WO2012019139A1 - Combined drug delivery methods and apparatus - Google Patents
Combined drug delivery methods and apparatus Download PDFInfo
- Publication number
- WO2012019139A1 WO2012019139A1 PCT/US2011/046817 US2011046817W WO2012019139A1 WO 2012019139 A1 WO2012019139 A1 WO 2012019139A1 US 2011046817 W US2011046817 W US 2011046817W WO 2012019139 A1 WO2012019139 A1 WO 2012019139A1
- Authority
- WO
- WIPO (PCT)
- Prior art keywords
- therapeutic agent
- therapeutic
- inhibitor
- release
- reservoir
- Prior art date
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Classifications
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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
- 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
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/74—Synthetic polymeric materials
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K45/00—Medicinal preparations containing active ingredients not provided for in groups A61K31/00 - A61K41/00
- A61K45/06—Mixtures of active ingredients without chemical characterisation, e.g. antiphlogistics and cardiaca
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/0012—Galenical forms characterised by the site of application
- A61K9/0048—Eye, e.g. artificial tears
- A61K9/0051—Ocular inserts, ocular implants
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P27/00—Drugs for disorders of the senses
- A61P27/02—Ophthalmic agents
-
- 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
- A61F2250/00—Special features of prostheses classified in groups A61F2/00 - A61F2/26 or A61F2/82 or A61F9/00 or A61F11/00 or subgroups thereof
- A61F2250/0058—Additional features; Implant or prostheses properties not otherwise provided for
- A61F2250/0067—Means for introducing or releasing pharmaceutical products into the body
- A61F2250/0068—Means for introducing or releasing pharmaceutical products into the body the pharmaceutical product being in a reservoir
Definitions
- the present invention relates to delivery of therapeutic agents to the posterior segment of the eