker delivery or can house more drug for a longer release period.
- a drop of Xalatan contains about 2.5 ⁇ g of Latanoprost, assuming a 50 ⁇ L drop volume. Therefore, assuming that about 8% of 2.5 ⁇ g is present 5 minutes after instillation, only about 200 ng of drug remains on the eye. Based on the Latanoprost clinical trials, this amount is effective in lowering IOP for at least 24 hours.
- Pfizer/Pharmacia conducted several dose-response studies in support of the NDA for Xalatan. The doses ranged from 12.5 ⁇ g/mL to 115 ⁇ g/mL of Latanoprost. The current dose of Latanoprost, 50 ⁇ g/mL, given once per day, was shown to be optimal.
- the concentrations of Latanoprost are about 1/100 th , or 1 percent, that of Timolol, and in specific embodiments the concentrations of Latanoprost may be about 1/50 th , or 2 percent, that of Timolol.
- concentrations of Latanoprost may be about 1/50 th , or 2 percent, that of Timolol.
- commercially available solution preparations of Latanoprost are available at concentrations 0.005%, often delivered with one drop per day.
- the therapeutically effective concentration of drug released from the device per day can be about 1/100 th of Timolol, about 30 to 150 ng per day, for example about 80 ng, assuming tear washout and bioavailability similar to Timolol.
- the amount of drug on the implantable device can be significantly less—approximately 1% to 2% of Timolol, for example 2.7 to 13.5 ⁇ g, and can also be about 3 to 20 ⁇ g, for Latanoprost and other prostaglandin analogues.
- the sustained release amount of Latanoprost released each day can vary, a sustained release of 80 ng per day corresponds to about 3.2% of the 2.5 ⁇ g of Latanoprost applied with a single drop of a 0.005% solution
- this glaucoma medication may have concentrations that are 1/20 th or less than that of Timolol. Therefore, the amount of drug loaded on the extended release device for a 3 to 6 month extended release, depending on the bioavailability, can be significantly less, approximately 5-30 ⁇ g and typically 10-20 ⁇ g—for Bimatoprost and analogues and derivatives thereof.
- the implant can house more drug for a longer sustained release period, for example 20-40 ⁇ g for a sustained release period of 6 to 12 months with Bimatoprost and its derivatives. This decrease in drug concentration can also translate to a device that can be smaller than one required for a beta blocker delivery.
- Bimatoprost Commercially available solution concentrations of Bimatoprost are 0.03% by weight, often delivered once per day. Although the sustained release amount of Bimatoprost released each day can vary, a sustained release of 300 ng per day corresponds to about 2% of the 15 ⁇ g of Bimatoprost applied with a single drop of a 0.03% solution. Work in relation with the present invention suggests that even lower sustained release doses of Bimatoprost can provide at least some reduction in intraocular pressure, for example 20 to 200 ng of Bimatoprost and daily sustained release dosages of 0.2 to 2% of the daily drop dosage.
- this glaucoma medication may have concentrations that are 2% or less than that of Timolol.
- concentrations are 0.004%, often delivered once per day.
- the therapeutically effective concentration of drug released from the device per day can be about 65 ng, assuming tear washout and bioavailability similar to Timolol. Therefore, the amount of drug on the implantable device, depending on the bioavailability, would be significantly less. This also translates to a device that can either be smaller than one required for a beta blocker delivery or can house more drug for a longer release period.
- the amount of drug on the implantable device can be significantly less—approximately 1/100 of Timolol, for example 2.7 to 13.5 ⁇ g, and typically about 3 to 20 ⁇ g, for Travoprost, Latanoprost and other prostaglandin F2 ⁇ analogues.
- the sustained release amount of Latanoprost released each day can vary, a sustained release of 65 ng per day corresponds to about 3.2% of the 2.0 ⁇ g of Travoprost applied with a single drop of a 0.004% solution.
- the therapeutic agent may comprise a cortico steriod, for example fluocinolone acetonide, to treat a target ocular tissue.
- fluocinolone acetonide can be released from the canaliculus and delivered to the retina as a treatment for diabetic macular edema (DME).
- DME diabetic macular edema
- a bolus of the drug may be released by the formation of an erodable polymer cap that is immediately dissolved in the tear or tear film. As the polymer cap comes in contact with the tear or tear film, the solubility properties of the polymer enable the cap to erode and the drug is released all at once.
- a burst release of a drug can be performed using a polymer that also erodes in the tear or tear film based on the polymer solubility.
- the drug and polymer may be stratified along the length of the device so that as the outer polymer layer dissolves, the drug is immediately released.
- a high or low release rate of the drug could be accomplished by changing the solubility of the erodable polymer layer so that the drug layer released quickly or slowly.
- Other methods to release the drug could be achieved through porous membranes, soluble gels (such as those in typical ophthalmic solutions), microparticle encapsulations of the drug, or nanoparticle encapsulation, depending on the size of the drug molecule.
- the drug core comprises the therapeutic agent and materials to provide sustained release of the therapeutic agent.
- the therapeutic agent migrates from the drug core to the target tissue, for example ciliary muscles of the eye.
- the therapeutic agent may optionally be only slightly soluble in the matrix so that a small amount of therapeutic agent is dissolved in the matrix and available for release from the surface of drug core 110 .
- the rate of migration from the core to the tear or tear film can be related to the concentration of therapeutic agent dissolved in the matrix.
- the rate of migration of therapeutic agent from the core to the tear or tear film can be related to properties of the matrix in which the therapeutic agent dissolves.
- the rate of migration from the drug core to the tear or tear film can be based on a silicone formulation.
- the concentration of therapeutic agent dissolved in the drug core may be controlled to provide the desired rate of release of the therapeutic agent.
- the therapeutic agent included in the core can include liquid, solid, solid gel, solid crystalline, solid amorphous, solid particulate, and/or dissolved forms of the therapeutic agent.
- the drug core comprises a silicone matrix containing the therapeutic agent.
- the therapeutic agent may comprise liquid or solid inclusions, for example liquid Latanoprost droplets or solid Bimatoprost particles, respectively, dispersed in the silicone matrix.
- the drug core can comprise one or more biocompatible materials capable of providing a sustained release of the therapeutic agent.
- the drug core is described above with respect to an embodiment comprising a matrix with a substantially non-biodegradable silicone matrix with inclusions of the drug located therein that dissolve, the drug core can include structures that provide sustained release of the therapeutic agent, for example a biodegradable matrix, a porous drug core, liquid drug cores and solid drug cores.
- a matrix that contains the therapeutic agent can be formed from either biodegradable or non-biodegradable polymers.
- a non-biodegradable drug core can include silicone, acrylates, polyethylenes, polyurethane, polyurethane, hydrogel, polyester (e.g., DACRON® from E. I.
- PTFE polytetrafluoroethylene
- ePTFE expanded PTFE
- PEEK polyether ether ketone
- nylon extruded collagen
- polymer foam silicone rubber
- polyethylene terephthalate ultra high molecular weight polyethylene
- polycarbonate urethane polyurethane
- polyimides stainless steel, nickel-titanium alloy (e.g., Nitinol), titanium, stainless steel, cobalt-chrome alloy (e.g., ELGILOY® from Elgin Specialty Metals, Elgin, Ill.; CONICHROME® from Carpenter Metals Corp., Wyomissing, Pa.).
- ELGILOY® from Elgin Specialty Metals, Elgin, Ill.
- CONICHROME® from Carpenter Metals Corp., Wyomissing, Pa.
- a biodegradable drug core can comprise one or more biodegradable polymers, such as protein, hydrogel, polyglycolic acid (PGA), polylactic acid (PLA), poly(L-lactic acid) (PLLA), poly(L-glycolic acid) (PLGA), polyglycolide, poly-L-lactide, poly-D-lactide, poly(amino acids), polydioxanone, polycaprolactone, polygluconate, polylactic acid-polyethylene oxide copolymers, modified cellulose, collagen, polyorthoesters, polyhydroxybutyrate, polyanhydride, polyphosphoester, poly(alpha-hydroxy acid) and combinations thereof.
- the drug core can comprise at least one of hydrogel polymer.
- the rate of release of the therapeutic agent can be related to the concentration of therapeutic agent dissolved in the drug core.
- the drug core comprises non-therapeutic agents that are selected to provide a desired solubility of the therapeutic agent in the drug core.
- the non-therapeutic agent of the drug core can comprise polymers as described herein and additives.
- a polymer of the core can be selected to provide the desired solubility of the therapeutic agent in the matrix.
- the core can comprise hydrogel that may promote solubility of hydrophilic treatment agent.
- functional groups can be added to the polymer to provide the desired solubility of the therapeutic agent in the matrix.
- functional groups can be attached to silicone polymer.
- additives may be used to control the release kinetics of therapeutic agent.
- the additives may be used to control the concentration of therapeutic agent by increasing or decreasing solubility of the therapeutic agent in the drug core so as to control the release kinetics of the therapeutic agent.
- the solubility may be controlled by providing appropriate molecules and/or substances that increase and/or decrease the solubility of the dissolved from of the therapeutic agent to the matrix.
- the solubility of the dissolved from the therapeutic agent may be related to the hydrophobic and/or hydrophilic properties of the matrix and therapeutic agent.
- surfactants, tinuvin, salts and water can be added to the matrix and may increase the solubility of hydrophilic therapeutic agent in the matrix.
- oils and hydrophobic molecules and can be added to the matrix and may increase the solubility of hydrophobic treatment agent in the matrix.
- the surface area of the drug core can also be controlled to attain the desired rate of drug migration from the core to the target site.
- a larger exposed surface area of the core will increase the rate of migration of the treatment agent from the drug core to the target site, and a smaller exposed surface area of the drug core will decrease the rate of migration of the therapeutic agent from the drug core to the target site.
- the exposed surface area of the drug core can be increased in any number of ways, for example by any of castellation of the exposed surface, a porous surface having exposed channels connected with the tear or tear film, indentation of the exposed surface, protrusion of the exposed surface.
- the exposed surface can be made porous by the addition of salts that dissolve and leave a porous cavity once the salt dissolves.
- Hydrogels may also be used, and can swell in size to provide a larger exposed surface area. Such hydrogels can also be made porous to further increase the rate of migration of the therapeutic agent.
- an implant may be used that includes the ability to release two or more drugs in combination, such as the structure disclosed in U.S. Pat. No. 4,281,654 (Shell).
- a prostaglandin or a prostaglandin and a cholinergic agent or an adrenergic antagonist (beta blocker), such as Alphagan®, or a prostaglandin and a carbonic anhydrase inhibitor.
- drug impregnated meshes may be used such as those disclosed in US Patent Publication No. 2002/0055701 or layering of biostable polymers as described in US Patent Publication No. 2005/0129731.
- Certain polymer processes may be used to incorporate drug into the devices of the present invention such as, so-called “self-delivering drugs” or PolymerDrugs (Polymerix Corporation, Piscataway, N.J.) are designed to degrade only into therapeutically useful compounds and physiologically inert linker molecules, further detailed in US Patent Publication No. 2005/0048121 (East), hereby incorporated by reference in its entirety.
- Such delivery polymers may be employed in the devices of the present invention to provide a release rate that is equal to the rate of polymer erosion and degradation and is constant throughout the course of therapy.
- Such delivery polymers may be used as device coatings or in the form of microspheres for a drug depot injectable (such as a reservoir of the present invention).
- a further polymer delivery technology may also be adapted to the devices of the present invention such as that described in US Patent Publication No. 2004/0170685 (Carpenter), and technologies available from Medivas (San Diego, Calif.).
- the drug core matrix comprises a solid material, for example silicone, that encapsulates inclusions of the drug.
- the drug comprises molecules which are very insoluble in water and slightly soluble in the encapsulating drug core matrix.
- the inclusions encapsulated by the drug core can be micro-particles having dimensions from about 1 ⁇ m to about 100 ⁇ m across.
- the drug inclusions can comprise crystals, for example Bimatoprost crystals, and/or droplets of oil, for example with Latanoprost oil.
- the drug inclusions can dissolve into the solid drug core matrix and substantially saturate the drug core matrix with the drug, for example dissolution of Latanoprost oil into the solid drug core matrix.
- the rate limiting step of drug delivery is transport of the drug from the surface of the drug core matrix exposed to the tear film.
- the drug core matrix is substantially saturated with the drug, gradients in drug concentration within the matrix are minimal and do not contribute significantly to the rate of drug delivery.
- surface area of the drug core exposed to the tear film is nearly constant, the rate of drug transport from the drug core into the tear film can be substantially constant.
- the solubility of the therapeutic agent in water and molecular weight of the drug can effect transport of the drug from the solid matrix to the tear.
- the therapeutic agent is nearly insoluble in water and has a solubility in water of about 0.03% to 0.002% by weight and a molecular weight from about 400 grams/mol. to about 1200 grams/mol.
- the therapeutic agent has a very low solubility in water, for example from about 0.03% by weight to about 0.002% by weight, a molecular weight from about 400 grams per mole (g/mol.) to about 1200 g/mol, and is readily soluble in an organic solvent.
- Cyclosporin A (CsA) is a solid with an aqueous solubility of 27.67 ⁇ g/mL at 25° C., or about 0.0027% by weight, and a molecular weight (M.W.) of 1202.6 g/mol.
- Latanoprost is a prostaglandin F2 ⁇ analogue, a liquid oil at room temperature, and has an aqueous solubility of 50 ⁇ g/mL in water at 25° C., or about 0.005% by weight and a M.W. of 432.6 g/mol.
- Bimatoprost is a synthetic prostamide analogue, a solid at room temperature solubility in water of 300 ⁇ g/mL in water at 25° C., or 0.03% by weight, and has a M.W. of 415.6 g/mol.
- о ⁇ ки may effect transport of the drug dissolved in the solid matrix from the core to the tear film.
- the drug core can be adapted in response to the surfactant in the tear film to provide sustained delivery of the drug into the tear film at therapeutic levels.
- empirical data can be generated from a patient population, for example 10 patients whose tears are collected and analyzed for surfactant content. Elution profiles in the collected tears for a drug that is sparingly soluble in water, for example cyclosporine, can also be measured and compared with elution profiles in buffer and surfactant such that an in vitro model of tear surfactant is developed. An in vitro solution with surfactant based on this empirical data can be used to adjust the drug core in response to the surfactant of the tear film.
- the drug cores may also be modified to utilize carrier vehicles such as nanoparticles or microparticles depending on the size of the molecule to be delivered such as latent-reactive nanofiber compositions for composites and nanotextured surfaces (Innovative Surface Technologies, LLC, St. Paul, Minn.), nanostructured porous silicon, known as BioSilicont, including micron sized particles, membranes, woven fivers or micromachined implant devices (pSividia, Limited, UK) and protein nanocage systems that target selective cells to deliver a drug (Chimeracore).
- carrier vehicles such as nanoparticles or microparticles depending on the size of the molecule to be delivered such as latent-reactive nanofiber compositions for composites and nanotextured surfaces (Innovative Surface Technologies, LLC, St. Paul, Minn.), nanostructured porous silicon, known as BioSilicont, including micron sized particles, membranes, woven fivers or micromachined implant devices (pSividia, Limited, UK) and protein nanocage systems that target selective
- the drug insert comprises of a thin-walled polyimide tube sheath with a drug core comprising Latanoprost dispersed in Nusil 6385 (MAF 970), a medical grade solid silicone that serves as the matrix for drug delivery.
- the distal end of the drug insert is sealed with a cured film of solid Loctite 4305 medical grade adhesive.
- the drug insert may be placed within the bore of the punctum plug, the Loctite 4305 adhesive does not come into contact with either tissue or the tear film.
- the inner diameter of the drug insert can be 0.32 mm; and the length can be 0.95 mm.
- Drug cores can comprise 3.5, 7 or 14 ⁇ g Latanoprost, with percent by weight concentrations of 5, 10 and 20% respectively. Assuming an overall elution rate of approximately 100 ng/day, the drug core comprising 14 ⁇ g of Latanoprost is adapted to deliver drug for approximately at least 100 days, for example 120 days.
- the overall weight of the drug core, including Latanoprost can be ⁇ 70 ⁇ g.
- the weight of the drug insert including the polyimide sleeve can be approximately 100 ⁇ g.
- the drug core may elute with an initial elevated level of therapeutic agent followed by substantially constant elution of the therapeutic agent.
- an amount of therapeutic agent released daily from the core may be below the therapeutic levels and still provide a benefit to the patient.
- An elevated level of eluted therapeutic agent can result in a residual amount of therapeutic agent and/or residual effect of the therapeutic agent that is combined with a sub-therapeutic amount of therapeutic agent to provide relief to the patient.
- therapeutic level is about 80 ng per day
- the device may deliver about 100 ng per day for an initial delivery period.
- the extra 20 ng delivered per day can have a beneficial effect when therapeutic agent is released at levels below the therapeutic level, for example at 60 ng per day.
- an initial elevated dose may not result in complications and/or adverse events to the patient.
- Drug cores as described above have been fabricated with different cross sectional sizes of 0.006 inches, 0.012 inches, and 0.025 inches, and drug concentrations of 5%, 10% and 20% in a silicone matrix. Theses drug cores can be made with a Syringe Tube and Cartridge Assembly, Mixing Latanoprost with Silicone, and Injecting the mixture into a polyimide tube which is cut to desired lengths and sealed.
- the length of the drug cores were approximately 0.80 to 0.95 mm, which for a diameter of 0.012 inches (0.32 mm) corresponds to total Latanoprost content in the drug cores of approximately 3.5 ⁇ g, 7 ⁇ g and 14 ⁇ g for concentrations of 5%, 10% and 20%, respectively.
- Syringe Tube and Cartridge Assembly 1. Take polyimide tubing of three different diameters 0.006 inches, 0.0125 inches and 0.025 inches. 2. Cut polyimide tubing of different diameters to ⁇ 15 cm length. 3. Insert Polyimide tubes into a Syringe Adapter. 4. Adhesive bond polyimide tube into luer adapter (Loctite, low viscosity UV cure). 5. Trim end of assembly. 6. Clean the cartridge assembly using distilled water and then with methanol and dry it in oven at 60° C.
- Inject tube 1. Insert Cartridge and Polyimide tubes assembly into 1 ml syringe. 2. Add one drop of catalyst, (MED-6385 Curing Agent) in the syringe. 3. Force excess catalyst out of the polyimide tube with clean air. 4. Fill syringe with silicone drug matrix. 5. Inject tube with drug matrix until the tube is filled or the syringe plunger becomes too difficult to push. 6. Close off the distal end of the polyimide tube and maintain pressure until the silicone begins to solidify. 7. Allow to cure at room temperature for 12 hours. 8. Place under vacuum for 30 minutes. 9. Place tube in right size trim fixture (prepared in house to hold different size tubing) and cut drug inserts to length (0.80-0.95 mm).
- catalyst MED-6385 Curing Agent
- FIGS. 7A and 7B show elution data of Latanoprost at day 1 and day 14, respectively, for the three core diameters of 0.006, 0.012 and 0.025 inches and three Latanoprost concentrations of approximately 5%, 11% and 18%. Elution rate of the Latanoprost in nanograms (ng) per day is plotted versus percent concentration. These data show that the rate of elution is mildly dependent on the concentration and strongly dependent on the exposed surface area at both time periods.
- the 0.006 inch, 0.012 inch and 0.025 inch diameter cores released about 200 ng, 400 ng and 1200 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core.
- the quantity of Latanoprost released is compared to the concentration of drug in the drug core with a least square regression line.
- the slope of the regression lines are 11.8, 7.4 and 23.4, respectively.
- the 0.006 inch, 0.012 inch (0.32 mm) and 0.025 inch diameter cores released about 25 ng, 100 ng and 300 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core at extended periods of time, and that the quantity of Latanoprost released is mildly dependent on the concentration of therapeutic agent in the core.
- the quantity of Latanoprost released is compared to the concentration of drug in the drug core with a least square regression line.
- the slope of the regression lines are 3.0, 4.3 and 2.2, respectively.
- FIGS. 7D and 7E show dependence of the rate of elution on exposed surface area of the drug core for the three core diameters and the three concentrations as in FIGS. 7A and 7B Latanoprost at day 1 and day 14, respectively, according to embodiments of the present invention.
- Elution rate of the Latanoprost in nanograms (ng) per day is plotted versus the exposed surface area of the drug core in mm 2 as determined by the diameter of the drug core.
- the exposed surface areas of the 0.006 inch, 0.012 inch and 0.025 inch diameter cores are approximately 0.02, 0.07, and 0.32 mm 2 , respectively.
- the 0.02, 0.07, and 0.32 mm 2 cores released about 200 ng, 400 ng and 1200 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core.
- the quantity of Latanoprost released is compared to the exposed surface area of the drug core with a least square regression line.
- the slope of the regression lines are 2837.8, 3286.1 and 3411.6, respectively, with R 2 coefficients of 0.9925, 0.9701 and 1, respectively.
- the slope of the regression lines are 812.19, 1060.1 and 764.35, respectively, with R 2 coefficients of 0.9904, 0.9924 and 0.9663, respectively.
- FIG. 7C shows elution data for Latanoprost from 0.32 mm diameter, 0.95 mm long drug cores with concentrations of 5, 10 and 20% and drug weights of 3.5, 7 and 14 ⁇ g, respectively, according to embodiments of the present invention.
- the drug cores were manufactured as described above.
- the elution rate is plotted in ng per day from 0 to 40 days.
- the 14 ⁇ g core shows rates of approximately 100 ng per day from about 10 to 40 days.
- the 7 ⁇ g core shows comparable rates from 10 to 20 days.
- Table 2 shows the expected parameters for each drug concentration. As shown in FIG. 1C , in vitro results in a buffered saline elution system show that the plug initially elutes approximately 500 ng of Latanoprost per day, dropping off rapidly within 7-14 days to approximately 100 ng/day, depending on the initial concentration of drug.
- the duration of the drug core can be determined based on the calculated time when ⁇ 10% of the original amount of drug remains in drug insert, for example where the elution rate levels out and remains substantially constant at approximately 10 ng/day.
- FIG. 8A shows elution profiles of cyclosporin from drug cores into a buffer solution without surfactant and into a buffer solution with surfactant, according to embodiments of the present invention.
- the buffer solution was made as described above.
- the solution with surfactant includes 95% buffer and 5% surfactant, UP-1005 Ultra Pure Fluid from Dow Corning, Midland Mich.
- Work in relation with embodiments of the present invention indicates that in at least some instances, surfactants may be used in in vitro to model in situ elution from the eye as the eye can include natural surfactants, for example Surfactant Protein D, in the tear film.
- the elution profile of cyclosporin into surfactant is approximately 50 to 100 ng per day from 30 to 60 days.
- Empirical data from tears of a patient population for example 10 patients, can be measured and used to refine the in vitro model with appropriate amounts of surfactant.
- the drug core matrix may be modified in response to the human tear surfactant as determined with the modified in vitro model.
- the drug core can be modified in many ways in response to the human tear film surfactant, for example with an increased exposed surface area and/or additives to increase an amount of cyclosporine drug dissolved in the core, as described above, to increase elution from the core to therapeutic levels, if appropriate.
- the calculated heights ranged from 0.33 cm to 0.42 cm.
- the exposed surface area on each end of each bulk sample was approximately 0.045 cm 2 , providing volumes of 0.019 cm and 0.015 cm 3 for the 0.42 and 0.33 cm samples, respectively.
- the exposed an exposed surface area of samples calculated from the height and diameter without a drug sheath was approximately 0.1 cm 2 .
- Three formulations were evaluated: 1) silicone 4011, 1% Bimatoprost, 0% surfactant; 2) silicone 4011, 1% Bimatoprost, approximately 11% surfactant; and 3) silicone 4011, 1% Bimatoprost, approximately 33% surfactant.
- FIG. 9A shows normalized elution profiles in ng per device per day over 100 days for bulk sample of silicone with 1% Bimatoprost, assuming an exposed surface diameter of 0.3 mm on the end of the device, according to embodiments of the present invention.
- the normalized elution profile is about 10 ng per day.
- the data show approximately zero order release kinetics from about ten days to about 90 days for each of the formulations.
- the core can comprise a 0.76 mm diameter core with an exposed surface diameter of 0.76 mm, corresponding to an exposed surface area of 0.0045 cm 2 .
- the core can be covered with a sheath to define the exposed surface of the core as described above.
- the normalized elution profile for such a device is approximately 6 times (0.0045 cm 2 /0.00078 cm 2 ) the elution profile for the device with a 0.3 mm diameter exposed surface area.
- a zero order elution profile with an elution rate of about 60 ng per day can be obtained over a period of about 90 days.
- the zero order elution rat is about 100 ng per day over a period of about 90 days.
- the concentration can also be increased from 1%. Similar elution profiles can be obtained with Latanoprost.
- Drug cores were manufactured as described above with Latanoprost and silicone 4011, 6385 and/or NaCl.
- Four formulations were manufactured as follows: A) silicone 4011, approximately 20% Latanoprost, and approximately 20% NaCL; B) silicone 4011, approximately 20% Latanoprost, and approximately 10% NaCl; C) silicone 4011, approximately 10% Latanoprost, and approximately 10% NaCl; and D) silicone 6385, approximately 20% Latanoprost.
- FIG. 10A shows profiles of elution of Latanoprost form the cores for four formulations of Latanoprost, according to embodiments of the present invention.
- results show initial rates of approximately 300 ng per device per day that decreases to about 100 ng per device per day by 3 weeks (21 days).
- the results shown are for non-sterile drug cores. Similar results have been obtained with sterile drug cores of Latanoprost. These data are consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above
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Abstract
Description
- This application claims the benefit under 35 USC 119(e) of U.S. Provisional Application No. 60/787,775 filed on Mar. 31, 2006, and of U.S. Provisional Application No. 60/871,864, filed on Dec. 26, 2006, the full disclosures of which are incorporated herein by reference.
- The present application is related to implants for use in or near the nasolacrimal drainage system, with embodiments providing canalicular implants, lacrimal sac implants, punctal plugs and punctal plugs with drug delivery capabilities.
- A variety of challenges face patients and physicians in the area of ocular drug delivery. In particular, the repetitive nature of the therapies (multiple injections, instilling multiple eye drop regimens per day), the associated costs, and the lack of patient compliance may significantly impact the efficacy of the therapies available, leading to reduction in vision and many times blindness.
- Patient compliance in taking the medications, for example instilling the eye drops, can be erratic, and in some cases, patients may not follow the directed treatment regime. Lack of compliance can include, failure to instill the drops, ineffective technique (instilling less than required), excessive use of the drops (leading to systemic side effects), and use of non-prescribed drops or failure to follow the treatment regime requiring multiple types of drops. Many of the medications may require the patient to instill them up to 4 times a day.
- In addition to compliance, the cost of at least some eye drop medications is increasing, leading some patients on limited incomes to be faced with the choice of buying basic necessities or instead getting their prescriptions filled. Many times insurance does not cover the total cost of the prescribed eye drop medication, or in some cases eye drops containing multiple different medications.
- Further, in many cases, topically applied medications have a peak ocular effect within about two hours, after which additional applications of the medications should be performed to maintain the therapeutic benefit. In addition, inconsistency in self-administered or ingested medication regimes can result in a suboptimal therapy. PCT Publication WO 06/014434 (Lazar), which is incorporated herein by reference in its entirety, may be relevant to these and/or other issues associated with eye drops.
- One promising approach to ocular drug delivery is to place an implant that releases a drug in tissue near the eye. Although this approach can offer some improvement over eye drops, some potential problems of this approach may include implantation of the implant at the desire tissue location, retention of the implant at the desired tissue location, and sustaining release of the drug at the desired therapeutic level for an extended period of time. For example in the case of glaucoma treatment, undetected and premature loss of an implant can result in no drug being delivered, and the patient can potentially suffer a reduction in vision, possibly even blindness.
- In light of the above, it would be desirable to provide improved drug delivery implants that overcome at least some of the above mentioned shortcomings.
- The present invention provides implant devices, systems and methods for delivery of a therapeutic agent from a punctuin of a patient ocular tissues.
- In a first aspect, embodiments of the present invention provide an implant for insertion into a punctum of a patient. The punctum provides a flow path for a tear fluid from an eye to a canalicular lumen. The implant comprises a body. The body has a distal end, a proximal end, and an axis therebetween. The distal end of the body is insertable distally through the punctum into the canalicular lumen. The body comprises a therapeutic agent included within an agent matrix drug core. Exposure of the agent matrix to the tear fluid effects an effective therapeutic agent release into the tear fluid over a sustained period. The body has a sheath disposed over the agent matrix to inhibit release of the agent away from the proximal end. The body also has an outer surface configured to engage luminal wall tissues so as to inhibit expulsion when disposed therein.
- In some embodiments, the agent matrix comprises a non-bioabsorbable polymer, for example silicone in a non-homogenous mixture with the agent. The non-homogeneous mixture may comprise a silicone matrix saturated with the therapeutic agent and inclusions of the therapeutic agent.
- In many embodiments, the outer surface of the body can be disposed on the sheath, and the outer surface may define a body shape that inhibits expulsion of the body from the punctum. The body may further comprise a support structure over the agent matrix. The support structure may define the outer surface and be configured to inhibit expulsion of the body from the punctum. In specific embodiments, the support structure receives the sheath and agent matrix drug core therein, and inhibits inadvertent expulsion of the agent matrix in use. The support structure can comprise a helical coil. The support structure may have a receptacle therein, and the receptacle may fittingly receive the sheath and agent matrix therein so as to allow unrestricted fluid communication between the proximal end and the tear film in use. The outer surface may expand radially when released within the punctum, and the radial expansion may inhibits the expulsion from the punctum.
- In specific embodiments, the agent comprises a prostaglandin analogue, and the extended period comprises at least 3 months.
- In many embodiments, an implant for insertion into a patient is provided. The patient having path for tear fluid associated with an eye, and the implant comprises a body. The body can comprise a therapeutic agent and a support structure. The body can be configured to, when implanted at a target location along the tear fluid path, release a quantity of the therapeutic agent into the tear fluid each day for a sustained release period of days. The quantity can be significantly less than a recommended daily drop-administered quantity of the therapeutic agent. For example, the quantity can be less than 10% of the recommended drop-administered quantity. In specific embodiments, the quantity can be less than 5% of the recommended drop-administered quantity.
- In many embodiments, the period comprises at least three weeks and may comprise at least three months. The therapeutic agent may comprise Timolol maleate. The body may comprise in a range from about 270 μg to about 1350 μg of the therapeutic agent. The quantity released each day can be in a range from about 20 μg to about 135 μg.
- In many embodiments, the therapeutic agent may comprise a prostaglandin analogue, for example Latanoprost and/or Bimatoprost, and the body can comprise therapeutic agent in a range from about 3 μg to about 135 μg. The quantity can be in a range from about 5 ng to about 500 ng. In specific embodiments, the body may comprise therapeutic agent in a range from about 5 μg to about 30 μg, and the quantity can be in a range from about 10 ng to 150 ng.
- In another aspect, embodiments of the present invention provide a method of delivering a therapeutic agent to an eye having associated tear fluid. The method comprises placing a drug core in a canaliculus of the eye. The drug core comprises a matrix and inclusions of the therapeutic agent within the matrix. A portion of the drug core is exposed to the tear. The therapeutic agent is released to the tear of the eye. The therapeutic agent dissolves into the matrix such that the matrix remains substantially saturated with the therapeutic agent while the therapeutic agent is released through the exposed portion at therapeutic levels over a sustained period.
- In many embodiments, a rate of release is substantially determined by solubility of the agent in the core, the solubility of the agent in the tear and an area of the exposed portion. The drug can be released through the exposed portion at therapeutic levels for about 90 days. The therapeutic agent may comprise a prostaglandin analogue, and the inclusions of the therapeutic agent comprise an oil. The therapeutic agent can be encapsulated within the matrix, and the matrix may comprise a non-bioabsorbable polymer.
- In many embodiments, the therapeutic agent has a solubility in water of less than about 0.03% percent by weight. The therapeutic agent can be released at therapeutic levels in response to a surfactant of the tear. A sheath may be disposed over the core to define the exposed portion, and the exposed portion oriented toward the eye on a proximal end of the core.
- In many embodiments, a punctal plug to treat glaucoma is provided. The plug comprises a body no more than about 2.0 mm across. When inserted in the punctum for 35 days the body delivers at least a therapeutic quantity of therapeutic agent each day of the 35 days. In some embodiments, the body no more than about 2.0 mm across comprises a cross sectional size no more than about 1.0 mm across while inserted into the patient. In specific embodiments, the body comprises a drug core and the therapeutic agent is delivered from the drug core. The drug core may be no more than about 1 mm across, and the body may be no more than about 2 mm in length.
- In many embodiments, a method of treating glaucoma is provided with a punctal plug, The method comprises eluting at least 10 ng per day of a therapeutic agent from the punctal plug for at least 90 days. In specific embodiments, the therapeutic agent comprises at least one of Bimatoprost or Latanoprost. The therapeutic agent may have a solubility in water no more than about 0.03% by weight.
- In many embodiments, a punctal plug to treat glaucoma is provided, the plug comprises a body. The body comprises a therapeutic agent, and the body is adapted to release the therapeutic agent at therapeutic levels in response to a surfactant of the eye. In specific embodiments, the therapeutic agent has a solubility in water no more than about 0.03% by weight. The therapeutic agent may comprise cyclosporin.
- In many embodiments, a punctal plug to treat glaucoma is provided. The plug comprises a plug body. The body comprises a therapeutic agent. The body is adapted to release from about 80 to 120 ng of the therapeutic agent into a tear of the eye for at least about 20 days. In specific embodiments, the therapeutic agent may comprise at least one of Bimatoprost or Latanoprost.
- In some embodiments, a punctal plug to treat glaucoma is provided. The punctal plug comprises a body. The body comprises therapeutic agent stored within a volume no more than about 0.02 cm3. The body is adapted to deliver therapeutic levels of the therapeutic agent for at least about 1 month. In specific embodiments, the body is adapted to deliver the therapeutic agent at therapeutic levels for at least about 3 months. The body can be adapted to deliver the therapeutic agent with a substantially zero order release rate for the at least one month.
- In some embodiments, composition of matter to treat glaucoma of an eye having an associated tear is provided. The composition comprises inclusions. The inclusions comprise a concentrated form of a therapeutic agent. The therapeutic agent comprises a solubility in water no more than about 0.03% by weight. A silicone matrix encapsulates the inclusions. The therapeutic agent is soluble in the silicone matrix to release the therapeutic agent from the silicon matrix into the tear at therapeutic levels. In specific embodiments, the therapeutic agent inclusions are encapsulated within the silicon matrix comprise an inhomogeneous mixture of the inclusions encapsulated within the silicon matrix. The inclusions can comprise Latanoprost oil.
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FIGS. 1-1 and 1-2 show anatomical tissue structures of the eye suitable for use with implants, according to embodiments of the present invention; -
FIG. 1A shows a top cross sectional view of a sustained release implant to treat an optical defect of an eye, according to an embodiment of the present invention; -
FIG. 1B shows a side cross sectional view of the sustained release implant ofFIG. 1A ; -
FIG. 1C shows a perspective view of a sustained release implant with a coil retention structure, according to an embodiment of the present invention; -
FIG. 1D shows a perspective view of a sustained release implant with a retention structure comprising struts, according to an embodiment of the present invention; -
FIG. 1E shows a perspective view of a sustained release implant with a cage retention structure, according to an embodiment of the present invention; -
FIG. 1F shows a perspective view of a sustained release implant comprising a core and sheath, according to an embodiment of the present invention; -
FIG. 1G schematically illustrates a sustained release implant comprising a flow restricting retention element, a core and a sheath, according to an embodiment of the present invention; -
FIG. 2A shows a cross sectional view of a sustained release implant with core comprising an enlarged exposed surface area, according to an embodiment of the present invention; -
FIG. 2B shows a cross sectional view of a sustained release implant with a core comprising an enlarged exposed surface area, according to an embodiment of the present invention; -
FIGS. 2C and 2D show perspective view and cross sectional views, respectively, of a sustained release implant with a core comprising a reduced exposed surface area, according to an embodiment of the present invention: -
FIG. 2E shows a cross sectional view of a sustained release implant with a core comprising an enlarged exposed surface area with an indentation and castellation, according to an embodiment of the present invention; -
FIG. 2F shows a perspective view of a sustained release implant comprising a core with folds, according to an embodiment of the present invention; -
FIG. 2G shows a perspective view of a sustained release implant with a core comprising a channel with an internal porous surface, according to an embodiment of the present invention; -
FIG. 2H shows a perspective view of a sustained release implant with a core comprising porous channels to increase drug migration, according to an embodiment of the invention; -
FIG. 2I shows a perspective view of a sustained release implant with a convex exposed drug core surface, according to an embodiment of the present invention; -
FIG. 2J shows a side view of a sustained release implant with a core comprising an exposed surface area with several soft brush-like members extending therefrom, according to an embodiment of the present invention; -
FIG. 2K shows a side view of a sustained release implant with a drug core comprising a convex exposed surface and a retention structure, according to an embodiment of the present invention; -
FIG. 2L shows a side view of a sustained release implant with a drug core comprising a concave indented surface to increase exposed surface area of the core, according to an embodiment of the present invention; -
FIG. 2M shows a side view of a sustained release implant with a drug core comprising a concave surface with a channel formed therein to increase an exposed surface area of the core, according to an embodiment of the present invention; -
FIG. 3A shows an implant with a sheath body with extensions that attach the sheath body and core to the retention element, according to an embodiment of the present invention; -
FIG. 3B shows an implant with a retention element with an extension that retains a sheath body and a core, according to an embodiment of the present invention; -
FIGS. 4A and 4B show a cross-sectional view of an implant with a retention structure that is shorter in length while in a large cross-sectional profile configuration than a small cross-sectional profile configuration, according to an embodiment of the present invention; -
FIGS. 5A to 5C schematically illustrate replacement of a drug core and a sheath body, according to an embodiment of the present invention; -
FIGS. 6A to 6C show deployment of a sustained release implant, according to an embodiment of the present invention; and -
FIGS. 7A and 7B show elution data of Latanoprost atday 1 andday 14, respectively, for the three core diameters of 0.006, 0.012 and 0.025 inches and three Latanoprost concentrations of approximately 5%, 11% and 18%, according to embodiments of the present invention; -
FIG. 7C shows elution data for Latanoprost from 0.32 mm diameter, 0.95 mm long drug cores with concentrations of 5, 10 and 20% and drug weights of 3.5, 7 and 14 μg, respectively, according to embodiments of the present invention; -
FIGS. 7D and 7E show dependence of the rate of elution on exposed surface area of the drug core for the three core diameters and the three concentrations as inFIGS. 7A and 7B Latanoprost atday 1 andday 14, respectively, according to embodiments of the present invention; -
FIG. 8A shows elution profiles of cyclosporine from drug cores into a buffer solution with surfactant and a buffer solution with surfactant, according to embodiments of the present invention; -
FIG. 9A shows normalized elution profiles in nano-grams per device per day over 100 days for bulk sample of silicone with 1% Bimatoprost, according to embodiments of the present invention. -
FIG. 10A shows profiles of elution of Latanoprost from the cores for four formulations of Latanoprost according to embodiments of the present invention. -
FIGS. 1-1 and 1-2 show anatomical tissue structures of aneye 2 suitable for treatment with implants, according to an embodiment of the present invention.Eye 2 includes acornea 4 and aniris 6. Asclera 8 surroundscornea 4 andiris 6 and appears white. Aconjunctival layer 9 is substantially transparent and disposed oversclera 8. Acrystalline lens 5 is located within the eye. Aretina 7 is located near the back ofeye 2 and is generally sensitive to light.Retina 7 includes afovea 7F that provides high visual acuity and color vision.Cornea 4 andlens 5 refract light to form an image onfovea 7F andretina 7. The optical power ofcornea 4 andlens 5 contribute to the formation of images onfovea 7F andretina 7. The relative locations ofcornea 4,lens 5 andfovea 7F are also important to image quality. For example, if the axial length ofeye 2 fromcornea 4 toretina 7F is large,eye 2 can be myopic. Also, during accommodation,lens 5 moves towardcornea 4 to provide good near vision of objects proximal to the eye. - The anatomical tissue structures shown in
FIG. 1-1 also include the lacrimal system, which includes anupper canaliculus 10 and alower canaliculus 12, collectively the canaliculae, and the naso-lacrimal duct orsac 14. The upper and lower canaliculae terminate in anupper punctum 11 and alower punctum 13, also referred to as punctal apertures. The punctal apertures are situated on a slight elevation at the medial end of the lid margin at thejunction 15 of the ciliary and lacrimal portions near themedial canthus 17. The punctal apertures are round or slightly ovoid openings surrounded by a connective ring of tissue. Each of thepunctal openings vertical portion lacrimal sac 14. The canaliculae are tubular and lined by stratified squamous epithelium surrounded by elastic tissue which permits the canaliculus to be dilated. -
FIG. 1A shows a top cross sectional view of asustained release implant 100 to treat an optical defect of an eye, according to embodiments of the present invention.Implant 100 includes adrug core 110.Drug core 110 is an implantable structure that retains a therapeutic agent.Drug core 110 comprises amatrix 170 that containsinclusions 160 of therapeutic agent.Inclusions 160 will often comprise a concentrated form of the therapeutic agent, for example a crystalline form of the therapeutic agent, and the therapeutic agent may over time dissolve intomatrix 170 ofdrug core 110.Matrix 170 can comprise a silicone matrix or the like, and the mixture of therapeutic agent withinmatrix 170 can be non-homogeneous. In many embodiments, the non-homogenous mixture comprises a silicone matrix portion that is saturated with the therapeutic agent and an inclusions portion comprising inclusions of the therapeutic agent, such that the non-homogenous mixture comprises a multiphase non-homogenous mixture. In some embodiments,inclusions 160 comprise droplets of an oil of the therapeutic agent, for example Latanoprost oil. In some embodiments,inclusions 160 may comprise particles of the therapeutic agent, for example solid Bimatoprost particles in crystalline form. In many embodiments,matrix 170 encapsulatesinclusions 160, andinclusions 160 may comprise microparticles have dimensions from about 1 μm to about 100 μm. The encapsulated inclusions dissolve into the surrounding solid matrix, for example silicone, that encapsulates the micro particles such thatmatrix 170 is substantially saturated with the therapeutic agent while the therapeutic agent is released from the core. -
Drug core 110 is surrounded by asheath body 120.Sheath body 120 is can be substantially impermeable to the therapeutic agent, so that the therapeutic agent is often released from an exposed surface on an end ofdrug core 110 that is not covered withsheath body 120. Aretention structure 130 is connected todrug core 110 andsheath body 120.Retention structure 130 is shaped to retain the implant in a hollow tissue structure, for example, a punctum of a canaliculus as described above. - An
occlusive element 140 is disposed on and aroundretention structure 130.Occlusive element 140 is impermeable to tear flow and occludes the hollow tissue structure and may also serve to protect tissues of the tissue structure fromretention structure 130 by providing a more benign tissue-engaging surface.Sheath body 120 includes asheath body portion 150 that connects toretention structure 130 to retainsheath body 120 anddrug core 110.Sheath body portion 150 can include a stop to limit movement ofsheath body 120 anddrug core 110. In many embodiments,sheath body portion 150 can be formed with abulbous tip 150B.Bulbous tip 150B can comprise a convex rounded external portion that provides atraumatic entry upon introduction into the canaliculus. In many embodiments,sheath body portion 150B can be integral withocclusive element 140. -
FIG. 1B shows a side cross sectional view of the sustained release implant ofFIG. 1A .Drug core 110 is cylindrical and shown with a circular cross-section.Sheath body 120 comprises an annular portion disposed ondrug core 110.Retention structure 130 comprises several longitudinal struts 131. Longitudinal struts 131 are connected together near the ends of the retention structure. Although longitudinal struts are shown, circumferential struts can also be used.Occlusive element 140 is supported by and disposed over longitudinal struts 131 ofretention structure 130 and may comprise a radially expandable membrane or the like. -
FIG. 1C shows a perspective view of asustained release implant 102 with acoil retention structure 132, according to an embodiment of the present invention.Retention structure 132 comprises a coil and retains adrug core 112. A lumen, forexample channel 112C, may extend through thedrug core 112 to permit tear flow through the lumen for the delivery of therapeutic agent for nasal and systemic applications of the therapeutic agent. In addition or in combination withchannel 112C,retention structure 132 andcore 112 can be sized to permit tear flow around the drug core and sheath body while the retention element holds tissue of the canaliculus away from the drug core.Drug core 112 may be partially covered. The sheath body comprises afirst component 122A that covers a first end ofdrug cove 112 and asecond component 122B that covers a second end of the drug core. An occlusive element can be placed over the retention structure and/or the retention structure can be dip coated as described above. -
FIG. 1D shows a perspective view of asustained release implant 104 with aretention structure 134 comprising struts, according to an embodiment of the present invention.Retention structure 134 comprises longitudinal struts and retains adrug core 114.Drug core 114 is covered with asheath body 124 over most ofdrug core 114. The drug core releases therapeutic agent through an exposed end andsheath body 124 is annular over most of the drug core as described above. An occlusive element can be placed over the retention structure or the retention structure can be dip coated as described above. A protrusion that can be engaged with an instrument, for example a hook, a loop, a suture, orring 124R, can extend fromsheath body 124 to permit removal of the drug core and sheath body together so as to facilitate replacement of the sheath body and drug core while the retention structure remains implanted in the canaliculus. In some embodiments, a protrusion that can be engaged with an instrument comprising hook, a loop, a suture or a ring, can extend fromretention structure 134 to permit removal of the sustained release implant by removing the retention structure with the protrusion, drug core and sheath body. -
FIG. 1E shows a perspective view of asustained release implant 106 with acage retention structure 136, according to an embodiment of the present invention.Retention structure 136 comprises several connected strands of metal and retains adrug core 116.Drug core 116 is covered with asheath body 126 over most ofdrug core 116. The drug core releases therapeutic agent through an exposed end andsheath body 126 is annular over most of the drug core as described above. An occlusive element can be placed over the retention structure or the retention structure can be dip coated as described above. -
FIG. 1F shows a perspective view of a sustained release implant comprising a core and sheath, according to an embodiment of the present invention.Drug core 118 is covered with asheath body 128 over most ofdrug core 118. The drug core releases therapeutic agent through an exposed end andsheath body 128 is annular over most of the drug core as described above. - The rate of therapeutic agent release is controlled by the surface area of the exposed drug core and materials included within
drug core 118. In many embodiments, the rate of elution of the therapeutic agent is strongly and substantially related to the exposed surface area of the drug core and weakly dependent on the concentration of drug disposed in the inclusions in the drug core. - For circular exposed surfaces the rate of elution is strongly dependent on the diameter of the exposed surface, for example the diameter of an exposed drug core surface near an end of a cylindrical drug core. Such an implant can be implanted in ocular tissues, for example below
conjunctival tissue layer 9 of the eye and either abovesclera tissue layer 8, as shown inFIG. 1F , or only partially within the scleral tissue layer so as not to penetrate the scleral tissue. It should be noted thatdrug core 118 can be used with any of the retention structures and occlusive elements as described herein. - In an embodiment, the drug core is implanted between
sclera 8 andconjunctiva 9 withoutsheath body 128. In this embodiment without the sheath body, the physical characteristics of the drug core can be adjusted to compensate for the increased exposed surface of drug core, for example by reducing the concentration of dissolved therapeutic agent in the drug core matrix as described herein. -
FIG. 1G schematically illustrates asustained release implant 180 comprising a flow restrictingretention structure 186, acore 182 and asheath 184, according to an embodiment of the present invention.Sheath body 184 can at least partially coverdrug core 182.Drug core 182 may contain inclusions of the therapeutic agent therein to provide a sustained release of the therapeutic agent.Drug core 182 can include an exposedconvex surface area 182A. Exposedconvex surface area 182A may provide an increased surface area to release the therapeutic agent. - An
occlusive element 188 can be disposed overretention structure 186 to block the flow of tear through the canaliculus. In many embodiments,retention structure 186 can be located withinocclusive structure 188 to provide the occlusive element integrated with the retention structure. - Flow restricting
retention structure 186 andocclusive element 188 can be sized to block tear flow through the canaliculus. - The cores and sheath bodies described herein can be implanted in a variety of tissues in several ways. Many of the cores and sheaths described herein, in particular the structures described with reference to
FIGS. 2A to 2J can be implanted alone as punctal plugs. - Alternatively, many of the cores and sheath bodies described herein can comprise a drug core, sheath body, and/or the like so as to be implanted with the retention structures and occlusive elements described herein.
-
FIG. 2A shows a cross sectional view of asustained release implant 200 with core comprising an enlarged exposed surface area, according to an embodiment of the present invention. Adrug core 210 is covered with asheath body 220.Sheath body 220 includes anopening 220A.Opening 220 has a diameter that approximates the maximum cross sectional diameter ofdrug core 210.Drug core 210 includes an exposedsurface 210E, also referred to as an active surface. Exposedsurface 210E includes 3 surfaces: anannular surface 210A, acylindrical surface 210B and anend surface 210C.Annular surface 210A has an outer diameter that approximates the maximum cross sectional diameter ofcore 210 and an inner diameter that approximates the outer diameter ofcylindrical surface 210B.End surface 210C has a diameter that matches the diameter ofcylindrical surface 210B. The surface area of exposedsurface 210E is the sum of the areas ofannular surface 210A,cylindrical surface 210B andend surface 210C. - The surface area may be increased by the size of
cylindrical surface area 210B that extends longitudinally along an axis ofcore 210. -
FIG. 2B shows a cross sectional view of asustained release implant 202 with acore 212 comprising an enlarged exposedsurface area 212A, according to an embodiment of the present invention. Asheath body 222 extends overcore 212. The treatment agent can be released from the core as described above. Exposedsurface area 212A is approximately conical, can be ellipsoidal or spherical, and extends outward from the sheath body to increase the exposed surface area ofdrug core 212. -
FIGS. 2C and 2D show perspective and cross sectional views, respectively, of asustained release implant 204 with adrug core 214 comprising a reduced exposedsurface area 214A, according to an embodiment of the present invention.Drug core 214 is enclosed within asheath body 224. Sheath body 22 includes anannular end portion 224A that defines an opening through whichdrug core 214 extends.Drug core 214 includes an exposedsurface 214A that releases the therapeutic agent. Exposedsurface 214A has adiameter 214D that is less than a maximum dimension, for example a maximum diameter, acrossdrug core 214. -
FIG. 2E shows a cross sectional view of asustained release implant 206 with adrug core 216 comprising an enlarged exposedsurface area 216A with castellation extending therefrom, according to an embodiment of the present invention. The castellation includes several spaced apartfingers 216F to provide increased surface area of the exposedsurface 216A. - In addition to increased surface area provided by castellation,
drug core 216 may also include anindentation 2161.Indentation 2161 may have the shape of an inverted cone.Core 216 is covered with asheath body 226.Sheath body 226 is open on one end to provide an exposedsurface 216A ondrug core 216.Sheath body 226 also includes fingers and has a castellation pattern that matchescore 216. -
FIG. 2F shows a perspective view of asustained release implant 250 comprising a core with folds, according to an embodiment of the present invention.Implant 250 includes acore 260 and asheath body 270.Core 260 has an exposedsurface 260A on the end of the core that permits drug migration to the surrounding tear or tear film fluid.Core 260 also includesfolds 260F.Folds 260F increase the surface area of core that is exposed to the surrounding fluid tear or tear film fluid. With this increase in exposed surface area, folds 260F increase migration of the therapeutic agent fromcore 260 into the tear or tear film fluid and target treatment area. -
Folds 260F are formed so that achannel 260C is formed incore 260.Channel 260C connects to the end of the core to an opening in exposedsurface 260A and provides for the migration of treatment agent. Thus, the total exposed surface area ofcore 260 includes exposedsurface 260A that is directly exposed to the tear or tear film fluid and the surfaces offolds 260F that are exposed to the tear or tear film fluids via connection ofchannel 260C with exposedsurface 260A and the tear or tear film fluid. -
FIG. 2G shows a perspective view of a sustained release implant with a core comprising a channel with an internal porous surface, according to an embodiment of the present invention. -
Implant 252 includes acore 262 andsheath body 272.Core 262 has an exposedsurface 262A on the end of the core that permits drug migration to the surrounding tear or tear film fluid.Core 262 also includes achannel 262C.Channel 262C increases the surface area of the channel with a porous internal surface 262P formed on the inside of the channel against the core.Channel 262C extends to the end of the core near exposedsurface 262A of the core. The surface area of core that is exposed to the surrounding tear or tear film fluid can include the inside ofcore 262 that is exposed tochannel 262C. This increase in exposed surface area can increase migration of the therapeutic agent fromcore 262 into the tear or tear film fluid and target treatment area. Thus, the total exposed surface area ofcore 262 can include exposedsurface 260A that is directly exposed to the tear or tear film fluid and porous internal surface 262P that is exposed to the tear or tear film fluids via connection ofchannel 262C with exposedsurface 262A and the tear or tear film fluid. -
FIG. 2H shows a perspective view of asustained release implant 254 with acore 264 comprising channels to increase drug migration, according to an embodiment of the invention.Implant 254 includescore 264 andsheath body 274. Exposedsurface 264A is located on the end ofcore 264, although the exposed surface can be positioned at other locations. Exposedsurface 264A permits drug migration to the surrounding tear or tear film fluid.Core 264 also includeschannels 264C.Channels 264C extend to exposedsurface 264.Channels 264C are large enough that tear or tear film fluid can enter the channels and therefore increase the surface area ofcore 264 that is in contact with tear or tear film fluid. The surface area of the core that is exposed to the surrounding fluid tear or tear film fluid includes the inner surfaces 264P ofcore 262 that definechannels 264C. With this increase in exposed surface area,channels 264C increase migration of the therapeutic agent fromcore 264 into the tear or tear film fluid and target treatment area. Thus, the total exposed surface area ofcore 264 includes exposedsurface 264A that is directly exposed to the tear or tear film fluid and internal surface 264P that is exposed to the tear or tear film fluids via connection ofchannels 262C with exposedsurface 264A and the tear or tear film fluid. -
FIG. 2I shows a perspective view of asustained release implant 256 with adrug core 266 comprising a convex exposedsurface 266A, according to an embodiment of the present invention.Drug core 266 is partially covered with asheath body 276 that extends at least partially overdrug core 266 to define convex exposedsurface 266A.Sheath body 276 comprises ashaft portion 276S. Convex exposedsurface 266A provides an increased exposed surface area above the sheath body. A cross sectional area of convex exposedsurface 266A is larger than a cross sectional area ofshaft portion 276S ofsheath body 276. In addition to the larger cross sectional area, convex exposedsurface 266A has a larger surface area due to the convex shape which extends outward from the core.Sheath body 276 comprisesseveral fingers 276F that supportdrug core 266 in the sheath body and provide support to the drug core to holddrug core 266 in place insheath body 276.Fingers 276F are spaced apart to permit drug migration from the core to the tear or tear film fluid between the fingers.Protrusions 276P extend outward onsheath body 276.Protrusions 276P can be pressed inward to ejectdrug core 266 fromsheath body 276.Drug core 266 can be replaced with another drug core after an appropriate time, for example afterdrug core 266 has released most of the therapeutic agent. -
FIG. 2J shows a side view of asustained release implant 258 with acore 268 comprising an exposed surface area with several soft brush-like members 268F, according to an embodiment of the present invention.Drug core 268 is partially covered with asheath body 278 that extends at least partially overdrug core 268 to define exposedsurface 268A.Sheath body 278 comprises ashaft portion 278S. Soft brush-like members 268F extend outward fromdrug core 268 and provide an increased exposed surface area todrug core 268. Soft brush-like members 268F are also soft and resilient and easily deflected such that these members do not cause irritation to neighboring tissue. Althoughdrug core 268 can be made of many materials as explained above, silicone is a suitable material for the manufacture ofdrug core 268 comprises soft brush likemembers 268F. Exposedsurface 268A ofdrug core 268 also includes anindentation 2681 such that at least a portion of exposedsurface 268A is concave. -
FIG. 2K shows a side view of asustained release implant 259 with adrug core 269 comprising a convex exposedsurface 269A, according to an embodiment of the present invention.Drug core 269 is partially covered with asheath body 279 that extends at least partially overdrug core 269 to define convex exposedsurface 269A.Sheath body 279 comprises ashaft portion 279S. Convex exposedsurface 269 provides an increased exposed surface area above the sheath body. A cross sectional area of convex exposedsurface 269A is larger than a cross sectional area ofshaft portion 279S ofsheath body 279. In addition to the larger cross sectional area, convex exposedsurface 269A has a larger surface area due to the convex shape that extends outward on the core. Aretention structure 289 can be attached tosheath body 279.Retention structure 289 can comprise any of the retention structures as describe herein, for example a coil comprising a super elastic shape memory alloy such as Nitinol™.Retention structure 289 can be dip coated to makeretention structure 289 biocompatible. -
FIG. 2L shows a side view of asustained release implant 230 with adrug core 232 comprising a concaveindented surface 232A to increase exposed surface area of the core, according to an embodiment of the present invention. Asheath body 234 extends at least partially overdrug core 232. Concaveindented surface 232A is formed on an exposed end ofdrug core 232 to provide an increased exposed surface area of the drug core. -
FIG. 2M shows a side view of asustained release implant 240 with adrug core 242 comprising aconcave surface 242A with achannel 242C formed therein to increase an exposed surface area of the core, according to an embodiment of the present invention. Asheath body 244 extends at least partially overdrug core 242. Concaveindented surface 242A is formed on an exposed end ofdrug core 232 to provide an increased exposed surface area of the drug core.Channel 242C formed indrug core 242 to provide an increased exposed surface area of the drug core.Channel 242C can extend to concaveindented surface 242A such thatchannel 242C and provide an increase in surface area of the core exposed to the tear or tear film film. -
FIG. 3A shows animplant 310 comprising asheath body 320 withextensions 322, according to an embodiment of the present invention.Extensions 322 attachsheath body 320 to the retention element to retain the core near the punctum.Sheath body 320 extends overcore 330 to define an exposedsurface 332 ofcore 330.Extensions 322 can be resilient and engage the retention element and/or occlusive element to attach the sheath body core to the retention element to retain the core near the punctum. -
FIG. 3B shows animplant 350 comprising aretention element 380 with anextension 382, according to an embodiment of the present invention.Extension 382 retains asheath body 360 and acore 370.Sheath body 360 extends overcore 370 to define an exposedsurface 372 ofcore 370. Exposedsurface 372 is disposed near the proximal end ofcore 370.Extension 382 extends downward to retaincore 370 andsheath body 370. -
FIGS. 4A and 4B show a cross-sectional view of animplant 400 with aretention structure 430 that is shorter in length while in a large cross-sectional profile configuration than a small cross-sectional profile configuration, according to an embodiment of the present invention.Implant 400 includes adistal end 402 and aproximal end 404.Implant 400 includes adrug core 410 and asheath body 420.Sheath body 420 at least partially coversdrug core 410 and defines an exposedsurface 412 ofdrug core 410. Anocclusive element 440 can be attached to and supported byretention structure 430.Occlusive element 440 can move withretention structure 430, for example whenretention element 430 expands from a small profile configuration to a large profile configuration. In many embodiments, the retention structure and occlusive element are sized to correspond to a diameter of the canaliculus, for example to match a diameter of the canaliculus or slightly larger than the canalicular diameter, so as occlude fluid flow through the canaliculus and/or anchor in the canaliculus. - As shown in
FIG. 4A ,retention structure 430 andocclusive element 440 are in a small profile configuration. Such a small profile configuration can occur while the occlusive element and retention structure are placed in a tip of an insertion tool and covered for deployment.Retention element 430 andocclusive element 440 extend fully along the length ofsheath body 420 anddrug core 410.Retention element 430 is attached tosheath body 420 neardistal end 402. In many embodiments,retention structure 430 andocclusive element 440 have diameters that are sized to fit inside and slide within the canaliculus while in the small profile configuration, and the retention structure and occlusive element can be sized to anchor within the canaliculus while in a second large profile configuration. - As shown in
FIG. 4B ,retention structure 430 andocclusive element 440 are in a large profile configuration. Such a large profile configuration can occur when the occlusive element and retention structure are placed in the canaliculus. In the large profile configuration, the length ofocclusive element 440 andretention structure 430 is shorter than in the small profile configuration by adistance 450. The proximal end ofretention structure 430 andocclusive element 440 can slide oversheath body 420 when the sheath body and retention structure assume the large profile configuration such that the proximal end ofdrug core 410 andsheath body 420 extend from the retention structure and occlusive element. In some embodiments, the sheath body is shorter thandrug core 410 bydistance 450 so that more of the drug core is exposed while the retention structure and occlusive element are in the large profile configuration than is exposed while the retention structure and occlusive element are in the small profile configuration. In such embodiments, the retention structure and occlusive element retract to expose the drug core. -
FIGS. 5A to 6 show embodiments of tools that can be used to insert many of the implants as describe herein. -
FIG. 5A shows aninsertion tool 500 to insert an implant into the punctum with aplunger 530 that can be depressed, according to an embodiment of the present invention.Insertion tool 500 includes adilator 510 that can be inserted into the punctum to pre-dilate the punctum prior to insertion of an implant. Animplant 520 can be pre-loaded ontotool 500 prior to dilation of the punctum. An internal wire 540 can be connected to implant 520 to retain the implant. Following pre-dilation of the punctum withdilator 510,tool 500 can be used to insertimplant 520 into the punctum. Whileimplant 520 is positioned in the punctum,plunger 530 can be depressed to engage wire 540 andrelease implant 520 fromtool 500. -
FIG. 5B shows an insertion tool 550 to insert animplant 570 into the punctum with a plunger that can slide, according to an embodiment of the present invention. Insertion tool 550 includes adilator 560 with a conical section to dilate the punctum. Implant 550 includes a plunger 580 that can slide distally to advanceimplant 570 into the lumen. Ashaft 590 is connected to plunger 580 to advanceimplant 570 distally when plunger 580 is advanced distally. While the punctum is dilated withdilator 560, plunger 580 can be advanced distally to placeimplant 570 in the canalicular lumen near the punctum. In many embodiments, a button can be depressed to advance distally the implant into the lumen, for example a button connected toshaft 590 with an intermediate mechanism. -
FIG. 6 shows aninsertion tool 600 to insert an implant into the punctum with asheath 610 that retracts to position the implant in the canalicular lumen, according to an embodiment of the present invention. At least a portion ofsheath 610 is shaped to dilate the punctum.Sheath 610 is shaped to hold animplant 620 in a small profile configuration.Insertion tool 600 includes an annular structure 615, which can comprise a portion of a body 605 ofinsertion tool 600.Sheath 610 and annular structure 615 are shaped to dilate the punctum and often comprise proximally inclined surfaces to dilate the punctum.Implant 620,sheath 610 and annular structure 615 can be at least partially inserted into the punctum to place the implant in the canalicular lumen. Annular structure 615 is disposed oversheath 610 so thatsheath 610 can be retracted and slide under annular structure 615. A stop 625 can be connected to body 605 to retainimplant 620 at the desired depth within the canalicular lumen whilesheath 610 is retracted proximally to exposeimplant 620. - Once
implant 620 has been positioned in the canalicular lumen at the desired depth in relation to the punctum,sheath 610 is retracted to exposeimplant 620 at the desired location in the canalicular lumen. Aplunger 630 can be used to retractsheath 610. Ashaft 640 mechanically couplessheath 610 toplunger 630. Thus, retraction ofplunger 630 in the proximal direction can retractsheath 610 in the proximal direction to exposeimplant 620 at the desired location in the canalicular lumen.Implant 620 can be any of the implants as described herein. Often,implant 620 will comprise a resilient member that expands to a large profile configuration whensheath 610 is retracted. In many embodiments,insertion tool 600 can include a dilator to dilate the punctum prior to insertion of the implant, and the dilator can be positioned on an end of the insertion tool that opposes the end loaded with the implant, as described herein above. -
FIGS. 5A to 5C schematically illustrate replacement of adrug core 510 and asheath body 520, according to an embodiment of the present invention. An implant 700 comprisesdrug core 510,sheath body 520 and aretention structure 530.Implant 500 can include an occlusive element support by and movable withretention structure 530. Oftenretention structure 530 can assume a first small profile configuration prior to implantation and a second large profile configuration while implanted.Retention structure 530 is shown in the large profile configuration and implanted in the canalicular lumen.Sheath body 520 includesextension 525A andextension 525B to attach the sheath body and drug core toretention structure 530 so that the sheath body and drug core are retained byretention structure 530.Drug core 510 andsheath body 520 can be removed together by drawingdrug core 510 proximally as shown byarrow 530.Retention structure 530 can remain implanted in the canalicular tissue afterdrug core 510 andsheath body 520 have been removed as shown inFIG. 5B . Areplacement core 560 andreplacement sheath body 570 can be inserted together as shown inFIG. 5C . Such replacement can be desirable afterdrug core 510 has released effective amounts of therapeutic agent such that the supply of therapeutic agent in the drug core has diminished and the rate of therapeutic agent released is near the minimum effective level.Replacement sheath body 570 includes extension 575A andextension 575B.Replacement drug core 560 andreplacement sheath body 570 can be advanced distally as shown byarrow 590 to insertreplacement drug core 560 andreplacement sheath body 570 intoretention structure 530.Retention structure 530 remains at substantially the same location whilereplacement drug core 560 andreplacement sheath body 570 are inserted intoresilient member 530. -
FIGS. 6A to 6C show deployment of a sustained release implant, according to an embodiment of the present invention. As shown inFIG. 6A , adeployment instrument 610 is inserted into acanaliculus 600 through apunctum 600A. Asustained release implant 620 is loaded into a tip ofdeployment instrument 610, and asheath 612 covers sustainedrelease implant 620.Retention structure 630 assumes a small profile configuration whilesheath 612 is positioned overretention structure 630. As shown inFIG. 6B ,outer sheath 612 ofdeployment instrument 610 is withdrawn to expose aretention structure 630 ofsustained release implant 620. The exposed portion ofretention element 630 assumes a large profile configuration. As shown inFIG. 6C ,deployment instrument 610 has been removed andsustained release implant 620 is implanted incanaliculus 600. Adrug core 640 is attachedretention structure 630 and retained in the canaliculus. Anouter body sheath 650 covers at least a portion ofdrug core 640 anddrug core 640 releases a therapeutic agent into a liquid tear or tearfilm 660 nearpunctum 600A ofcanaliculus 600. - Sheath Body
- The sheath body comprises appropriate shapes and materials to control migration of the therapeutic agent from the drug core. The sheath body houses the core and can fit snugly against the core. The sheath body is made from a material that is substantially impermeable to the therapeutic agent so that the rate of migration of the therapeutic agent may be largely controlled by the exposed surface area of the drug core that is not covered by the sheath body. In many embodiments, migration of the therapeutic agent through the sheath body can be about one tenth of the migration of the therapeutic agent through the exposed surface of the drug core, or less, often being one hundredth or less. In other words, the migration of the therapeutic agent through the sheath body is at least about an order of magnitude less that the migration of the therapeutic agent through the exposed surface of the drug core. Suitable sheath body materials include polyimide, polyethylene terephthalate” (hereinafter “PET”). The sheath body has a thickness, as defined from the sheath surface adjacent the core to the opposing sheath surface away from the core, from about 0.00025″ to about 0.0015″. The total diameter of the sheath that extends across the core ranges from about 0.2 mm to about 1.2 mm. The core may be formed by dip coating the core in the sheath material. Alternatively or in combination, the sheath body can comprise a tube and the core introduced into the sheath, for example as a liquid or solid that can be slid, injected and/or extruded into the sheath body tube. The sheath body can also be dip coated around the core, for example dip coated around a pre-formed core.
- The sheath body can be provided with additional features to facilitate clinical use of the implant. For example, the sheath may receive a drug core that is exchangeable while the retention structure and sheath body remain implanted in the patient. The sheath body is often rigidly attached to the retention structure as described above, and the core is exchangeable while the retention structure retains the sheath body. In specific embodiments, the sheath body can be provided with external protrusions that apply force to the sheath body when squeezed and eject the core from the sheath body. Another drug core can then be positioned in the sheath body. In many embodiments, the sheath body and/or retention structure may have a distinguishing feature, for example a distinguishing color, to show placement such that the placement of the sheath body and/or retention structure in the canaliculus or other body tissue structure can be readily detected by the patient. The retention element and/or sheath body may comprise at least one mark to indicate the depth of placement in the canaliculus such that the retention element and/or sheath body can be positioned to a desired depth in the canaliculus based on the at least one mark.
- Retention Structure
- The retention structure comprises an appropriate material that is sized and shaped so that the implant can be easily positioned in the desired tissue location, for example the canaliculus. The retention structure is mechanically deployable and typically expands to a desired cross sectional shape, for example with the retention structure comprising a super elastic shape memory alloy such as Nitinol™. Other materials in addition to Nitinol™ can be used, for example resilient metals or polymers, plastically deformable metals or polymers, shape memory polymers, and the like, to provide the desired expansion. In some embodiments polymers and coated fibers available from Biogeneral, Inc. of San Diego, Calif. may be used. Many metals such as stainless steels and non-shape memory alloys can be used and provide the desired expansion. This expansion capability permits the implant to fit in hollow tissue structures of varying sizes, for example canaliculac ranging from 0.3 mm to 1.2 mm (i.e. one size fits all).
- Although a single retention structure can be made to fit canaliculae from 0.3 to 1.2 mm across, a plurality of alternatively selectable retention structures can be used to fit this range if desired, for example a first retention structure for canaliculae from 0.3 to about 0.9 mm and a second retention structure for canaliculae from about 0.9 to 1.2 mm. The retention structure has a length appropriate to the anatomical structure to which the retention structure attaches, for example a length of about 3 mm for a retention structure positioned near the punctum of the canaliculus. For different anatomical structures, the length can be appropriate to provide adequate retention force, e.g. 1 mm to 15 mm lengths as appropriate.
- Although the sheath body and drug core are attached to one end of the retention structure as described above, in many embodiments the other end of retention structure is not attached to drug core and sheath body so that the retention structure can slide over the sheath body and drug core while the retention structure expands. This sliding capability on one end is desirable as the retention structure may shrink in length as the retention structure expands in width to assume the desired cross sectional width. However, it should be noted that many embodiments may employ a sheath body that does not slide in relative to the core.
- In many embodiments, the retention structure can be retrieved from tissue. A protrusion, for example a hook, a loop, or a ring, can extend from the retention structure to facilitate removal of the retention structure.
- Occlusive Element
- The occlusive element comprises an appropriate material that is sized and shaped so that the implant can at least partially inhibit, even block, the flow of fluid through the hollow tissue structure, for example lacrimal fluid through the canaliculus. The occlusive material shown is a thin walled membrane of a biocompatible material, for example silicone, that can expand and contract with the retention structure. The occlusive element is formed as a separate thin tube of material that is slid over the end of the retention structure and anchored to one end of the retention structure as described above. Alternatively, the occlusive element can be formed by dip coating the retention structure in a biocompatible polymer, for example silicone polymer. The thickness of the occlusive element can be in a range from about 0.01 mm to about 0.15 mm, and often from about 0.05 mm to 0.1 mm.
- Therapeutic Agents
- A “therapeutic agent” can comprise a drug may be any of the following or their equivalents, derivatives or analogs, including, anti-glaucoma medications, (e.g. adrenergic agonists, adrenergic antagonists (beta blockers), carbonic anhydrase inhibitors (CAIs, systemic and topical), parasympathomimetics, prostaglandins and hypotensive lipids, and combinations thereof), antimicrobial agent (e.g., antibiotic, antiviral, antiparacytic, antifungal, etc.), a coiticosteroid or other anti-inflammatory (e.g., an NSAID), a decongestant (e.g., vasoconstrictor), an agent that prevents of modifies an allergic response (e.g., an antihistamine, cytokine inhibitor, leucotriene inhibitor, IgE inhibitor, immunomodulator), a mast cell stabilizer, cycloplegic or the like. Examples of conditions that may be treated with the therapeutic agent(s) include but are not limited to glaucoma, pre and post surgical treatments, dry eye and allergies. In some embodiments, the therapeutic agent may be a lubricant or a surfactant, for example a lubricant to treat dry eye.
- Exemplary therapeutic agents include, but are not limited to, thrombin inhibitors; antithrombogenic agents; thrombolytic agents; fibrinolytic agents; vasospasm inhibitors; vasodilators; antihypertensive agents; antimicrobial agents, such as antibiotics (such as tetracycline, chlortetracycline, bacitracin, neomycin, polymyxin, gramicidin, cephalexin, oxytetracycline, chloramphenicol, rifampicin, ciprofloxacin, tobramycin, gentamycin, erythromycin, penicillin, sulfonamides, sulfadiazine, sulfacetamide, sulfamethizole, sulfisoxazole, nitrofurazone, sodium propionate), antifungals (such as amphotericin B and miconazole), and antivirals (such as idoxuridine trifluorothymidine, acyclovir, gancyclovir, interferon); inhibitors of surface glycoprotein receptors; antiplatelet agents; antimitotics; microtubule inhibitors; anti-secretory agents; active inhibitors; remodeling inhibitors; antisense nucleotides; anti-metabolites; antiproliferatives (including antiangiogenesis agents); anticancer chemotherapeutic agents; anti-inflaTnmatories (such as hydrocortisone, hydrocortisone acetate, dexamethasone 21-phosphate, fluocinolone, medrysone, methylprednisolone, prednisolone 21-phosphate, prednisolone acetate, fluoromethalone, betamethasone, triamcinolone, triamcinolone acetonide); non steroidal anti-inflammatories (NSAIDs) (such as salicylate, indomethacin, ibuprofen, diclofenac, flurbiprofen, piroxicam indomethacin, ibuprofen, naxopren, piroxicam and nabumetone). Such anti inflammatory steroids contemplated for use in the methodology of the present invention, include triamcinolone acetonide (generic name) and corticosteroids that include, for example, triamcinolone, dexamethasone, fluocinolone, cortisone, prednisolone, flumetholone, and derivatives thereof.); antiallergenics (such as sodium chromoglycate, antazoline, methapyriline, chlorpheniramine, cetrizine, pyrilamine, prophenpyridamine); anti proliferative agents (such as 1,3-cis retinoic acid, 5-fluorouracil, taxol, rapamycin, mitomycin C and cisplatin); decongestants (such as phenylephrine, naphazoline, tetrahydrazoline); miotics and anti-cholinesterase (such as pilocarpine, salicylate, carbachol, acetylcholine chloride, physostigmine, eserine, diisopropyl fluorophosphate, phospholine iodine, demecarium bromide); antineoplastics (such as carmustine, cisplatin, fluorouracil3; immunological drugs (such as vaccines and immune stimulants); hormonal agents (such as estrogens, —estradiol, progestational, progesterone, insulin, calcitonin, parathyroid hormone, peptide and vasopressin hypothalamus releasing factor); immunosuppressive agents, growth hormone antagonists, growth factors (such as epidermal growth factor, fibroblast growth factor, platelet derived growth factor, transforming growth factor beta, somatotrapin, fibronectin); inhibitors of angiogenesis (such as angiostatin, anecortave acetate, thrombospondin, anti-VEGF antibody); dopamine agonists; radiotherapeutic agents; peptides; proteins; enzymes; extracellular matrix; components; ACE inhibitors; free radical scavengers; chelators; antioxidants; anti polymerases; photodynamic therapy agents; gene therapy agents; and other therapeutic agents such as prostaglandins, antiprostaglandins, prostaglandin precursors, including antiglaucoma drugs including beta-blockers such as Timolol, betaxolol, levobunolol, atenolol, and prostaglandin analogues such as Bimatoprost, travoprost, Latanoprost etc; carbonic anhydrase inhibitors such as acetazolamide, dorzolamide, brinzolamide, methazolamide, dichlorphenamide, diamox; and neuroprotectants such as lubezole, nimodipine and related compounds; and parasympathomimetrics such as pilocarpine, carbachol, physostigmine and the like.
- The amount of drug associated with the drug-delivery device may vary depending on the particular agent, the desired therapeutic benefit and the time during which the device is intended to deliver the therapy. Since the devices of the present invention present a variety of shapes, sizes and delivery mechanisms, the amount of drug associated with the device will depend on the particular disease or condition to be treated, and the dosage and duration that is desired to achieve the therapeutic effect. Generally, the amount of drug is at least the amount of drug that upon release from the device, is effective to achieve the desired physiological or pharmacological local or systemic effects.
- Embodiments of the drug delivery devices of the present invention can be adapted to provide delivery of drug at a daily rate that is substantially below the therapeutically effective drop form of treatment so as to provide a large therapeutic range with a wide safety margin. For example, many embodiments treat the eye with therapeutic levels for extended periods that are no more than 5 or 10 percent of the daily drop dosage. Consequently, during an initial bolus or washout period of about one to three days, the implant can elute the therapeutic agent at a rate that is substantially higher than the sustained release levels and well below the daily drop form dosage. For example, with an average sustained release level of 100 ng per day, and an initial release rate of 1000 to 1500 ng per day, the amount of drug initially released is less than the 2500 ng of drug that may be present in a drop of drug delivered to the eye. This used use of sustained release levels substantially below the amount of drug in a drop and/or drops administered daily allows the device to release a therapeutically beneficial amount of drug to achieve the desired therapeutic benefit with a wide safety margin, while avoiding an inadequate or excessive amount of drug at the intended site or region.
- An extended period of time may mean a relatively short period of time, for example minutes or hours (such as with the use of an anesthetic), through days or weeks (such as the use of pre-surgical or post-surgical antibiotics, steroids, or NSAIDs and the like), or longer (such as in the case of glaucoma treatments), for example months or years (on a recurring basis of use of the device).
- For example, a drug such as Timolol maleate, a beta1 and beta2 (non-selective) adrenergic receptor blocking agent can be used in the device for a release over an extended period of time such as 3 months. Three months is a relatively typical elapsed time between physician visits for a glaucoma patient undergoing topical drop therapy with a glaucoma drug, although the device could provide treatment for longer or shorter durations. In the three month example, a 0.25% concentration of Timolol translates to from 2.5 to 5 mg/1000 μL, typically being 2.5 mg/l 000 μL. A drop of Timolol for topical application is usually in the range of 40-60 μL, typically being 50 μL. Thus, there may be 0.08-0.15 mg, typically being 0.125 mg of Timolol in a drop. There may be approximately 8% (optionally 6-10%) of the drop left in the eye after 5 minutes, so about 10 μg of the drug is available at that time. Timolol may have a bioavailability of 30-50%, which means that from 1.5 to 7.5 μg, for example 4 μg of the drug is available to the eye. Timolol is generally applied twice a day, so 8 (or 3-15) μg is available to the eye each day. Therefore, a delivery device might contain from 270 to 1350 μg, for example 720 μg, of the drug for a 90 day, or 3 month, extended release. The drug would be contained within the device and eluted based on the polymer or drug/hydrogel concentration. The drug can be similarly contained on the device and eluted for olopatadine hydrochloride (Patanol®) and other drugs in a manner similar to Timolol.
- Commercially available solutions of Timolol maleate are available in 0.25% and 0.5% preparations, and the initial dosage can be 1 drop twice per day of 0.25% solution. A 0.25% concentration of Timolol is equivalent to 2.5 mg per 1000 μl. A sustained release quantity of Timolol released each day from the drug core can be from about 3 to 15 μg each day. Although the sustained release quantity delivered each day from the device may vary, a sustained release delivery of about 8 μg per day corresponds to about 3.2% of the 0.250 mg of Timolol applied with two drops of a 0.25% solution.
- For example, in the case of Latanoprost (Xalatan), a prostaglandin F2α analogue, this glaucoma medication has concentrations that are about 1/10th that of Timolol. Therefore, the amount of drug on the implantable device, depending on the bioavailability, would be significantly less—approximately 20-135 μg and typically 50-100 μg—for Latanoprost and other prostaglandin analogues. This also translates to a device that can either be smaller than one required for a beta blocker delivery or can house more drug for a longer release period.
- A drop of Xalatan contains about 2.5 μg of Latanoprost, assuming a 50 μL drop volume. Therefore, assuming that about 8% of 2.5 μg is present 5 minutes after instillation, only about 200 ng of drug remains on the eye. Based on the Latanoprost clinical trials, this amount is effective in lowering IOP for at least 24 hours. Pfizer/Pharmacia conducted several dose-response studies in support of the NDA for Xalatan. The doses ranged from 12.5 μg/mL to 115 μg/mL of Latanoprost. The current dose of Latanoprost, 50 μg/mL, given once per day, was shown to be optimal. However, even the lowest doses of 12.5 μg/mL QD or 15 μg/mL BID consistently gave about 60-75% of the IOP reduction of the 50 μg/mL QD dose. Based on the assumptions above, a 12.5 μg/mL concentration provides 0.625 μg of Latanoprost in a 50 μL drop, which results in only about 50 ng (8%) of drug remaining in the eye after 5 minutes.
- In many embodiments, the concentrations of Latanoprost are about 1/100th, or 1 percent, that of Timolol, and in specific embodiments the concentrations of Latanoprost may be about 1/50th, or 2 percent, that of Timolol. For example, commercially available solution preparations of Latanoprost are available at concentrations 0.005%, often delivered with one drop per day. In many embodiments, the therapeutically effective concentration of drug released from the device per day can be about 1/100th of Timolol, about 30 to 150 ng per day, for example about 80 ng, assuming tear washout and bioavailability similar to Timolol. For example, the amount of drug on the implantable device, can be significantly less—approximately 1% to 2% of Timolol, for example 2.7 to 13.5 μg, and can also be about 3 to 20 μg, for Latanoprost and other prostaglandin analogues. Although the sustained release amount of Latanoprost released each day can vary, a sustained release of 80 ng per day corresponds to about 3.2% of the 2.5 μg of Latanoprost applied with a single drop of a 0.005% solution
- For example, in the case of Bimatoprost (Lumigan), a synthetic prostamide prostaglandin analogue, this glaucoma medication may have concentrations that are 1/20th or less than that of Timolol. Therefore, the amount of drug loaded on the extended release device for a 3 to 6 month extended release, depending on the bioavailability, can be significantly less, approximately 5-30 μg and typically 10-20 μg—for Bimatoprost and analogues and derivatives thereof. In many embodiments, the implant can house more drug for a longer sustained release period, for example 20-40 μg for a sustained release period of 6 to 12 months with Bimatoprost and its derivatives. This decrease in drug concentration can also translate to a device that can be smaller than one required for a beta blocker delivery.
- Commercially available solution concentrations of Bimatoprost are 0.03% by weight, often delivered once per day. Although the sustained release amount of Bimatoprost released each day can vary, a sustained release of 300 ng per day corresponds to about 2% of the 15 μg of Bimatoprost applied with a single drop of a 0.03% solution. Work in relation with the present invention suggests that even lower sustained release doses of Bimatoprost can provide at least some reduction in intraocular pressure, for example 20 to 200 ng of Bimatoprost and daily sustained release dosages of 0.2 to 2% of the daily drop dosage.
- For example, in the case of Travoprost (Travatan), a prostaglandin F2α analogue, this glaucoma medication may have concentrations that are 2% or less than that of Timolol. For example, commercially available solution concentrations are 0.004%, often delivered once per day. In many embodiments, the therapeutically effective concentration of drug released from the device per day can be about 65 ng, assuming tear washout and bioavailability similar to Timolol. Therefore, the amount of drug on the implantable device, depending on the bioavailability, would be significantly less. This also translates to a device that can either be smaller than one required for a beta blocker delivery or can house more drug for a longer release period. For example, the amount of drug on the implantable device, can be significantly less—approximately 1/100 of Timolol, for example 2.7 to 13.5 μg, and typically about 3 to 20 μg, for Travoprost, Latanoprost and other prostaglandin F2α analogues. Although the sustained release amount of Latanoprost released each day can vary, a sustained release of 65 ng per day corresponds to about 3.2% of the 2.0 μg of Travoprost applied with a single drop of a 0.004% solution.
- In some embodiments, the therapeutic agent may comprise a cortico steriod, for example fluocinolone acetonide, to treat a target ocular tissue. In specific embodiments, fluocinolone acetonide can be released from the canaliculus and delivered to the retina as a treatment for diabetic macular edema (DME).
- It is also within the scope of this invention to modify or adapt the devices to deliver a high release rate, a low release rate, a bolus release, a burst release, or combinations thereof. A bolus of the drug may be released by the formation of an erodable polymer cap that is immediately dissolved in the tear or tear film. As the polymer cap comes in contact with the tear or tear film, the solubility properties of the polymer enable the cap to erode and the drug is released all at once. A burst release of a drug can be performed using a polymer that also erodes in the tear or tear film based on the polymer solubility. In this example, the drug and polymer may be stratified along the length of the device so that as the outer polymer layer dissolves, the drug is immediately released. A high or low release rate of the drug could be accomplished by changing the solubility of the erodable polymer layer so that the drug layer released quickly or slowly. Other methods to release the drug could be achieved through porous membranes, soluble gels (such as those in typical ophthalmic solutions), microparticle encapsulations of the drug, or nanoparticle encapsulation, depending on the size of the drug molecule.
- Drug Core
- The drug core comprises the therapeutic agent and materials to provide sustained release of the therapeutic agent. The therapeutic agent migrates from the drug core to the target tissue, for example ciliary muscles of the eye. The therapeutic agent may optionally be only slightly soluble in the matrix so that a small amount of therapeutic agent is dissolved in the matrix and available for release from the surface of
drug core 110. As the therapeutic agent diffuses from the exposed surface of the core to the tear or tear film, the rate of migration from the core to the tear or tear film can be related to the concentration of therapeutic agent dissolved in the matrix. In addition or in combination, the rate of migration of therapeutic agent from the core to the tear or tear film can be related to properties of the matrix in which the therapeutic agent dissolves. In specific embodiments, the rate of migration from the drug core to the tear or tear film can be based on a silicone formulation. In some embodiments, the concentration of therapeutic agent dissolved in the drug core may be controlled to provide the desired rate of release of the therapeutic agent. The therapeutic agent included in the core can include liquid, solid, solid gel, solid crystalline, solid amorphous, solid particulate, and/or dissolved forms of the therapeutic agent. In a preferred embodiment, the drug core comprises a silicone matrix containing the therapeutic agent. The therapeutic agent may comprise liquid or solid inclusions, for example liquid Latanoprost droplets or solid Bimatoprost particles, respectively, dispersed in the silicone matrix. - The drug core can comprise one or more biocompatible materials capable of providing a sustained release of the therapeutic agent. Although the drug core is described above with respect to an embodiment comprising a matrix with a substantially non-biodegradable silicone matrix with inclusions of the drug located therein that dissolve, the drug core can include structures that provide sustained release of the therapeutic agent, for example a biodegradable matrix, a porous drug core, liquid drug cores and solid drug cores. A matrix that contains the therapeutic agent can be formed from either biodegradable or non-biodegradable polymers. A non-biodegradable drug core can include silicone, acrylates, polyethylenes, polyurethane, polyurethane, hydrogel, polyester (e.g., DACRON® from E. I. Du Pont de Nemours and Company, Wilmington, Del.), polypropylene, polytetrafluoroethylene (PTFE), expanded PTFE (ePTFE), polyether ether ketone (PEEK), nylon, extruded collagen, polymer foam, silicone rubber, polyethylene terephthalate, ultra high molecular weight polyethylene, polycarbonate urethane, polyurethane, polyimides, stainless steel, nickel-titanium alloy (e.g., Nitinol), titanium, stainless steel, cobalt-chrome alloy (e.g., ELGILOY® from Elgin Specialty Metals, Elgin, Ill.; CONICHROME® from Carpenter Metals Corp., Wyomissing, Pa.). A biodegradable drug core can comprise one or more biodegradable polymers, such as protein, hydrogel, polyglycolic acid (PGA), polylactic acid (PLA), poly(L-lactic acid) (PLLA), poly(L-glycolic acid) (PLGA), polyglycolide, poly-L-lactide, poly-D-lactide, poly(amino acids), polydioxanone, polycaprolactone, polygluconate, polylactic acid-polyethylene oxide copolymers, modified cellulose, collagen, polyorthoesters, polyhydroxybutyrate, polyanhydride, polyphosphoester, poly(alpha-hydroxy acid) and combinations thereof. In some embodiments the drug core can comprise at least one of hydrogel polymer.
- Release of Therapeutic Agent at Effective Levels
- The rate of release of the therapeutic agent can be related to the concentration of therapeutic agent dissolved in the drug core. In many embodiments, the drug core comprises non-therapeutic agents that are selected to provide a desired solubility of the therapeutic agent in the drug core. The non-therapeutic agent of the drug core can comprise polymers as described herein and additives. A polymer of the core can be selected to provide the desired solubility of the therapeutic agent in the matrix. For example, the core can comprise hydrogel that may promote solubility of hydrophilic treatment agent. In some embodiments, functional groups can be added to the polymer to provide the desired solubility of the therapeutic agent in the matrix. For example, functional groups can be attached to silicone polymer.
- In some embodiments, additives may be used to control the release kinetics of therapeutic agent. For example, the additives may be used to control the concentration of therapeutic agent by increasing or decreasing solubility of the therapeutic agent in the drug core so as to control the release kinetics of the therapeutic agent. The solubility may be controlled by providing appropriate molecules and/or substances that increase and/or decrease the solubility of the dissolved from of the therapeutic agent to the matrix. The solubility of the dissolved from the therapeutic agent may be related to the hydrophobic and/or hydrophilic properties of the matrix and therapeutic agent. For example, surfactants, tinuvin, salts and water can be added to the matrix and may increase the solubility of hydrophilic therapeutic agent in the matrix. In addition, oils and hydrophobic molecules and can be added to the matrix and may increase the solubility of hydrophobic treatment agent in the matrix.
- Instead of or in addition to controlling the rate of migration based on the concentration of therapeutic agent dissolved in the matrix, the surface area of the drug core can also be controlled to attain the desired rate of drug migration from the core to the target site. For example, a larger exposed surface area of the core will increase the rate of migration of the treatment agent from the drug core to the target site, and a smaller exposed surface area of the drug core will decrease the rate of migration of the therapeutic agent from the drug core to the target site. The exposed surface area of the drug core can be increased in any number of ways, for example by any of castellation of the exposed surface, a porous surface having exposed channels connected with the tear or tear film, indentation of the exposed surface, protrusion of the exposed surface. The exposed surface can be made porous by the addition of salts that dissolve and leave a porous cavity once the salt dissolves. Hydrogels may also be used, and can swell in size to provide a larger exposed surface area. Such hydrogels can also be made porous to further increase the rate of migration of the therapeutic agent.
- Further, an implant may be used that includes the ability to release two or more drugs in combination, such as the structure disclosed in U.S. Pat. No. 4,281,654 (Shell). For example, in the case of glaucoma treatment, it may be desirable to treat a patient with multiple prostaglandins or a prostaglandin and a cholinergic agent or an adrenergic antagonist (beta blocker), such as Alphagan®, or a prostaglandin and a carbonic anhydrase inhibitor.
- In addition, drug impregnated meshes may be used such as those disclosed in US Patent Publication No. 2002/0055701 or layering of biostable polymers as described in US Patent Publication No. 2005/0129731. Certain polymer processes may be used to incorporate drug into the devices of the present invention such as, so-called “self-delivering drugs” or PolymerDrugs (Polymerix Corporation, Piscataway, N.J.) are designed to degrade only into therapeutically useful compounds and physiologically inert linker molecules, further detailed in US Patent Publication No. 2005/0048121 (East), hereby incorporated by reference in its entirety. Such delivery polymers may be employed in the devices of the present invention to provide a release rate that is equal to the rate of polymer erosion and degradation and is constant throughout the course of therapy. Such delivery polymers may be used as device coatings or in the form of microspheres for a drug depot injectable (such as a reservoir of the present invention). A further polymer delivery technology may also be adapted to the devices of the present invention such as that described in US Patent Publication No. 2004/0170685 (Carpenter), and technologies available from Medivas (San Diego, Calif.).
- In specific embodiments, the drug core matrix comprises a solid material, for example silicone, that encapsulates inclusions of the drug. The drug comprises molecules which are very insoluble in water and slightly soluble in the encapsulating drug core matrix. The inclusions encapsulated by the drug core can be micro-particles having dimensions from about 1 μm to about 100 μm across. The drug inclusions can comprise crystals, for example Bimatoprost crystals, and/or droplets of oil, for example with Latanoprost oil. The drug inclusions can dissolve into the solid drug core matrix and substantially saturate the drug core matrix with the drug, for example dissolution of Latanoprost oil into the solid drug core matrix. The drug dissolved in the drug core matrix is transported, often by diffusion, from the exposed surface of the drug core into the tear film. As the drug core is substantially saturated with the drug, in many embodiments the rate limiting step of drug delivery is transport of the drug from the surface of the drug core matrix exposed to the tear film. As the drug core matrix is substantially saturated with the drug, gradients in drug concentration within the matrix are minimal and do not contribute significantly to the rate of drug delivery. As surface area of the drug core exposed to the tear film is nearly constant, the rate of drug transport from the drug core into the tear film can be substantially constant. Work in relation with the present invention suggests that the solubility of the therapeutic agent in water and molecular weight of the drug can effect transport of the drug from the solid matrix to the tear. In many embodiments, the therapeutic agent is nearly insoluble in water and has a solubility in water of about 0.03% to 0.002% by weight and a molecular weight from about 400 grams/mol. to about 1200 grams/mol.
- In many embodiments the therapeutic agent has a very low solubility in water, for example from about 0.03% by weight to about 0.002% by weight, a molecular weight from about 400 grams per mole (g/mol.) to about 1200 g/mol, and is readily soluble in an organic solvent. Cyclosporin A (CsA) is a solid with an aqueous solubility of 27.67 μg/mL at 25° C., or about 0.0027% by weight, and a molecular weight (M.W.) of 1202.6 g/mol. Latanoprost (Xalatan) is a prostaglandin F2α analogue, a liquid oil at room temperature, and has an aqueous solubility of 50 μg/mL in water at 25° C., or about 0.005% by weight and a M.W. of 432.6 g/mol. Bimatoprost (Lumigan) is a synthetic prostamide analogue, a solid at room temperature solubility in water of 300 μg/mL in water at 25° C., or 0.03% by weight, and has a M.W. of 415.6 g/mol.
- Work in relation with the present invention indicates that naturally occurring surfactants in the tear film, for example surfactant D and phospholipids, may effect transport of the drug dissolved in the solid matrix from the core to the tear film. The drug core can be adapted in response to the surfactant in the tear film to provide sustained delivery of the drug into the tear film at therapeutic levels. For example, empirical data can be generated from a patient population, for example 10 patients whose tears are collected and analyzed for surfactant content. Elution profiles in the collected tears for a drug that is sparingly soluble in water, for example cyclosporine, can also be measured and compared with elution profiles in buffer and surfactant such that an in vitro model of tear surfactant is developed. An in vitro solution with surfactant based on this empirical data can be used to adjust the drug core in response to the surfactant of the tear film.
- The drug cores may also be modified to utilize carrier vehicles such as nanoparticles or microparticles depending on the size of the molecule to be delivered such as latent-reactive nanofiber compositions for composites and nanotextured surfaces (Innovative Surface Technologies, LLC, St. Paul, Minn.), nanostructured porous silicon, known as BioSilicont, including micron sized particles, membranes, woven fivers or micromachined implant devices (pSividia, Limited, UK) and protein nanocage systems that target selective cells to deliver a drug (Chimeracore).
- In many embodiments, the drug insert comprises of a thin-walled polyimide tube sheath with a drug core comprising Latanoprost dispersed in Nusil 6385 (MAF 970), a medical grade solid silicone that serves as the matrix for drug delivery. The distal end of the drug insert is sealed with a cured film of solid Loctite 4305 medical grade adhesive. The drug insert may be placed within the bore of the punctum plug, the Loctite 4305 adhesive does not come into contact with either tissue or the tear film. The inner diameter of the drug insert can be 0.32 mm; and the length can be 0.95 mm. Three Latanoprost concentrations in the finished drug product can be tested clinically: Drug cores can comprise 3.5, 7 or 14 μg Latanoprost, with percent by weight concentrations of 5, 10 and 20% respectively. Assuming an overall elution rate of approximately 100 ng/day, the drug core comprising 14 μg of Latanoprost is adapted to deliver drug for approximately at least 100 days, for example 120 days. The overall weight of the drug core, including Latanoprost, can be ˜70 μg. The weight of the drug insert including the polyimide sleeve can be approximately 100 μg.
- In many embodiments, the drug core may elute with an initial elevated level of therapeutic agent followed by substantially constant elution of the therapeutic agent. In many instances, an amount of therapeutic agent released daily from the core may be below the therapeutic levels and still provide a benefit to the patient. An elevated level of eluted therapeutic agent can result in a residual amount of therapeutic agent and/or residual effect of the therapeutic agent that is combined with a sub-therapeutic amount of therapeutic agent to provide relief to the patient. In embodiments where therapeutic level is about 80 ng per day, the device may deliver about 100 ng per day for an initial delivery period. The extra 20 ng delivered per day can have a beneficial effect when therapeutic agent is released at levels below the therapeutic level, for example at 60 ng per day. As the amount of drug delivered can be precisely controlled, an initial elevated dose may not result in complications and/or adverse events to the patient.
- Drug cores as described above have been fabricated with different cross sectional sizes of 0.006 inches, 0.012 inches, and 0.025 inches, and drug concentrations of 5%, 10% and 20% in a silicone matrix. Theses drug cores can be made with a Syringe Tube and Cartridge Assembly, Mixing Latanoprost with Silicone, and Injecting the mixture into a polyimide tube which is cut to desired lengths and sealed. The length of the drug cores were approximately 0.80 to 0.95 mm, which for a diameter of 0.012 inches (0.32 mm) corresponds to total Latanoprost content in the drug cores of approximately 3.5 μg, 7 μg and 14 μg for concentrations of 5%, 10% and 20%, respectively.
- Syringe Tube and Cartridge Assembly. 1. Take polyimide tubing of three different diameters 0.006 inches, 0.0125 inches and 0.025 inches. 2. Cut polyimide tubing of different diameters to ˜15 cm length. 3. Insert Polyimide tubes into a Syringe Adapter. 4. Adhesive bond polyimide tube into luer adapter (Loctite, low viscosity UV cure). 5. Trim end of assembly. 6. Clean the cartridge assembly using distilled water and then with methanol and dry it in oven at 60° C.
- Mix Latanoprost with Silicone. Prepare Latanoprost. Latanoprost is provided as a 1% solution in methylacetate. Place the appropriate amount of solution into a dish and using a nitrogen stream, evaporate the solution until only the Latanoprost remains. Place the dish with the Latanoprost oil under vacuum for 30 minutes. Combine Latanoprost with silicone. Prepare three different concentrations of Latanoprost (5%, 10% and 20%) in silicon Nusil 6385 and inject it into tubing of different diameters (0.006 in, 0.012 in and 0.025 inches) to generate 3×3 matrixes. The percent of Latanoprost to silicone is determined by the total weight of the drug matrix. Calculation: Weight of Latanoprost/(weight of Latanoprost+weight of silicone)×100=percent drug.
- Inject tube. 1. Insert Cartridge and Polyimide tubes assembly into 1 ml syringe. 2. Add one drop of catalyst, (MED-6385 Curing Agent) in the syringe. 3. Force excess catalyst out of the polyimide tube with clean air. 4. Fill syringe with silicone drug matrix. 5. Inject tube with drug matrix until the tube is filled or the syringe plunger becomes too difficult to push. 6. Close off the distal end of the polyimide tube and maintain pressure until the silicone begins to solidify. 7. Allow to cure at room temperature for 12 hours. 8. Place under vacuum for 30 minutes. 9. Place tube in right size trim fixture (prepared in house to hold different size tubing) and cut drug inserts to length (0.80-0.95 mm).
- Testing. Elution study (in vitro). 1.
Place 10 plugs of same size and same concentration per centrifuge tube and add 1.5 ml of 7.4 pH buffer solution to it. 2. Change the solvent with fresh 7.4 pH buffer after appropriate time. 3. Take HPLC of the elutant at 210 nm with PDA detector 2996 using Sunfire C18, 3 mm×10 mm column (Waters Corporation, Milford, Mass.). Acetonitrile and water mixture is used for gradient elution. Calibration was done in house before and after each analysis, using in-house standards with precisely weighed concentration of Latanoprost. 4. Calculate the amount of drug release per day per device for different size tubings having different concentrations of Latanoprost. 5. Plot elution rate vs area and concentration forday 1 andday 14. -
FIGS. 7A and 7B show elution data of Latanoprost atday 1 andday 14, respectively, for the three core diameters of 0.006, 0.012 and 0.025 inches and three Latanoprost concentrations of approximately 5%, 11% and 18%. Elution rate of the Latanoprost in nanograms (ng) per day is plotted versus percent concentration. These data show that the rate of elution is mildly dependent on the concentration and strongly dependent on the exposed surface area at both time periods. Atday 1, the 0.006 inch, 0.012 inch and 0.025 inch diameter cores released about 200 ng, 400 ng and 1200 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core. For each tube diameter, the quantity of Latanoprost released is compared to the concentration of drug in the drug core with a least square regression line. For the 0.006, 0.012 and 0.025 inch drug cores the slope of the regression lines are 11.8, 7.4 and 23.4, respectively. These values indicate that a doubling of concentration of the Latanoprost drug in the core does not lead to a doubling of the elution rate of the Latanoprost from the core, consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above. - At
day 14, the 0.006 inch, 0.012 inch (0.32 mm) and 0.025 inch diameter cores released about 25 ng, 100 ng and 300 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core at extended periods of time, and that the quantity of Latanoprost released is mildly dependent on the concentration of therapeutic agent in the core. For each tube diameter, the quantity of Latanoprost released is compared to the concentration of drug in the drug core with a least square regression line. For the 0.006, 0.012 and 0.025 inch drug cores the slope of the regression lines are 3.0, 4.3 and 2.2, respectively. For the 0.012 and 0.025 inch cores, these values indicate that a doubling of concentration of the Latanoprost drug in the core does not lead to a doubling of the elution rate of the Latanoprost from the core, consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above. However, for the 0.006 inch diameter core, there is an approximately first order relationship between the quantity of initially in the core and the amount of drug released atday 14, which can may be caused by depletion of Latanoprost drug droplets in the core. -
FIGS. 7D and 7E show dependence of the rate of elution on exposed surface area of the drug core for the three core diameters and the three concentrations as inFIGS. 7A and 7B Latanoprost atday 1 andday 14, respectively, according to embodiments of the present invention. Elution rate of the Latanoprost in nanograms (ng) per day is plotted versus the exposed surface area of the drug core in mm2 as determined by the diameter of the drug core. - These data show that the rate of elution is mildly dependent on the concentration of drug in the core and strongly dependent on the exposed surface area at both one day and a 14 days. The exposed surface areas of the 0.006 inch, 0.012 inch and 0.025 inch diameter cores are approximately 0.02, 0.07, and 0.32 mm2, respectively. At
day 1, the 0.02, 0.07, and 0.32 mm2, cores released about 200 ng, 400 ng and 1200 ng of Latanoprost, respectively, showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core. For each concentration of therapeutic agent in the drug core, the quantity of Latanoprost released is compared to the exposed surface area of the drug core with a least square regression line. For the 5.1%, 11.2%, and 17.9% drug cores the slope of the regression lines are 2837.8, 3286.1 and 3411.6, respectively, with R2 coefficients of 0.9925, 0.9701 and 1, respectively. Atday 14, the 0.02, 0.07, and 0.32 mm2, cores released about 25 ng, 100 ng and 300 ng of Latanoprost, respectively showing that the quantity of Latanoprost released increases with an increased size of the exposed surface area of the drug core. For the 5.1%, 11.2%, and 17.9% drug cores the slope of the regression lines are 812.19, 1060.1 and 764.35, respectively, with R2 coefficients of 0.9904, 0.9924 and 0.9663, respectively. These values indicate the elution rate of the Latanoprost from the core increases linearly with the surface area of the drug core, consistent with a drug sheath that can control the exposed surface area, as described above. The weak dependence of Latanoprost elution on concentration in the drug core is consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above. -
FIG. 7C shows elution data for Latanoprost from 0.32 mm diameter, 0.95 mm long drug cores with concentrations of 5, 10 and 20% and drug weights of 3.5, 7 and 14 μg, respectively, according to embodiments of the present invention. The drug cores were manufactured as described above. The elution rate is plotted in ng per day from 0 to 40 days. The 14 μg core shows rates of approximately 100 ng per day from about 10 to 40 days. The 7 μg core shows comparable rates from 10 to 20 days. These data are consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above. - Table 2 shows the expected parameters for each drug concentration. As shown in
FIG. 1C , in vitro results in a buffered saline elution system show that the plug initially elutes approximately 500 ng of Latanoprost per day, dropping off rapidly within 7-14 days to approximately 100 ng/day, depending on the initial concentration of drug. -
TABLE 2 Drug Elution Properties Total Latanoprost content 14 μg 7 μg 3.5 μg In vitro elution rate See FIG. 1C See FIG. 1C See FIG. 1C Duration ~100 days ~45 days ~25 days - In many embodiments, the duration of the drug core can be determined based on the calculated time when ˜10% of the original amount of drug remains in drug insert, for example where the elution rate levels out and remains substantially constant at approximately 10 ng/day.
- Drug cores as described in Example 1 were made with cyclosporin having a concentration of 21.2%.
FIG. 8A shows elution profiles of cyclosporin from drug cores into a buffer solution without surfactant and into a buffer solution with surfactant, according to embodiments of the present invention. The buffer solution was made as described above. The solution with surfactant includes 95% buffer and 5% surfactant, UP-1005 Ultra Pure Fluid from Dow Corning, Midland Mich. Work in relation with embodiments of the present invention indicates that in at least some instances, surfactants may be used in in vitro to model in situ elution from the eye as the eye can include natural surfactants, for example Surfactant Protein D, in the tear film. The elution profile of cyclosporin into surfactant is approximately 50 to 100 ng per day from 30 to 60 days. Empirical data from tears of a patient population, for example 10 patients, can be measured and used to refine the in vitro model with appropriate amounts of surfactant. The drug core matrix may be modified in response to the human tear surfactant as determined with the modified in vitro model. The drug core can be modified in many ways in response to the human tear film surfactant, for example with an increased exposed surface area and/or additives to increase an amount of cyclosporine drug dissolved in the core, as described above, to increase elution from the core to therapeutic levels, if appropriate. - Bulk samples of 1% Bimatoprost having a known diameter of 0.076 cm (0.76 mm) were prepared. The height of each sample was determined from the weight and known diameter of the sample.
-
TABLE 2 Bulk Sample Size wt diameter calculated Exposed Surface sample (mg) (cm) height (cm) Area(cm{circumflex over ( )}2) 14-2-10 1.9 0.076 0.42 0.109 14-2-11 1.5 0.076 0.33 0.088 14-2-12 1.9 0.076 0.42 0.109 - The calculated heights ranged from 0.33 cm to 0.42 cm. The exposed surface area on each end of each bulk sample was approximately 0.045 cm2, providing volumes of 0.019 cm and 0.015 cm3 for the 0.42 and 0.33 cm samples, respectively. The exposed an exposed surface area of samples calculated from the height and diameter without a drug sheath was approximately 0.1 cm2. Three formulations were evaluated: 1)
silicone 4011, 1% Bimatoprost, 0% surfactant; 2)silicone 4011, 1% Bimatoprost, approximately 11% surfactant; and 3)silicone 4011, 1% Bimatoprost, approximately 33% surfactant. The elution data measured for the bulk samples withformulation FIG. 9A shows normalized elution profiles in ng per device per day over 100 days for bulk sample of silicone with 1% Bimatoprost, assuming an exposed surface diameter of 0.3 mm on the end of the device, according to embodiments of the present invention. The normalized elution profile is about 10 ng per day. The data show approximately zero order release kinetics from about ten days to about 90 days for each of the formulations. These data are consistent with particles of Bimatoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Bimatoprost dissolved therein, as described above. Similar formulations can be used with drug core sheaths and a shaped exposed surface of the core exposed to the tear to increase the exposed surface area as described above and deliver the drug in therapeutic amounts over an extended period. - In some embodiments, the core can comprise a 0.76 mm diameter core with an exposed surface diameter of 0.76 mm, corresponding to an exposed surface area of 0.0045 cm2. The core can be covered with a sheath to define the exposed surface of the core as described above The normalized elution profile for such a device, based on the bulk sample data above, is approximately 6 times (0.0045 cm2/0.00078 cm2) the elution profile for the device with a 0.3 mm diameter exposed surface area. Thus, a zero order elution profile with an elution rate of about 60 ng per day can be obtained over a period of about 90 days. If the exposed surface area is increased to about 0.0078 cm2, for example with many of the exposed surface shapes as described above, the zero order elution rat is about 100 ng per day over a period of about 90 days. The concentration can also be increased from 1%. Similar elution profiles can be obtained with Latanoprost.
- Drug cores were manufactured as described above with Latanoprost and silicone 4011, 6385 and/or NaCl. Four formulations were manufactured as follows: A) silicone 4011, approximately 20% Latanoprost, and approximately 20% NaCL; B) silicone 4011, approximately 20% Latanoprost, and approximately 10% NaCl; C) silicone 4011, approximately 10% Latanoprost, and approximately 10% NaCl; and D) silicone 6385, approximately 20% Latanoprost.
FIG. 10A shows profiles of elution of Latanoprost form the cores for four formulations of Latanoprost, according to embodiments of the present invention. The results show initial rates of approximately 300 ng per device per day that decreases to about 100 ng per device per day by 3 weeks (21 days). The results shown are for non-sterile drug cores. Similar results have been obtained with sterile drug cores of Latanoprost. These data are consistent with droplets of Latanoprost suspended in a drug core matrix and substantial saturation of the drug core matrix with Latanoprost dissolved therein, as described above - While the exemplary embodiments have been described in some detail, by way of example and for clarity of understanding, those of skill in the art will recognize that a variety of modification, adaptations, and changes may be employed. For example, multiple delivery mechanisms may be employed, and each device embodiment may be adapted to include features or materials of the other, and further multiple features or multiple materials may be employed in a single device. Hence, the scope of the present invention may be limited solely by the appending claims.
Claims (77)
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Cited By (49)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US20050232972A1 (en) * | 2004-04-15 | 2005-10-20 | Steven Odrich | Drug delivery via punctal plug |
US20070212397A1 (en) * | 2005-09-15 | 2007-09-13 | Roth Daniel B | Pharmaceutical delivery device and method for providing ocular treatment |
US20070243230A1 (en) * | 2006-03-31 | 2007-10-18 | Forsight Labs, Llc | Nasolacrimal Drainage System Implants for Drug Therapy |
US20090104243A1 (en) * | 2007-09-07 | 2009-04-23 | Qlt Plug Delivery, Inc. - Qpdi | Drug cores for sustained release of therapeutic agents |
US20090118702A1 (en) * | 2004-07-02 | 2009-05-07 | Forsight Labs, Llc | Treatment Medium Delivery Device and Methods for Delivery of Such Treatment Mediums to the Eye Using such a Delivery Device |
US20090280158A1 (en) * | 2008-05-09 | 2009-11-12 | Qlt Plug Delivery, Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US20090318549A1 (en) * | 2008-06-24 | 2009-12-24 | Qlt Plug Delivery, Inc. | Combination treatment of glaucoma |
US20100034870A1 (en) * | 2008-04-30 | 2010-02-11 | QLT. Plug Delivery, Inc. | Composite lacrimal insert and related methods |
US20100274224A1 (en) * | 2008-07-08 | 2010-10-28 | Qlt Plug Delivery, Inc. | Lacrimal implant body including comforting agent |
WO2010141729A1 (en) * | 2009-06-03 | 2010-12-09 | Forsight Labs, Llc | Anterior segment drug delivery |
US8277830B2 (en) | 2009-01-29 | 2012-10-02 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US8623395B2 (en) | 2010-01-29 | 2014-01-07 | Forsight Vision4, Inc. | Implantable therapeutic device |
US8715712B2 (en) | 2011-09-14 | 2014-05-06 | Forsight Vision5, Inc. | Ocular insert apparatus and methods |
US8715713B2 (en) | 2011-04-29 | 2014-05-06 | Allergan, Inc. | Solvent cast film sustained release latanoprost implant |
US8900620B2 (en) | 2005-10-13 | 2014-12-02 | DePuy Synthes Products, LLC | Drug-impregnated encasement |
US8905963B2 (en) | 2010-08-05 | 2014-12-09 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
WO2016083891A1 (en) * | 2014-11-25 | 2016-06-02 | Eyal Sheetrit | Compositions and methods for delivering a bio-active agent or bio-active agents |
US9381683B2 (en) | 2011-12-28 | 2016-07-05 | DePuy Synthes Products, Inc. | Films and methods of manufacture |
US9474756B2 (en) | 2014-08-08 | 2016-10-25 | Forsight Vision4, Inc. | Stable and soluble formulations of receptor tyrosine kinase inhibitors, and methods of preparation thereof |
US9492315B2 (en) | 2010-08-05 | 2016-11-15 | Forsight Vision4, Inc. | Implantable therapeutic device |
US9526654B2 (en) | 2013-03-28 | 2016-12-27 | Forsight Vision4, Inc. | Ophthalmic implant for delivering therapeutic substances |
US9610271B2 (en) | 2011-08-29 | 2017-04-04 | Mati Therapeutics Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US9750636B2 (en) | 2012-10-26 | 2017-09-05 | Forsight Vision5, Inc. | Ophthalmic system for sustained release of drug to eye |
US9883968B2 (en) | 2011-09-16 | 2018-02-06 | Forsight Vision4, Inc. | Fluid exchange apparatus and methods |
US9968603B2 (en) | 2013-03-14 | 2018-05-15 | Forsight Vision4, Inc. | Systems for sustained intraocular delivery of low solubility compounds from a port delivery system implant |
US9974685B2 (en) | 2011-08-29 | 2018-05-22 | Mati Therapeutics | Drug delivery system and methods of treating open angle glaucoma and ocular hypertension |
US10004634B2 (en) | 2015-06-16 | 2018-06-26 | The Regents Of The University Of Colorado | Nasolacrimal implants and related methods for tear stimulation |
US10010448B2 (en) | 2012-02-03 | 2018-07-03 | Forsight Vision4, Inc. | Insertion and removal methods and apparatus for therapeutic devices |
US10166142B2 (en) | 2010-01-29 | 2019-01-01 | Forsight Vision4, Inc. | Small molecule delivery with implantable therapeutic device |
US10195078B2 (en) | 2013-02-19 | 2019-02-05 | Aquesys, Inc. | Adjustable intraocular flow regulation |
US10206813B2 (en) | 2009-05-18 | 2019-02-19 | Dose Medical Corporation | Implants with controlled drug delivery features and methods of using same |
US10245178B1 (en) | 2011-06-07 | 2019-04-02 | Glaukos Corporation | Anterior chamber drug-eluting ocular implant |
US10258503B2 (en) | 2014-07-15 | 2019-04-16 | Forsight Vision4, Inc. | Ocular implant delivery device and method |
US10398592B2 (en) | 2011-06-28 | 2019-09-03 | Forsight Vision4, Inc. | Diagnostic methods and apparatus |
US10406029B2 (en) | 2001-04-07 | 2019-09-10 | Glaukos Corporation | Ocular system with anchoring implant and therapeutic agent |
US10500304B2 (en) | 2013-06-21 | 2019-12-10 | DePuy Synthes Products, Inc. | Films and methods of manufacture |
US10500091B2 (en) | 2014-11-10 | 2019-12-10 | Forsight Vision4, Inc. | Expandable drug delivery devices and methods of use |
US10617557B2 (en) | 2010-08-05 | 2020-04-14 | Forsight Vision4, Inc. | Combined drug delivery methods and apparatus |
US10874548B2 (en) | 2010-11-19 | 2020-12-29 | Forsight Vision4, Inc. | Therapeutic agent formulations for implanted devices |
US10959941B2 (en) | 2014-05-29 | 2021-03-30 | Glaukos Corporation | Implants with controlled drug delivery features and methods of using same |
US11141312B2 (en) | 2007-09-07 | 2021-10-12 | Mati Therapeutics Inc. | Lacrimal implant detection |
US11224602B2 (en) | 2015-04-13 | 2022-01-18 | Forsight Vision5, Inc. | Ocular insert composition of a semi-crystalline or crystalline pharmaceutically active agent |
US11318043B2 (en) | 2016-04-20 | 2022-05-03 | Dose Medical Corporation | Bioresorbable ocular drug delivery device |
US11419759B2 (en) | 2017-11-21 | 2022-08-23 | Forsight Vision4, Inc. | Fluid exchange apparatus for expandable port delivery system and methods of use |
US11432959B2 (en) | 2015-11-20 | 2022-09-06 | Forsight Vision4, Inc. | Porous structures for extended release drug delivery devices |
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US11617680B2 (en) | 2016-04-05 | 2023-04-04 | Forsight Vision4, Inc. | Implantable ocular drug delivery devices |
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USD1033637S1 (en) | 2022-01-24 | 2024-07-02 | Forsight Vision4, Inc. | Fluid exchange device |
Families Citing this family (122)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
GB9808052D0 (en) | 1998-04-17 | 1998-06-17 | Secr Defence | Implants for administering substances and methods of producing implants |
US20040225250A1 (en) | 2003-05-05 | 2004-11-11 | Michael Yablonski | Internal shunt and method for treating glaucoma |
US7291125B2 (en) | 2003-11-14 | 2007-11-06 | Transcend Medical, Inc. | Ocular pressure regulation |
WO2006078320A2 (en) | 2004-08-04 | 2006-07-27 | Brookwood Pharmaceuticals, Inc. | Methods for manufacturing delivery devices and devices thereof |
ES2400091T3 (en) | 2005-08-11 | 2013-04-05 | Massachusetts Institute Of Technology | Intravesical drug delivery device and method |
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US9084662B2 (en) | 2006-01-17 | 2015-07-21 | Transcend Medical, Inc. | Drug delivery treatment device |
DE602007012417D1 (en) | 2006-03-14 | 2011-03-24 | Univ Southern California | Mems device for drug release |
US9474645B2 (en) * | 2006-06-21 | 2016-10-25 | Johnson & Johnson Vision Care, Inc. | Punctal plugs for the delivery of active agents |
SG138567A1 (en) * | 2006-06-21 | 2008-01-28 | Johnson & Johnson Vision Care | Punctal plugs for the delivery of active agents |
CA2669642A1 (en) * | 2006-11-09 | 2008-05-22 | Alcon Research, Ltd. | Punctal plug comprising a water-insoluble polymeric matrix |
PL2091514T3 (en) | 2006-11-09 | 2014-03-31 | Alcon Res Ltd | Water insoluble polymer matrix for drug delivery |
UY30883A1 (en) | 2007-01-31 | 2008-05-31 | Alcon Res | PUNCTURAL PLUGS AND METHODS OF RELEASE OF THERAPEUTIC AGENTS |
WO2009012406A1 (en) * | 2007-07-17 | 2009-01-22 | Transcend Medical, Inc. | Ocular implant with hydrogel expansion capabilities reference to priority document |
EP2865361B1 (en) | 2007-09-07 | 2019-05-22 | Mati Therapeutics Inc. | Lacrimal implants and related methods |
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WO2009079559A1 (en) * | 2007-12-17 | 2009-06-25 | University Of Florida Research Foundation, Inc. | Dry eye treatment by puncta plugs |
ES2425769T5 (en) | 2007-12-20 | 2017-07-28 | University Of Southern California | Apparatus for the administration of therapeutic agents |
EP2222281B1 (en) | 2007-12-20 | 2018-12-05 | Evonik Corporation | Process for preparing microparticles having a low residual solvent volume |
WO2009105178A2 (en) | 2008-02-18 | 2009-08-27 | Qlt Plug Delivery, Inc. | Lacrimal implants and related methods |
US9849238B2 (en) | 2008-05-08 | 2017-12-26 | Minipumps, Llc | Drug-delivery pump with intelligent control |
ES2534865T3 (en) | 2008-05-08 | 2015-04-29 | Minipumps, Llc | Drug delivery pumps |
EP2320989B1 (en) | 2008-05-08 | 2015-03-11 | MiniPumps, LLC | Implantable pumps and cannulas therefor |
EP3298995A1 (en) | 2008-06-25 | 2018-03-28 | Novartis AG | Ocular implant with shape change capabilities |
BRPI0917135A2 (en) | 2008-08-09 | 2015-11-10 | Massachusetts Inst Technology | medical device for extension and retention in a patient's seminal vesicle, ejaculatory duct, prostate or vas deferens, use of a resorbable elastomer, and osmotic pump device. |
US20100204335A1 (en) * | 2008-12-01 | 2010-08-12 | Allergan, Inc. | Kit and composition for eyelash growth |
WO2010071844A1 (en) * | 2008-12-19 | 2010-06-24 | Qlt Plug Delivery, Inc | Substance delivering punctum implants and methods |
RU2011134043A (en) * | 2009-01-23 | 2013-02-20 | Клт Инк. | DELIVERY OF ONE OR MORE AGENT WITH LONG-TERM RELEASE |
WO2010088258A2 (en) | 2009-01-28 | 2010-08-05 | Transcend Medical, Inc. | Ocular implant with stiffness qualities, methods of implantation and system |
US20100204325A1 (en) * | 2009-02-11 | 2010-08-12 | Allergan, Inc. | Valproic acid drug delivery systems and intraocular therapeutic uses thereof |
CA2750242C (en) * | 2009-02-12 | 2018-05-22 | Incept, Llc | Drug delivery through hydrogel plugs |
WO2010096822A2 (en) * | 2009-02-23 | 2010-08-26 | Qlt Plug Delivery, Inc. | Lacrimal implants and related methods |
US8911495B2 (en) * | 2009-03-16 | 2014-12-16 | Endoshape, Inc. | Reliably retained shape memory ophthalmological implants |
TWI495459B (en) * | 2009-03-31 | 2015-08-11 | Johnson & Johnson Vision Care | Punctal plugs |
US9421127B2 (en) | 2009-03-31 | 2016-08-23 | Johnson & Johnson Vision Care, Inc. | Punctal plugs |
AU2010246067B2 (en) | 2009-05-04 | 2016-07-07 | Eyepoint Pharmaceuticals Us, Inc. | Porous silicon drug-eluting particles |
US10543166B2 (en) | 2009-06-26 | 2020-01-28 | Taris Biomedical Llc | Implantable drug delivery devices and methods of making the same |
JP5758388B2 (en) | 2009-08-18 | 2015-08-05 | ミニパンプス, エルエルシー | Electrolyte drug delivery pump with adaptive control |
US8808257B2 (en) * | 2009-08-31 | 2014-08-19 | Johnson & Johnson Vision Care, Inc. | Methods and apparatus for pulsatile release of medicaments from a punctal plug |
US9017312B2 (en) | 2009-09-10 | 2015-04-28 | Taris Biomedical Llc | Implantable device for controlled drug delivery |
WO2011066479A1 (en) | 2009-11-27 | 2011-06-03 | Qlt Plug Delivery, Inc. | Lacrimal implants including split and insertable drug core |
US8529492B2 (en) | 2009-12-23 | 2013-09-10 | Trascend Medical, Inc. | Drug delivery devices and methods |
US9259352B2 (en) | 2010-03-29 | 2016-02-16 | Johnson & Johnson Vision Care, Inc. | Punctal plugs |
US9259351B2 (en) | 2010-03-29 | 2016-02-16 | Johnson & Johnson Vision Care, Inc. | Punctal plugs |
US20110251568A1 (en) * | 2010-04-08 | 2011-10-13 | Beeley Nathan R F | Punctal plugs for controlled release of therapeutic agents |
DK2600848T3 (en) | 2010-08-05 | 2019-06-24 | Taris Biomedical Llc | Implantable drug delivery devices for urogenital positions |
US8821457B2 (en) * | 2010-09-08 | 2014-09-02 | Johnson & Johnson Vision Care, Inc. | Punctal plug containing drug formulation |
US8591484B2 (en) | 2010-09-15 | 2013-11-26 | AlphaMed, Inc. | Lacrimal punctum measurement and occlusion |
US9022967B2 (en) | 2010-10-08 | 2015-05-05 | Sinopsys Surgical, Inc. | Implant device, tool, and methods relating to treatment of paranasal sinuses |
AU2011323524B2 (en) | 2010-11-01 | 2016-12-08 | Eyepoint Pharmaceuticals Us, Inc. | Bioerodible silicon-based devices for delivery of therapeutic agents |
AP2013006939A0 (en) * | 2010-11-26 | 2013-06-30 | Univ Witwatersrand Jhb | A drug delivery device |
US20120157938A1 (en) * | 2010-12-16 | 2012-06-21 | Tokarski Jason M | Punctal plug with drug core retention features |
EP2663300B1 (en) | 2011-01-10 | 2023-03-08 | TARIS Biomedical LLC | Lidocaine regimen for the use of sustained treatment of bladder pain and irritative voiding |
EP2670398B1 (en) | 2011-02-04 | 2017-06-07 | TARIS Biomedical LLC | Implantable device for controlled release of low solubility drug |
RU2456005C1 (en) * | 2011-04-20 | 2012-07-20 | Общество с ограниченной ответственностью фирма "Биокор" | Method for preparing biologically active preparation |
US10226417B2 (en) | 2011-09-16 | 2019-03-12 | Peter Jarrett | Drug delivery systems and applications |
GB201120771D0 (en) * | 2011-12-02 | 2012-01-11 | Ljt Projects Ltd | tear duct resistance measuring system |
US8765210B2 (en) | 2011-12-08 | 2014-07-01 | Aquesys, Inc. | Systems and methods for making gelatin shunts |
US10342700B2 (en) * | 2012-02-22 | 2019-07-09 | Ira H. Schachar | Device and method for treatment of retinal detachment and other maladies of the eye |
SG193127A1 (en) * | 2012-02-29 | 2013-09-30 | Johnson & Johnson Vision Care | Punctal plug with energized containment array |
US9572964B2 (en) | 2012-04-11 | 2017-02-21 | Sinapsys Surgical, Inc. | Implantation tools, tool assemblies, kits and methods |
US10085633B2 (en) | 2012-04-19 | 2018-10-02 | Novartis Ag | Direct visualization system for glaucoma treatment |
US9241832B2 (en) | 2012-04-24 | 2016-01-26 | Transcend Medical, Inc. | Delivery system for ocular implant |
WO2013164671A1 (en) | 2012-05-03 | 2013-11-07 | Qlt Inc. | Drug delivery system and methods of treating open angle glaucoma and ocular hypertension |
KR101969594B1 (en) * | 2012-05-11 | 2019-04-16 | 서강대학교산학협력단 | Implant for intraocular drug delivery |
US9480598B2 (en) | 2012-09-17 | 2016-11-01 | Novartis Ag | Expanding ocular implant devices and methods |
WO2014078288A1 (en) | 2012-11-14 | 2014-05-22 | Transcend Medical, Inc. | Flow promoting ocular implant |
PT2903575T (en) | 2013-01-25 | 2018-01-08 | Sinopsys Surgical Inc | Paranasal sinus access implant device and kit |
US9125723B2 (en) | 2013-02-19 | 2015-09-08 | Aquesys, Inc. | Adjustable glaucoma implant |
AU2014235051B2 (en) | 2013-03-15 | 2019-01-17 | Eyepoint Pharmaceuticals Us, Inc. | Bioerodible silicon-based compositions for delivery of therapeutic agents |
EP2968880A1 (en) | 2013-03-15 | 2016-01-20 | TARIS Biomedical LLC | Drug delivery devices with drug-permeable component and methods |
US9987163B2 (en) | 2013-04-16 | 2018-06-05 | Novartis Ag | Device for dispensing intraocular substances |
KR102488491B1 (en) | 2013-08-19 | 2023-01-12 | 타리스 바이오메디컬 엘엘씨 | Multi-unit drug delivery devices and methods |
WO2015069433A1 (en) | 2013-10-16 | 2015-05-14 | Sinopsys Surgical, Inc. | Apparatuses, tools and kits relating to fluid manipulation treatments of paranasal sinuses |
US9585790B2 (en) | 2013-11-14 | 2017-03-07 | Aquesys, Inc. | Intraocular shunt inserter |
HU231309B1 (en) | 2014-02-25 | 2022-11-28 | Darholding Kft. | Compositions comprising indometacine, its pharmaceutically acceptable salts and cocrystals; and process for the preparation |
EP3179968B1 (en) * | 2014-07-24 | 2019-09-11 | Sinopsys Surgical, Inc. | Paranasal sinus access implant devices and related products and methods |
RU2562515C1 (en) * | 2014-08-19 | 2015-09-10 | федеральное государственное бюджетное учреждение "Межотраслевой научно-технический комплекс "Микрохирургия глаза" имени академика С.Н. Федорова" Министерства здравоохранения Российской Федерации | Intubation kit for bicanalicular drainage of lachrymal passages |
ES2756301T3 (en) | 2014-08-19 | 2020-04-27 | Univ California | Localized drug delivery implants and methods of using them |
US10507101B2 (en) | 2014-10-13 | 2019-12-17 | W. L. Gore & Associates, Inc. | Valved conduit |
WO2016099946A1 (en) | 2014-12-17 | 2016-06-23 | Paul Gavaris | Canalicular plug, method and kit for treating dry eye |
RU2581823C1 (en) * | 2015-03-17 | 2016-04-20 | федеральное государственное бюджетное учреждение "Межотраслевой научно-технический комплекс "Микрохирургия глаза" имени академика С.Н. Федорова" Министерства здравоохранения Российской Федерации | Drainage for surgical treatment of glaucoma |
CN107529985B (en) | 2015-03-31 | 2020-03-31 | 加州理工学院 | Biocompatible encapsulation for long-term implantable sensors and electronics |
GB201505527D0 (en) | 2015-03-31 | 2015-05-13 | Jmedtech Pte Ltd | Composition |
WO2016172704A1 (en) | 2015-04-23 | 2016-10-27 | Taris Biomedical Llc | Drug delivery devices with drug-permeable component and methods |
WO2016187355A1 (en) * | 2015-05-20 | 2016-11-24 | Glaukos Corporation | Therapeutic drug compositions and implants for delivery of same |
WO2017007819A1 (en) * | 2015-07-06 | 2017-01-12 | The Regents Of The University Of Colorado, A Body Corporate | Lacrimal drainage system diagnostic implant |
KR20180034541A (en) | 2015-07-22 | 2018-04-04 | 인셉트, 엘엘씨 | Coated tear point plug |
WO2017062770A1 (en) | 2015-10-08 | 2017-04-13 | Silverberg Noah | Punctal plug and bioadhesives |
RU2620249C1 (en) * | 2015-12-17 | 2017-05-23 | Федеральное государственное автономное учреждение "Межотраслевой научно-технический комплекс "Микрохирургия глаза" имени академика С.Н. Федорова" Министерства здравоохранения Российской Федерации | Multilayer biodegradable ocular implant with dosed drug release and method of its manufacture |
RU2613435C1 (en) * | 2015-12-17 | 2017-03-16 | Федеральное государственное автономное учреждение "Межотраслевой научно-технический комплекс "Микрохирургия глаза" имени академика С.Н. Федорова" Министерства здравоохранения Российской Федерации | Drainage for glaucoma surgery |
JP6936801B2 (en) * | 2015-12-21 | 2021-09-22 | バイエル・オーイュー | Manufacturing method of drug delivery device and drug delivery device manufactured according to the method |
AU2017268379A1 (en) | 2016-05-20 | 2018-12-06 | The Regents Of The University Of Colorado, A Body Corporate | Lacrimal drug delivery device |
GB2555373A (en) * | 2016-08-23 | 2018-05-02 | Reproductive Medicine And Gynaecology Associates Ltd | Implant |
DK3518897T3 (en) | 2016-09-30 | 2022-03-07 | Mati Therapeutics Inc | DEPOSIT FORMAL OPTIONAL MEDICINAL PRODUCT AND ITS USE |
US9925028B1 (en) * | 2016-11-15 | 2018-03-27 | Proximate Concepts Llc | Device for the delivery of a prosthetic implant and method of use thereof |
US10722335B1 (en) * | 2016-11-15 | 2020-07-28 | Proximate Concepts Llc | Device for the delivery of a prosthetic implant and method of use thereof |
US11351058B2 (en) | 2017-03-17 | 2022-06-07 | W. L. Gore & Associates, Inc. | Glaucoma treatment systems and methods |
EP3621512B1 (en) * | 2017-05-12 | 2024-02-28 | California Institute of Technology | Implantable extracompartmental pressure sensor |
KR20200069261A (en) * | 2017-05-30 | 2020-06-16 | 엑시모어 엘티디. | Compositions and methods for treating dry eye syndrome delivering antibiotic macrolides |
CN111065359A (en) | 2017-06-16 | 2020-04-24 | 埃斯库莱泰克股份有限公司 | Thermally reactive polymers and their use |
JP7193865B2 (en) | 2017-07-31 | 2022-12-21 | 慶應義塾 | Short-term tumorigenicity screening system |
US11129972B2 (en) | 2017-09-20 | 2021-09-28 | Sinopsys Surgical, Inc. | Paranasal sinus fluid access implantation tools, assemblies, kits and methods |
EP3691618A1 (en) | 2017-10-06 | 2020-08-12 | Foundry Therapeutics, Inc. | Implantable depots for the controlled release of therapeutic agents |
SG11202009056PA (en) * | 2018-03-22 | 2020-10-29 | Alphamed Inc | Intracanalicular dissolvable punctum plug inserter |
WO2020050968A1 (en) | 2018-09-04 | 2020-03-12 | University Hospitals Health System, Inc. | Ocular device for treating glaucoma and related minimally invasive glaucoma surgery method |
US11678983B2 (en) | 2018-12-12 | 2023-06-20 | W. L. Gore & Associates, Inc. | Implantable component with socket |
US11850135B2 (en) | 2019-08-01 | 2023-12-26 | Paul H. Rosenberg Family Trust | Prosthetic implant delivery device utilizing surface active agents |
US11207267B2 (en) | 2019-10-02 | 2021-12-28 | Segal Innovations LLC | Bio-adhesive dissolving compounds and device |
US11701504B2 (en) | 2020-01-17 | 2023-07-18 | California Institute Of Technology | Implantable intracranial pressure sensor |
IL295357A (en) | 2020-02-06 | 2022-10-01 | Ocular Therapeutix Inc | Compositions and methods for treating ocular diseases |
US11344526B2 (en) | 2020-03-20 | 2022-05-31 | The Regents Of The University Of California | Implantable drug delivery devices for localized drug delivery |
US11338119B2 (en) | 2020-03-20 | 2022-05-24 | The Regents Of The University Of California | Implantable drug delivery devices for localized drug delivery |
US11173291B2 (en) | 2020-03-20 | 2021-11-16 | The Regents Of The University Of California | Implantable drug delivery devices for localized drug delivery |
HUE062928T2 (en) | 2020-03-25 | 2023-12-28 | Ocular Therapeutix Inc | Ocular implant containing a tyrosine kinase inhibitor |
US20210338481A1 (en) * | 2020-04-20 | 2021-11-04 | Bruce B. Becker | Lacrimal gland implant for drug delivery and method |
AU2021347318A1 (en) | 2020-09-24 | 2023-03-23 | Ocular Therapeutix, Inc. | Sustained release biodegradable intracanalicular inserts comprising a hydrogel and cyclosporine |
CA3209420A1 (en) | 2021-02-24 | 2022-09-01 | Peter Jarrett | Intracanalicular depot inserter device |
CN118190718A (en) * | 2024-03-15 | 2024-06-14 | 广州市纳爱生物科技有限公司 | An ophthalmic Chinese medicinal preparation and its active ingredient extraction method |
Citations (7)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US6225348B1 (en) * | 1998-08-20 | 2001-05-01 | Alfred W. Paulsen | Method of treating macular degeneration with a prostaglandin derivative |
US6416780B1 (en) * | 1997-05-07 | 2002-07-09 | Galen (Chemicals) Limited | Intravaginal drug delivery devices for the administration of testosterone and testosterone precursors |
US20040144392A1 (en) * | 2003-01-23 | 2004-07-29 | Mueller Richard L. | Breast nipple duct protective device |
US20040176341A1 (en) * | 2002-05-07 | 2004-09-09 | Kang-Jye Chou | Injectable sustained release delivery devices |
US20040208910A1 (en) * | 2000-04-26 | 2004-10-21 | Control Delivery Systems, Inc. | Sustained release device and method for ocular delivery of adrenergic agents |
US20050232972A1 (en) * | 2004-04-15 | 2005-10-20 | Steven Odrich | Drug delivery via punctal plug |
US20050244506A1 (en) * | 2004-04-30 | 2005-11-03 | Allergan, Inc. | Sustained release intraocular implants and methods for preventing retinal dysfunction |
Family Cites Families (237)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US3880991A (en) * | 1969-03-24 | 1975-04-29 | Brook David E | Polymeric article for dispensing drugs |
US3865108A (en) | 1971-05-17 | 1975-02-11 | Ortho Pharma Corp | Expandable drug delivery device |
US3828777A (en) | 1971-11-08 | 1974-08-13 | Alza Corp | Microporous ocular device |
US3949750A (en) * | 1974-10-07 | 1976-04-13 | Freeman Jerre M | Punctum plug and method for treating keratoconjunctivitis sicca (dry eye) and other ophthalmic aliments using same |
US4014335A (en) | 1975-04-21 | 1977-03-29 | Alza Corporation | Ocular drug delivery device |
US4281654A (en) | 1980-04-07 | 1981-08-04 | Alza Corporation | Drug delivery system for controlled ocular therapy |
US4304765A (en) * | 1980-10-14 | 1981-12-08 | Alza Corporation | Ocular insert housing steroid in two different therapeutic forms |
NZ200429A (en) * | 1981-04-30 | 1984-10-19 | Smith & Nephew Ass | Applicator for placing pharmaceutically active agent in contact with moist surface,e.g.,eye |
US4660546A (en) | 1984-11-07 | 1987-04-28 | Robert S. Herrick | Method for treating for deficiency of tears |
US5049142A (en) | 1984-11-07 | 1991-09-17 | Herrick Robert S | Intracanalicular implant for horizontal canalicular blockade treatment of the eye |
US5053030A (en) | 1984-11-07 | 1991-10-01 | Herrick Robert S | Intracanalicular implant for horizontal canalicular blockade treatment of the eye |
US5229128A (en) | 1986-06-11 | 1993-07-20 | Haddad Heskel M | Drug delivery ophthalmic insert and method of preparing same |
US5322691A (en) * | 1986-10-02 | 1994-06-21 | Sohrab Darougar | Ocular insert with anchoring protrusions |
US4747404A (en) * | 1986-11-10 | 1988-05-31 | Kresge Eye Institute Of Wayne State University | Foldable intraocular lens inserter |
US4886488A (en) | 1987-08-06 | 1989-12-12 | White Thomas C | Glaucoma drainage the lacrimal system and method |
GB8806367D0 (en) * | 1988-03-17 | 1988-04-13 | Erba Carlo Spa | Siloxane matrices with internal non-uniform drug distribution |
US4915684A (en) | 1988-06-21 | 1990-04-10 | Mackeen Donald L | Method and apparatus for modulating the flow of lacrimal fluid through a punctum and associated canaliculus |
US4915664A (en) | 1988-12-22 | 1990-04-10 | Erik Bakker | Toy glider with wing converging mechanism |
US5133159A (en) | 1989-01-13 | 1992-07-28 | Nestle S.A. | Method for polishing silicone products |
US4959048A (en) * | 1989-01-17 | 1990-09-25 | Helix Medical, Inc. | Lacrimal duct occluder |
US5098443A (en) | 1989-03-23 | 1992-03-24 | University Of Miami | Method of implanting intraocular and intraorbital implantable devices for the controlled release of pharmacological agents |
US5128058A (en) * | 1989-05-31 | 1992-07-07 | Hoya Corporation | Contact lens cleaner containing a microcapsular polishing agent |
IE910450A1 (en) | 1990-02-15 | 1991-08-28 | Bausch & Lomb | Soft contact lens processing aid |
US5171270A (en) | 1990-03-29 | 1992-12-15 | Herrick Robert S | Canalicular implant having a collapsible flared section and method |
US5163959A (en) * | 1990-03-29 | 1992-11-17 | Herrick Robert S | Method for treating an eye with a canalicular implant having a collapsible flared section |
US5041081A (en) | 1990-05-18 | 1991-08-20 | Odrich Ronald B | Ocular implant for controlling glaucoma |
US5116371A (en) | 1990-07-06 | 1992-05-26 | Christensen James M | Prosthesis with improved biocompatibility |
US5143724A (en) * | 1990-07-09 | 1992-09-01 | Biomatrix, Inc. | Biocompatible viscoelastic gel slurries, their preparation and use |
US5077033A (en) * | 1990-08-07 | 1991-12-31 | Mediventures Inc. | Ophthalmic drug delivery with thermo-irreversible gels of polxoxyalkylene polymer and ionic polysaccharide |
HU219594B (en) | 1991-12-27 | 2001-05-28 | Merck And Co. Inc. | A controlled release drug dispersion delivery device and process for producing the same |
US5283063A (en) * | 1992-01-31 | 1994-02-01 | Eagle Vision | Punctum plug method and apparatus |
US5334137A (en) | 1992-02-21 | 1994-08-02 | Eagle Vision, Inc. | Lacrimal fluid control device |
US5254089A (en) * | 1992-04-02 | 1993-10-19 | Boston Scientific Corp. | Medication dispensing balloon catheter |
US5178635A (en) | 1992-05-04 | 1993-01-12 | Allergan, Inc. | Method for determining amount of medication in an implantable device |
US5514379A (en) * | 1992-08-07 | 1996-05-07 | The General Hospital Corporation | Hydrogel compositions and methods of use |
US5469867A (en) * | 1992-09-02 | 1995-11-28 | Landec Corporation | Cast-in place thermoplastic channel occluder |
US5318513A (en) * | 1992-09-24 | 1994-06-07 | Leib Martin L | Canalicular balloon fixation stent |
FR2700265B1 (en) * | 1993-01-08 | 1995-03-31 | France Chirurgie Instr | Meatic plug for lacrimal pathology. |
US5707643A (en) * | 1993-02-26 | 1998-01-13 | Santen Pharmaceutical Co., Ltd. | Biodegradable scleral plug |
US6117907A (en) * | 1993-04-14 | 2000-09-12 | Sher; Neal A. | Topical treatment of ocular pain after corneal surgery |
US5824048A (en) | 1993-04-26 | 1998-10-20 | Medtronic, Inc. | Method for delivering a therapeutic substance to a body lumen |
US5417651A (en) | 1993-07-01 | 1995-05-23 | Guena; Nicolas | Punctum plug and monocanalicular probe for lacrimal pathology |
US5770589A (en) | 1993-07-27 | 1998-06-23 | The University Of Sydney | Treatment of macular degeneration |
US5423777A (en) | 1993-10-27 | 1995-06-13 | Tajiri; Akira | Punctum plug |
US5443505A (en) * | 1993-11-15 | 1995-08-22 | Oculex Pharmaceuticals, Inc. | Biocompatible ocular implants |
US6350781B1 (en) * | 1994-01-14 | 2002-02-26 | Lee Shahinia, Jr. | Method and analgesic preparations for sustained and extended corneal analgesia with subanesthetic concentrations of lidocaine |
US5466233A (en) | 1994-04-25 | 1995-11-14 | Escalon Ophthalmics, Inc. | Tack for intraocular drug delivery and method for inserting and removing same |
JP3486758B2 (en) | 1994-06-24 | 2004-01-13 | 株式会社高研 | Injectable lacrimal canaliculus |
JPH0878130A (en) | 1994-09-08 | 1996-03-22 | Wako:Kk | Method for burying ground electrode |
US6416760B2 (en) | 1995-01-26 | 2002-07-09 | Societe L'oreal | Therapeutic/cosmetic compositions comprising CGRP antagonists for treating sensitive human skin |
AU5857396A (en) * | 1995-05-14 | 1996-11-29 | Optonol Ltd. | Intraocular implant, delivery device, and method of implanta tion |
US6149684A (en) | 1995-06-07 | 2000-11-21 | Herrick; Robert S. | Punctum plug having a thin elongated lip and a distal starting tip and method of using |
US5723005A (en) | 1995-06-07 | 1998-03-03 | Herrick Family Limited Partnership | Punctum plug having a collapsible flared section and method |
JPH11507269A (en) * | 1995-06-07 | 1999-06-29 | ケラビジョン,インコーポレイテッド | Intrastromal corneal radial insert and insertion method |
US5766243A (en) | 1995-08-21 | 1998-06-16 | Oasis Medical, Inc. | Abrasive polished canalicular implant |
US5773019A (en) | 1995-09-27 | 1998-06-30 | The University Of Kentucky Research Foundation | Implantable controlled release device to deliver drugs directly to an internal portion of the body |
US5741292A (en) * | 1995-10-26 | 1998-04-21 | Eagle Vision | Punctum dilating and plug inserting instrument with push-button plug release |
US6441047B2 (en) | 1995-11-17 | 2002-08-27 | Alcon Manufacturing Ltd.. | Combination therapy for treating glaucoma |
WO1997020578A1 (en) * | 1995-12-04 | 1997-06-12 | University Of Miami | Non-preserved topical corticosteroid for treatment of dry eye, filamentary keratitis, and delayed tear clearance |
US5824073A (en) * | 1996-03-18 | 1998-10-20 | Peyman; Gholam A. | Macular indentor for use in the treatment of subretinal neovascular membranes |
FR2747033B1 (en) * | 1996-04-03 | 1998-05-22 | Parrat Michel Jesus Hubert | DYNAMIC MEATIC SHUTTER FOR LACRYMAL CANALICLES |
JP3675035B2 (en) | 1996-06-10 | 2005-07-27 | トヨタ自動車株式会社 | Fuel injection amount control device for internal combustion engine |
JPH1033584A (en) | 1996-07-26 | 1998-02-10 | M L C:Kk | Lacrimal duct insertion appliance |
US5928662A (en) * | 1996-07-31 | 1999-07-27 | Phillips; Andrew F. | Ocular drug delivery device |
CA2260992C (en) | 1996-08-20 | 2004-03-09 | The Regents Of The University Of California | Eye treatments using synthetic thyroid hormone compositions |
US5993407A (en) | 1996-10-25 | 1999-11-30 | Moazed; Kambiz Thomas | Transnasal lacrimal insert |
AU716980B2 (en) | 1996-11-01 | 2000-03-16 | Alcon Laboratories, Inc. | Cryogenic polishing method for soft acrylic articles |
JP2001509705A (en) | 1997-02-04 | 2001-07-24 | フエール,アラン | Screw-in tear tube cap |
US6027470A (en) | 1998-06-10 | 2000-02-22 | Eagle Vision, Inc. | Punctum plug and method for inserting the same into the punctual opening |
US6041785A (en) | 1997-03-27 | 2000-03-28 | Eaglevision, Inc. | Punctum plug |
US6082362A (en) * | 1997-03-27 | 2000-07-04 | Eagle Vision, Inc. | Punctum plug |
US6016806A (en) | 1997-03-27 | 2000-01-25 | Eaglevision, Inc | Punctum plug |
US5961370A (en) * | 1997-05-08 | 1999-10-05 | Chiron Vision Corporation | Intraocular lens tumbling process using coated beads |
MY125870A (en) * | 1997-07-25 | 2006-08-30 | Alza Corp | Osmotic delivery system flow modulator apparatus and method |
US6306426B1 (en) * | 1997-08-11 | 2001-10-23 | Allergan Sales, Inc. | Implant device with a retinoid for improved biocompatibility |
US5830171A (en) | 1997-08-12 | 1998-11-03 | Odyssey Medical, Inc. | Punctal occluder |
US5902598A (en) * | 1997-08-28 | 1999-05-11 | Control Delivery Systems, Inc. | Sustained release drug delivery devices |
US6060439A (en) * | 1997-09-29 | 2000-05-09 | Kyzen Corporation | Cleaning compositions and methods for cleaning resin and polymeric materials used in manufacture |
US6335335B2 (en) | 1997-11-05 | 2002-01-01 | Senju Pharmaceutical Co., Ltd. | Prolonged-action eye drop |
US5947974A (en) * | 1997-12-09 | 1999-09-07 | Allergan | Folding device and method for an intraocular lens |
US6646001B2 (en) | 1997-12-19 | 2003-11-11 | Alcon Manufacturing, Ltd. | Use of non-steroidal anti-inflammatory agents in combination with prostaglandin FP receptor agonists to treat glaucoma and ocular hypertension |
NL1008090C2 (en) | 1998-01-22 | 1999-07-26 | Lubberman Bernardus H M | Plug for closing a tear duct. |
WO1999044553A1 (en) | 1998-03-02 | 1999-09-10 | Herrick Family Limited Partnership | A punctum plug having a collapsible flared section and method |
US6290684B1 (en) * | 1998-03-02 | 2001-09-18 | Herrick Family Limited Partnership | Punctum plug having a collapsible expanded section and distal tip extending substantially perpendicular thereto and method of inserting same |
US6512747B1 (en) | 1998-03-05 | 2003-01-28 | Nippon Telegraph And Telephone Corporation | ATM transmission system |
US6196993B1 (en) * | 1998-04-20 | 2001-03-06 | Eyelab Group, Llc | Ophthalmic insert and method for sustained release of medication to the eye |
US6224630B1 (en) * | 1998-05-29 | 2001-05-01 | Advanced Bio Surfaces, Inc. | Implantable tissue repair device |
US6015433A (en) * | 1998-05-29 | 2000-01-18 | Micro Therapeutics, Inc. | Rolled stent with waveform perforation pattern |
US6306114B1 (en) * | 1998-06-16 | 2001-10-23 | Eagle Vision, Inc. | Valved canalicular plug for lacrimal duct occlusion |
US6117441A (en) * | 1998-07-02 | 2000-09-12 | The Population Council, Inc. | Silicone core long term androgen delivery implant |
ES2159209T3 (en) | 1998-07-14 | 2001-09-16 | Alcon Lab Inc | USE OF ACID 11- (3-DIMETHYLAMOPROPILIDEN) -6,11-DIHIDRODIBENZ (B, E) OXEPIN-2-ACETIC AND ITS PHARMACEUTICALLY ACCEPTABLE SALTS FOR THE MANUFACTURE OF A MEDICINAL PRODUCT FOR THE TREATMENT OF NON-ALBUM ADMINISTRATION OF OCULAR NEOVASCULARIZATION. |
JP2000070296A (en) | 1998-08-27 | 2000-03-07 | M L C:Kk | Intra-lacrimal duct intubation appliance |
US6095901A (en) | 1998-12-09 | 2000-08-01 | Alcon Laboratories, Inc. | Polishing method for soft acrylic articles |
US20040121014A1 (en) | 1999-03-22 | 2004-06-24 | Control Delivery Systems, Inc. | Method for treating and/or preventing retinal diseases with sustained release corticosteroids |
US6234175B1 (en) | 1999-03-23 | 2001-05-22 | Medennium, Inc. | Smart ocular plug design and method of insertion for punctal and intracanalicular implants |
US6383192B1 (en) * | 1999-04-28 | 2002-05-07 | Mlc Limited Company | Apparatus for intubation of lacrimal duct |
US6428502B1 (en) | 1999-06-25 | 2002-08-06 | Alcon Manufacturing, Ltd. | Punctal cannula |
US6706275B1 (en) * | 1999-09-08 | 2004-03-16 | Matthew W. Camp | Scleral plug system |
MXPA02002338A (en) * | 1999-10-21 | 2002-07-30 | Alcon Universal Ltd | Drug delivery device. |
US6331313B1 (en) * | 1999-10-22 | 2001-12-18 | Oculex Pharmaceticals, Inc. | Controlled-release biocompatible ocular drug delivery implant devices and methods |
US6264971B1 (en) * | 1999-11-04 | 2001-07-24 | Btg International Limited | Ocular insert |
US6566345B2 (en) | 2000-04-28 | 2003-05-20 | Fziomed, Inc. | Polyacid/polyalkylene oxide foams and gels and methods for their delivery |
US20050119737A1 (en) * | 2000-01-12 | 2005-06-02 | Bene Eric A. | Ocular implant and methods for making and using same |
US6344047B1 (en) * | 2000-02-02 | 2002-02-05 | Eagle Vision | Instrument for inserting a punctum plug and method for manufacturing the instrument |
US7708711B2 (en) | 2000-04-14 | 2010-05-04 | Glaukos Corporation | Ocular implant with therapeutic agents and methods thereof |
US7867186B2 (en) | 2002-04-08 | 2011-01-11 | Glaukos Corporation | Devices and methods for treatment of ocular disorders |
US6638239B1 (en) | 2000-04-14 | 2003-10-28 | Glaukos Corporation | Apparatus and method for treating glaucoma |
US20040175410A1 (en) * | 2000-04-26 | 2004-09-09 | Control Delivery Systems, Inc. | Sustained release device and method for ocular delivery of carbonic anhydrase inhibitors |
US6375972B1 (en) | 2000-04-26 | 2002-04-23 | Control Delivery Systems, Inc. | Sustained release drug delivery devices, methods of use, and methods of manufacturing thereof |
US6371122B1 (en) | 2000-06-20 | 2002-04-16 | Robert M. Mandelkorn | Gauge/dilator apparatus |
US6629533B1 (en) | 2000-06-30 | 2003-10-07 | Eagle Vision, Inc. | Punctum plug with at least one anchoring arm |
AU2001234337A1 (en) * | 2000-08-04 | 2002-02-18 | Medennium, Inc. | Ocular plug for punctal and intracanalicular implants |
US6534693B2 (en) | 2000-11-06 | 2003-03-18 | Afmedica, Inc. | Surgically implanted devices having reduced scar tissue formation |
EP1345588A2 (en) * | 2000-12-29 | 2003-09-24 | Bausch & Lomb Incorporated | Sustained release drug delivery devices |
US7041868B2 (en) * | 2000-12-29 | 2006-05-09 | Kimberly-Clark Worldwide, Inc. | Bioabsorbable wound dressing |
JP2004521882A (en) | 2001-01-03 | 2004-07-22 | ボシュ・アンド・ロム・インコーポレイテッド | Sustained release drug delivery device with assembled permeable plug |
EP1365738A2 (en) | 2001-01-26 | 2003-12-03 | Bausch & Lomb Incorporated | Improved process for the production of sustained release drug delivery devices |
US20020193441A1 (en) | 2001-02-21 | 2002-12-19 | Robertson Stella M. | Prostanoid therapies for the treatment of glaucoma |
US6713081B2 (en) | 2001-03-15 | 2004-03-30 | The United States Of America As Represented By The Department Of Health And Human Services | Ocular therapeutic agent delivery devices and methods for making and using such devices |
EP1977724A1 (en) | 2001-04-07 | 2008-10-08 | Glaukos Corporation | System for treating ocular disorders |
US6981958B1 (en) | 2001-05-02 | 2006-01-03 | Glaukos Corporation | Implant with pressure sensor for glaucoma treatment |
US7431710B2 (en) | 2002-04-08 | 2008-10-07 | Glaukos Corporation | Ocular implants with anchors and methods thereof |
US6605108B2 (en) * | 2001-04-13 | 2003-08-12 | Eagle Vision, Inc. | Monocanalicular stent |
US6982090B2 (en) * | 2001-05-10 | 2006-01-03 | Gillespie Donald E | More easily visualized punctum plug configurations |
US7404825B2 (en) | 2001-06-11 | 2008-07-29 | Herrick Ii Robert S | Implant capable of forming a differential image in an eye |
US6743439B1 (en) * | 2001-06-27 | 2004-06-01 | Alcon, Inc. | Ophthalmic compositions containing copolymers of sulfonated styrene and maleic anhydride |
WO2003009784A1 (en) * | 2001-07-23 | 2003-02-06 | Alcon, Inc. | Ophthalmic drug delivery device |
JP4346438B2 (en) * | 2001-08-03 | 2009-10-21 | グローコマ リサーチ テクノロジーズ,インコーポレイティッド | Methods and intrascleral implants for the treatment of glaucoma and presbyopia |
FR2829019B3 (en) | 2001-08-31 | 2003-10-31 | Alain Fouere | LACRYMAL PLUGS AND METHODS OF FITTING THESE DEVICES |
US20040234572A1 (en) | 2001-09-11 | 2004-11-25 | Martinod Serge R. | Preparation of sustained release pharmaceutical composition |
US6996063B2 (en) | 2001-11-16 | 2006-02-07 | Asustek Computer Inc. | Applicable PDU range test and calculation for window-based polling |
FR2833175B1 (en) | 2001-12-06 | 2004-05-14 | Sobem | FLOW CONTROL DEVICE FOR MEDICAL USE |
US7001615B1 (en) | 2001-12-07 | 2006-02-21 | Alcon, Inc. | Sustained release ophthalmic, otic and nasal suspension |
US6729939B2 (en) * | 2001-12-17 | 2004-05-04 | Bausch & Lomb Incorporated | Polishing method for intraocular lens |
FR2834446B1 (en) | 2002-01-08 | 2004-02-13 | Ioltechnologie Production | EXPANDING MEATIC NAIL |
US20050255564A1 (en) | 2002-01-18 | 2005-11-17 | Takara Bio Inc | Sulfated fucan |
GB2399753B (en) * | 2002-01-18 | 2006-04-19 | Michael E Snyder | Method of making a sustained release ophthalmological device |
TW200305424A (en) * | 2002-01-29 | 2003-11-01 | Santen Pharmaceutical Co Ltd | Glaucoma-treating agent comprising bunazosin and prostaglandin |
US7204995B2 (en) | 2002-01-31 | 2007-04-17 | El-Sherif Dalia M | Treatment and control of dry eye by use of biodegradable polymer capsules |
US20040116524A1 (en) * | 2002-02-04 | 2004-06-17 | Cohen Ben Z. | Method of administering opthalmic fluids |
RU2322233C2 (en) * | 2002-03-11 | 2008-04-20 | Алькон, Инк. | Implaned system for delivering medicinal preparations |
US20040147870A1 (en) * | 2002-04-08 | 2004-07-29 | Burns Thomas W. | Glaucoma treatment kit |
US9301875B2 (en) | 2002-04-08 | 2016-04-05 | Glaukos Corporation | Ocular disorder treatment implants with multiple opening |
CA2484632C (en) * | 2002-05-07 | 2012-12-11 | Control Delivery Systems, Inc. | Processes for forming a drug delivery device |
US20040043067A1 (en) | 2002-06-19 | 2004-03-04 | Salamone Joseph C. | Fluorosiloxane matrix controlled diffusion drug delivery systems |
US6866563B2 (en) * | 2002-06-27 | 2005-03-15 | Bausch & Lomb Incorporated | Apparatus and method for target polishing intraocular lenses |
FR2841770B1 (en) * | 2002-07-05 | 2004-10-01 | Ioltechnologie Production | MEATIC NAIL FOR SHUTTERING A LACRYMAL MEAT |
FR2844182B1 (en) | 2002-09-11 | 2004-12-03 | Humanoptics Ag | CLOSURE PLUG OF A LACRYMAL CANALICLE |
US7169163B2 (en) * | 2002-09-30 | 2007-01-30 | Bruce Becker | Transnasal method and catheter for lacrimal system |
US7785578B2 (en) | 2002-10-11 | 2010-08-31 | Aciont, Inc. | Non-invasive ocular drug delivery |
EP1411745B1 (en) | 2002-10-16 | 2007-08-08 | Alcatel Lucent | Packet switching for packet data transmission systems in a multi-channel radio arrangement |
US7354574B2 (en) * | 2002-11-07 | 2008-04-08 | Advanced Ocular Systems Limited | Treatment of ocular disease |
US7580394B2 (en) | 2002-11-27 | 2009-08-25 | Nokia Corporation | System and method for collision-free transmission scheduling in a network |
WO2004058289A1 (en) * | 2002-12-20 | 2004-07-15 | Chakshu Research, Inc. | Ophthalmic formulation for the prevention and treatment of ocular conditions |
WO2004066979A2 (en) * | 2003-01-24 | 2004-08-12 | Control Delivery Systems, Inc. | Sustained release device and method for ocular delivery of adrenergic agents |
AR043356A1 (en) * | 2003-01-24 | 2005-07-27 | Control Delivery Sys Inc | SUSTAINED RELEASE DEVICE FOR THE OCULAR ADMINISTRATION OF CARBON ANHYDRATION INHIBITORS AND USE OF CARBON ANHYDRATION INHIBITORS FOR PREPARATION |
US8149707B2 (en) | 2003-02-12 | 2012-04-03 | Rockstar Bidco, LP | Minimization of radio resource usage in multi-hop networks with multiple routings |
US20040170685A1 (en) | 2003-02-26 | 2004-09-02 | Medivas, Llc | Bioactive stents and methods for use thereof |
MXPA05009429A (en) * | 2003-03-05 | 2005-12-12 | Halozyme Inc | SOLUBLE HYALURONIDASE GLYCOPROTEIN (sHASEGP), PROCESS FOR PREPARING THE SAME, USES AND PHARMACEUTICAL COMPOSITIONS COMPRISING THEREOF. |
US20050283109A1 (en) | 2003-03-07 | 2005-12-22 | Peyman Gholam A | Method and apparatus for lacrimal canal obstruction |
US7065376B2 (en) | 2003-03-20 | 2006-06-20 | Microsoft Corporation | Multi-radio unification protocol |
US20040193095A1 (en) * | 2003-03-29 | 2004-09-30 | Shadduck John H. | Implants for treating ocular hypertension, methods of use and methods of fabrication |
US20050255144A1 (en) * | 2003-04-09 | 2005-11-17 | Directcontact Llc | Methods and articles for the delivery of medicaments to the eye for the treatment of posterior segment diseases |
EP1633320A2 (en) | 2003-05-02 | 2006-03-15 | SurModics, Inc. | Implantable controlled release bioactive agent delivery device |
US7204253B2 (en) | 2003-05-22 | 2007-04-17 | Clarity Corporation | Punctum plug |
US7017580B2 (en) | 2003-05-22 | 2006-03-28 | Clarity Corporation | Punctum plug system including a punctum plug and passive insertion tool therefor |
US20040236343A1 (en) | 2003-05-23 | 2004-11-25 | Taylor Jon B. | Insertion tool for ocular implant and method for using same |
US20050054723A1 (en) * | 2003-05-27 | 2005-03-10 | Johan Stjernschantz | Method for the treatment of glaucoma and ocular hypertension with prostaglandin analogues without melanogenic side effect |
JP4104137B2 (en) | 2003-05-30 | 2008-06-18 | 有限会社エム・エル・シー | Punctum plug |
US7662864B2 (en) * | 2003-06-04 | 2010-02-16 | Rutgers, The State University Of New Jersey | Solution polymerization processes to prepare a polymer that degrades to release a physiologically active agent |
JP4339635B2 (en) | 2003-06-12 | 2009-10-07 | 有限会社エム・エル・シー | Punctum plug |
US6994684B2 (en) | 2003-06-16 | 2006-02-07 | Alphamed Inc. | Punctum plugs having fluid collecting recesses and methods of punctal occlusion |
US20040265356A1 (en) | 2003-06-30 | 2004-12-30 | Bausch & Lomb Incorporated | Drug delivery device |
US20070043332A1 (en) | 2003-07-10 | 2007-02-22 | Galen (Chemiclas) Liimited | Intravaginal drug delivery devices |
JP4280128B2 (en) | 2003-08-19 | 2009-06-17 | 有限会社エム・エル・シー | Punctum plug |
CA2539324A1 (en) * | 2003-09-18 | 2005-03-31 | Macusight, Inc. | Transscleral delivery |
JP2005110765A (en) | 2003-10-03 | 2005-04-28 | M L C:Kk | Lacrimal punctum plug set |
EP1667705A1 (en) * | 2003-10-03 | 2006-06-14 | Allergan, Inc. | Compositions and methods comprising prostaglandin-related compounds and trefoil factor family peptides for the treatment of glaucoma with reduced hyperemia |
JP2005110930A (en) | 2003-10-07 | 2005-04-28 | M L C:Kk | Lacrimal punctum plug set |
US20050129731A1 (en) | 2003-11-03 | 2005-06-16 | Roland Horres | Biocompatible, biostable coating of medical surfaces |
US20050095269A1 (en) | 2003-11-04 | 2005-05-05 | Ainpour Parviz R. | Gel plug for blockage of the canaliculus |
PL1696822T3 (en) * | 2003-11-13 | 2010-08-31 | Psivida Inc | Injectable sustained release implant having a bioerodible matrix core and a bioerodible skin |
US7291125B2 (en) | 2003-11-14 | 2007-11-06 | Transcend Medical, Inc. | Ocular pressure regulation |
AU2003290471A1 (en) | 2003-12-17 | 2005-07-05 | Telefonaktiebolaget Lm Ericsson (Publ) | A method, system, terminal and computer program product for selecting radio access system in a multiaccess system |
WO2005064839A1 (en) | 2003-12-29 | 2005-07-14 | Electronics And Telecommunications Research Institute | Method for creating feedback message for arq in mobile communication system |
US20050220882A1 (en) | 2004-03-04 | 2005-10-06 | Wilson Pritchard | Materials for medical implants and occlusive devices |
US20050197614A1 (en) * | 2004-03-04 | 2005-09-08 | Wilson Pritchard | Occlusive biomedical devices, punctum plugs, and methods of use thereof |
JP2004202276A (en) | 2004-04-16 | 2004-07-22 | M L C:Kk | Intubator implement for reconstructing lacrimal passage |
JP2005312835A (en) | 2004-04-30 | 2005-11-10 | M L C:Kk | Lacrimal passage stent reinforced by thread |
US7799336B2 (en) * | 2004-04-30 | 2010-09-21 | Allergan, Inc. | Hypotensive lipid-containing biodegradable intraocular implants and related methods |
US20050244469A1 (en) | 2004-04-30 | 2005-11-03 | Allergan, Inc. | Extended therapeutic effect ocular implant treatments |
US20050244461A1 (en) * | 2004-04-30 | 2005-11-03 | Allergan, Inc. | Controlled release drug delivery systems and methods for treatment of an eye |
JP4644438B2 (en) | 2004-05-11 | 2011-03-02 | 有限会社エム・エル・シー | Brim lacrimal stent |
JP4510511B2 (en) | 2004-05-18 | 2010-07-28 | 有限会社エム・エル・シー | A lacrimal stent and lacrimal plug with reinforced collars |
EP3470108A1 (en) | 2004-07-02 | 2019-04-17 | Mati Therapeutics Inc. | Treatment medium delivery device for delivery of treatment media to the eye |
US7117870B2 (en) * | 2004-07-26 | 2006-10-10 | Clarity Corporation | Lacrimal insert having reservoir with controlled release of medication and method of manufacturing the same |
WO2006014793A1 (en) | 2004-07-26 | 2006-02-09 | Clarity Corporation | Implantable device having reservoir with controlled release of medication and method of manufacturing the same |
US20060020253A1 (en) | 2004-07-26 | 2006-01-26 | Prescott Anthony D | Implantable device having reservoir with controlled release of medication and method of manufacturing the same |
US20080038317A1 (en) * | 2004-09-10 | 2008-02-14 | Chin-Ming Chang | Therapeutic Lacrimal Canalicular Inserts And Related Methods |
US20060074370A1 (en) | 2004-09-24 | 2006-04-06 | Medennium, Inc. | Ocular occluder and method of insertion |
RU2007115853A (en) * | 2004-10-04 | 2008-11-10 | КьюЭлТи ЮЭсЭй, ИНК. (US) | COMPOSITION APPLICABLE AS AN IMPLANT WITH CONTROLLED RELEASE |
RU2007123604A (en) | 2004-11-24 | 2008-12-27 | Тэракайн Корпорэйшн (Us)Тэракайн Корпорэйшн (Us) | IMPLANT FOR INTERNAL EYE DELIVERY OF MEDICINES |
CN1790976A (en) | 2004-12-17 | 2006-06-21 | 松下电器产业株式会社 | Re-transmitting method for multi-antenna transmission |
US7986633B2 (en) | 2004-12-27 | 2011-07-26 | Lg Electronics Inc. | Method of controlling data transmission for multimedia and broadcasting services in a broadband wireless access system |
CN100394900C (en) * | 2005-02-02 | 2008-06-18 | 周星 | Spiral spring type artificial tear duct |
EP1699249B1 (en) | 2005-03-04 | 2007-06-20 | Matsushita Electric Industrial Co., Ltd. | Method and apparatus for the synchronisation of the physical layers in heterogeneous mobile communications networks |
US20060233858A1 (en) | 2005-03-08 | 2006-10-19 | Allergan, Inc. | Systems and methods providing targeted intraocular drug delivery |
WO2006122414A1 (en) * | 2005-05-17 | 2006-11-23 | Matregen Corp. | Depot for sustained and controlled delivery of methotrexate |
US20060292099A1 (en) * | 2005-05-25 | 2006-12-28 | Michael Milburn | Treatment of eye disorders with sirtuin modulators |
WO2007009061A2 (en) * | 2005-07-13 | 2007-01-18 | Anthrogenesis Corporation | Ocular plug formed from placenta derived collagen biofabric |
US7862532B2 (en) | 2005-10-07 | 2011-01-04 | Delta Life Sciences, Inc. | Punctum plugs having insertion guides and strengthening beams |
US20070088444A1 (en) * | 2005-10-13 | 2007-04-19 | Robert A Hodorek | Method for repairing a bone defect using a formable implant which hardens in vivo |
US20070132125A1 (en) | 2005-12-08 | 2007-06-14 | Bausch & Lomb Incorporated | Use of a super-cooled fluid in lens processing |
JP4078371B2 (en) | 2006-01-27 | 2008-04-23 | 章弘 小栗 | Punctum plug |
BRPI0709672B8 (en) | 2006-03-31 | 2021-06-22 | 3088922 Inc | ocular implant insertable into an ocular lumen and method of delivering a therapeutic agent to an eye |
US20080045911A1 (en) | 2006-06-21 | 2008-02-21 | Borgia Maureen J | Punctal plugs for the delivery of active agents |
US9474645B2 (en) | 2006-06-21 | 2016-10-25 | Johnson & Johnson Vision Care, Inc. | Punctal plugs for the delivery of active agents |
US9173773B2 (en) | 2006-06-21 | 2015-11-03 | Johnson & Johnson Vision Care, Inc. | Punctal plugs for the delivery of active agents |
CA2657380A1 (en) * | 2006-07-20 | 2008-01-24 | Neurosystec Corporation | Devices, systems and methods for ophthalmic drug delivery |
FR2908042B1 (en) | 2006-11-08 | 2009-06-05 | Bruno Fayet | MONOCANALICULONASAL AND / OR MONOCANALICULAR INTUBATION ASSEMBLY, IN PARTICULAR FOR LACRYMONASAL IMPERFORATION. |
CA2674076A1 (en) * | 2006-12-26 | 2008-07-10 | Qlt Plug Delivery, Inc. | Drug delivery implants for inhibition of optical defects |
UY30883A1 (en) | 2007-01-31 | 2008-05-31 | Alcon Res | PUNCTURAL PLUGS AND METHODS OF RELEASE OF THERAPEUTIC AGENTS |
US20080299176A1 (en) | 2007-05-30 | 2008-12-04 | Yu-Chin Lai | Drug delivery device comprising crosslinked polyurethane-siloxane-containing copolymers |
AU2008300022A1 (en) | 2007-09-07 | 2009-03-19 | Qlt Inc. | Lacrimal implant detection |
WO2009035565A1 (en) | 2007-09-07 | 2009-03-19 | Qlt Plug Delivery, Inc | Prostaglandin analogues for implant devices and methods |
DK2207529T3 (en) | 2007-09-07 | 2015-03-09 | Mati Therapeutics Inc | PHARMACEUTICAL cores for the sustained release of therapeutic agents |
KR20100058620A (en) * | 2007-09-07 | 2010-06-03 | 큐엘티 플러그 딜리버리, 인코포레이티드 | Insertion and extraction tools for lacrimal implants |
EP2865361B1 (en) | 2007-09-07 | 2019-05-22 | Mati Therapeutics Inc. | Lacrimal implants and related methods |
WO2009105178A2 (en) | 2008-02-18 | 2009-08-27 | Qlt Plug Delivery, Inc. | Lacrimal implants and related methods |
CN104623741A (en) | 2008-04-30 | 2015-05-20 | 马缇医疗股份有限公司 | Composite lacrimal insert and related methods |
JP2011520805A (en) | 2008-05-09 | 2011-07-21 | キューエルティー プラグ デリバリー,インク. | Continuous delivery of active agents for the treatment of glaucoma and ocular hypertension |
CN102119075A (en) | 2008-05-30 | 2011-07-06 | Qlt栓塞输送公司 | Surface treated implantable articles and related methods |
JP2011525388A (en) | 2008-06-24 | 2011-09-22 | キューエルティー プラグ デリバリー,インク. | Combination treatment for glaucoma |
TW201006453A (en) | 2008-07-08 | 2010-02-16 | Qlt Plug Delivery Inc | Lacrimal implant body including comforting agent |
WO2010071844A1 (en) | 2008-12-19 | 2010-06-24 | Qlt Plug Delivery, Inc | Substance delivering punctum implants and methods |
RU2011134043A (en) | 2009-01-23 | 2013-02-20 | Клт Инк. | DELIVERY OF ONE OR MORE AGENT WITH LONG-TERM RELEASE |
WO2010096822A2 (en) | 2009-02-23 | 2010-08-26 | Qlt Plug Delivery, Inc. | Lacrimal implants and related methods |
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- 2018-05-11 JP JP2018091793A patent/JP2018187396A/en active Pending
- 2018-10-23 US US16/168,554 patent/US10300014B2/en active Active
- 2018-10-23 US US16/168,335 patent/US11406592B2/en active Active
-
2019
- 2019-08-02 JP JP2019142914A patent/JP2019213885A/en active Pending
- 2019-08-19 US US16/544,884 patent/US10874606B2/en active Active
-
2020
- 2020-12-24 US US17/133,980 patent/US20210212941A1/en active Pending
-
2021
- 2021-05-17 JP JP2021082984A patent/JP7273891B2/en active Active
-
2022
- 2022-08-06 US US17/882,552 patent/US20230165791A1/en not_active Abandoned
Patent Citations (7)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US6416780B1 (en) * | 1997-05-07 | 2002-07-09 | Galen (Chemicals) Limited | Intravaginal drug delivery devices for the administration of testosterone and testosterone precursors |
US6225348B1 (en) * | 1998-08-20 | 2001-05-01 | Alfred W. Paulsen | Method of treating macular degeneration with a prostaglandin derivative |
US20040208910A1 (en) * | 2000-04-26 | 2004-10-21 | Control Delivery Systems, Inc. | Sustained release device and method for ocular delivery of adrenergic agents |
US20040176341A1 (en) * | 2002-05-07 | 2004-09-09 | Kang-Jye Chou | Injectable sustained release delivery devices |
US20040144392A1 (en) * | 2003-01-23 | 2004-07-29 | Mueller Richard L. | Breast nipple duct protective device |
US20050232972A1 (en) * | 2004-04-15 | 2005-10-20 | Steven Odrich | Drug delivery via punctal plug |
US20050244506A1 (en) * | 2004-04-30 | 2005-11-03 | Allergan, Inc. | Sustained release intraocular implants and methods for preventing retinal dysfunction |
Cited By (119)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US10406029B2 (en) | 2001-04-07 | 2019-09-10 | Glaukos Corporation | Ocular system with anchoring implant and therapeutic agent |
US20100040670A1 (en) * | 2004-04-15 | 2010-02-18 | Qlt Plug Delivery, Inc. | Drug delivery via ocular implant |
US20050232972A1 (en) * | 2004-04-15 | 2005-10-20 | Steven Odrich | Drug delivery via punctal plug |
US9463114B2 (en) | 2004-04-15 | 2016-10-11 | Mati Therapeutics Inc. | Punctal plug with active agent |
US9820884B2 (en) | 2004-07-02 | 2017-11-21 | Mati Therapeutics Inc. | Treatment medium delivery device and methods for delivery of such treatment mediums to the eye using such delivery device |
US10610407B2 (en) | 2004-07-02 | 2020-04-07 | Mati Therapeutics Inc. | Treatment medium delivery device and methods for delivery of such treatment mediums to the eye using such delivery device |
US9180045B2 (en) | 2004-07-02 | 2015-11-10 | Mati Therapeutics Inc. | Treatment medium delivery device and methods for delivery of such treatment mediums to the eye using such a delivery device |
US20090118702A1 (en) * | 2004-07-02 | 2009-05-07 | Forsight Labs, Llc | Treatment Medium Delivery Device and Methods for Delivery of Such Treatment Mediums to the Eye Using such a Delivery Device |
US7922702B2 (en) | 2004-07-02 | 2011-04-12 | Qlt Inc. | Treatment medium delivery device and methods for delivery of such treatment mediums to the eye using such a delivery device |
US20070212397A1 (en) * | 2005-09-15 | 2007-09-13 | Roth Daniel B | Pharmaceutical delivery device and method for providing ocular treatment |
US8900620B2 (en) | 2005-10-13 | 2014-12-02 | DePuy Synthes Products, LLC | Drug-impregnated encasement |
US10814112B2 (en) | 2005-10-13 | 2020-10-27 | DePuy Synthes Products, Inc. | Drug-impregnated encasement |
US9579260B2 (en) | 2005-10-13 | 2017-02-28 | DePuy Synthes Products, Inc. | Drug-impregnated encasement |
US20070243230A1 (en) * | 2006-03-31 | 2007-10-18 | Forsight Labs, Llc | Nasolacrimal Drainage System Implants for Drug Therapy |
US10874606B2 (en) | 2006-03-31 | 2020-12-29 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US9849082B2 (en) | 2006-03-31 | 2017-12-26 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US9168222B2 (en) | 2006-03-31 | 2015-10-27 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US11406592B2 (en) | 2006-03-31 | 2022-08-09 | Mati Therapeutics Inc. | Drug delivery methods, structures, and compositions for nasolacrimal system |
US10383817B2 (en) | 2006-03-31 | 2019-08-20 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US7998497B2 (en) | 2006-03-31 | 2011-08-16 | Qlt Inc. | Nasolacrimal drainage system implants for drug therapy |
US8691265B2 (en) | 2006-03-31 | 2014-04-08 | Mati Therapeutics, Inc. | Drug delivery methods, structures, and compositions for nasolacrimal system |
US9610194B2 (en) | 2006-03-31 | 2017-04-04 | Mati Therapeutics Inc. | Drug delivery methods, structures, and compositions for nasolacrimal system |
US10300014B2 (en) | 2006-03-31 | 2019-05-28 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US8747884B2 (en) | 2006-03-31 | 2014-06-10 | Mati Therapeutics Inc. | Nasolacrimal drainage system implants for drug therapy |
US8628792B2 (en) | 2007-09-07 | 2014-01-14 | Mati Therapeutics, Inc. | Drug cores for sustained release of therapeutic agents |
US20090104243A1 (en) * | 2007-09-07 | 2009-04-23 | Qlt Plug Delivery, Inc. - Qpdi | Drug cores for sustained release of therapeutic agents |
US11141312B2 (en) | 2007-09-07 | 2021-10-12 | Mati Therapeutics Inc. | Lacrimal implant detection |
US20100034870A1 (en) * | 2008-04-30 | 2010-02-11 | QLT. Plug Delivery, Inc. | Composite lacrimal insert and related methods |
US9764066B2 (en) | 2008-04-30 | 2017-09-19 | Mati Therapeutics Inc. | Composite lacrimal insert and related methods |
US9132088B2 (en) | 2008-04-30 | 2015-09-15 | Mati Therapeutics Inc. | Composite lacrimal insert and related methods |
US9949942B2 (en) | 2008-05-09 | 2018-04-24 | Mati Therapeutics Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US20090280158A1 (en) * | 2008-05-09 | 2009-11-12 | Qlt Plug Delivery, Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US20090318549A1 (en) * | 2008-06-24 | 2009-12-24 | Qlt Plug Delivery, Inc. | Combination treatment of glaucoma |
US20100274224A1 (en) * | 2008-07-08 | 2010-10-28 | Qlt Plug Delivery, Inc. | Lacrimal implant body including comforting agent |
US8298578B2 (en) | 2009-01-29 | 2012-10-30 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US9851351B2 (en) | 2009-01-29 | 2017-12-26 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US8277830B2 (en) | 2009-01-29 | 2012-10-02 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US10813788B2 (en) | 2009-01-29 | 2020-10-27 | Forsight Vision4, Inc. | Implantable therapeutic device |
US9417238B2 (en) | 2009-01-29 | 2016-08-16 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US9066779B2 (en) | 2009-01-29 | 2015-06-30 | Forsight Vision4, Inc. | Implantable therapeutic device |
US8808727B2 (en) | 2009-01-29 | 2014-08-19 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US8399006B2 (en) | 2009-01-29 | 2013-03-19 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US11642310B2 (en) | 2009-01-29 | 2023-05-09 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US10656152B2 (en) | 2009-01-29 | 2020-05-19 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US8795712B2 (en) | 2009-01-29 | 2014-08-05 | Forsight Vision4, Inc. | Posterior segment drug delivery |
US11426306B2 (en) | 2009-05-18 | 2022-08-30 | Dose Medical Corporation | Implants with controlled drug delivery features and methods of using same |
US10206813B2 (en) | 2009-05-18 | 2019-02-19 | Dose Medical Corporation | Implants with controlled drug delivery features and methods of using same |
AU2010256558B2 (en) * | 2009-06-03 | 2013-10-03 | Forsight Labs, Llc | Anterior segment drug delivery |
KR101429881B1 (en) * | 2009-06-03 | 2014-08-13 | 포사이트 비젼4, 인크. | Anterior segment drug delivery |
US9421126B2 (en) | 2009-06-03 | 2016-08-23 | Forsight Vision5, Inc. | Anterior segment drug delivery |
US10004636B2 (en) | 2009-06-03 | 2018-06-26 | Forsight Vision5, Inc. | Anterior segment drug delivery |
CN102596097A (en) * | 2009-06-03 | 2012-07-18 | 弗赛特实验室有限责任公司 | Anterior segment drug delivery |
US10736774B2 (en) | 2009-06-03 | 2020-08-11 | Forsight Vision5, Inc. | Anterior segment drug delivery |
WO2010141729A1 (en) * | 2009-06-03 | 2010-12-09 | Forsight Labs, Llc | Anterior segment drug delivery |
US8623395B2 (en) | 2010-01-29 | 2014-01-07 | Forsight Vision4, Inc. | Implantable therapeutic device |
US10166142B2 (en) | 2010-01-29 | 2019-01-01 | Forsight Vision4, Inc. | Small molecule delivery with implantable therapeutic device |
US8939948B2 (en) | 2010-06-01 | 2015-01-27 | Forsight Vision5, Inc. | Ocular insert apparatus and methods |
US9937073B2 (en) | 2010-06-01 | 2018-04-10 | Forsight Vision5, Inc. | Ocular insert apparatus and methods |
US8905963B2 (en) | 2010-08-05 | 2014-12-09 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
US9861521B2 (en) | 2010-08-05 | 2018-01-09 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
US11786396B2 (en) | 2010-08-05 | 2023-10-17 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
US11679027B2 (en) | 2010-08-05 | 2023-06-20 | Forsight Vision4, Inc. | Combined drug delivery methods and apparatus |
US9033911B2 (en) | 2010-08-05 | 2015-05-19 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
US9492315B2 (en) | 2010-08-05 | 2016-11-15 | Forsight Vision4, Inc. | Implantable therapeutic device |
US10617557B2 (en) | 2010-08-05 | 2020-04-14 | Forsight Vision4, Inc. | Combined drug delivery methods and apparatus |
US10265215B2 (en) | 2010-08-05 | 2019-04-23 | Forsight Vision4, Inc. | Injector apparatus and method for drug delivery |
US11065151B2 (en) | 2010-11-19 | 2021-07-20 | Forsight Vision4, Inc. | Therapeutic agent formulations for implanted devices |
US10874548B2 (en) | 2010-11-19 | 2020-12-29 | Forsight Vision4, Inc. | Therapeutic agent formulations for implanted devices |
US8715713B2 (en) | 2011-04-29 | 2014-05-06 | Allergan, Inc. | Solvent cast film sustained release latanoprost implant |
US9161929B2 (en) | 2011-04-29 | 2015-10-20 | Allergan, Inc. | Solvent cast film sustained release latanoprost implant |
US10245178B1 (en) | 2011-06-07 | 2019-04-02 | Glaukos Corporation | Anterior chamber drug-eluting ocular implant |
US10398592B2 (en) | 2011-06-28 | 2019-09-03 | Forsight Vision4, Inc. | Diagnostic methods and apparatus |
US11813196B2 (en) | 2011-06-28 | 2023-11-14 | Forsight Vision4, Inc. | Diagnostic methods and apparatus |
US9610271B2 (en) | 2011-08-29 | 2017-04-04 | Mati Therapeutics Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US9974685B2 (en) | 2011-08-29 | 2018-05-22 | Mati Therapeutics | Drug delivery system and methods of treating open angle glaucoma and ocular hypertension |
US10632012B2 (en) | 2011-08-29 | 2020-04-28 | Mati Therapeutics Inc. | Sustained release delivery of active agents to treat glaucoma and ocular hypertension |
US8715712B2 (en) | 2011-09-14 | 2014-05-06 | Forsight Vision5, Inc. | Ocular insert apparatus and methods |
US10835416B2 (en) | 2011-09-14 | 2020-11-17 | Forsight Vision5, Inc. | Ocular insert apparatus and methods |
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US10653554B2 (en) | 2011-09-16 | 2020-05-19 | Forsight Vision4, Inc. | Fluid exchange apparatus and methods |
US9381683B2 (en) | 2011-12-28 | 2016-07-05 | DePuy Synthes Products, Inc. | Films and methods of manufacture |
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US10456293B2 (en) | 2012-10-26 | 2019-10-29 | Forsight Vision5, Inc. | Ophthalmic system for sustained release of drug to eye |
US10195078B2 (en) | 2013-02-19 | 2019-02-05 | Aquesys, Inc. | Adjustable intraocular flow regulation |
US10195079B2 (en) | 2013-02-19 | 2019-02-05 | Aquesys, Inc. | Adjustable intraocular implant |
US9968603B2 (en) | 2013-03-14 | 2018-05-15 | Forsight Vision4, Inc. | Systems for sustained intraocular delivery of low solubility compounds from a port delivery system implant |
US11253394B2 (en) | 2013-03-15 | 2022-02-22 | Dose Medical Corporation | Controlled drug delivery ocular implants and methods of using same |
US12115102B2 (en) | 2013-03-28 | 2024-10-15 | Forsight Vision4, Inc. | Ophthalmic implant for delivering therapeutic substances |
US11510810B2 (en) | 2013-03-28 | 2022-11-29 | Forsight Vision4, Inc. | Ophthalmic implant for delivering therapeutic substances |
US9526654B2 (en) | 2013-03-28 | 2016-12-27 | Forsight Vision4, Inc. | Ophthalmic implant for delivering therapeutic substances |
US10398593B2 (en) | 2013-03-28 | 2019-09-03 | Forsight Vision4, Inc. | Ophthalmic implant for delivering therapeutic substances |
US10500304B2 (en) | 2013-06-21 | 2019-12-10 | DePuy Synthes Products, Inc. | Films and methods of manufacture |
US10959941B2 (en) | 2014-05-29 | 2021-03-30 | Glaukos Corporation | Implants with controlled drug delivery features and methods of using same |
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US11337853B2 (en) | 2014-07-15 | 2022-05-24 | Forsight Vision4, Inc. | Ocular implant delivery device and method |
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US10363255B2 (en) | 2014-08-08 | 2019-07-30 | Forsight Vision4, Inc. | Stable and soluble formulations of receptor tyrosine kinase inhibitors, and methods of preparation thereof |
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US11110001B2 (en) | 2014-11-10 | 2021-09-07 | Forsight Vision4, Inc. | Expandable drug delivery devices and methods of use |
US10500091B2 (en) | 2014-11-10 | 2019-12-10 | Forsight Vision4, Inc. | Expandable drug delivery devices and methods of use |
WO2016083891A1 (en) * | 2014-11-25 | 2016-06-02 | Eyal Sheetrit | Compositions and methods for delivering a bio-active agent or bio-active agents |
EP3223793A4 (en) * | 2014-11-25 | 2018-08-01 | Eximore Ltd. | Compositions and methods for delivering a bio-active agent or bio-active agents |
US10471070B2 (en) * | 2014-11-25 | 2019-11-12 | Eyal Sheetrit | Methods for delivering a bio-active agent or bio-active agents to an eye of a mammal |
US11224602B2 (en) | 2015-04-13 | 2022-01-18 | Forsight Vision5, Inc. | Ocular insert composition of a semi-crystalline or crystalline pharmaceutically active agent |
US10004634B2 (en) | 2015-06-16 | 2018-06-26 | The Regents Of The University Of Colorado | Nasolacrimal implants and related methods for tear stimulation |
US10004635B2 (en) | 2015-06-16 | 2018-06-26 | The Regents Of The University Of Colorado | Nasolacrimal implants and related methods for tear stimulation |
US11925578B2 (en) | 2015-09-02 | 2024-03-12 | Glaukos Corporation | Drug delivery implants with bi-directional delivery capacity |
US11564833B2 (en) | 2015-09-25 | 2023-01-31 | Glaukos Corporation | Punctal implants with controlled drug delivery features and methods of using same |
US11432959B2 (en) | 2015-11-20 | 2022-09-06 | Forsight Vision4, Inc. | Porous structures for extended release drug delivery devices |
US11617680B2 (en) | 2016-04-05 | 2023-04-04 | Forsight Vision4, Inc. | Implantable ocular drug delivery devices |
US12102560B2 (en) | 2016-04-05 | 2024-10-01 | Forsight Vision4, Inc. | Implantable ocular drug delivery devices |
US11318043B2 (en) | 2016-04-20 | 2022-05-03 | Dose Medical Corporation | Bioresorbable ocular drug delivery device |
US11419759B2 (en) | 2017-11-21 | 2022-08-23 | Forsight Vision4, Inc. | Fluid exchange apparatus for expandable port delivery system and methods of use |
USD1033637S1 (en) | 2022-01-24 | 2024-07-02 | Forsight Vision4, Inc. | Fluid exchange device |
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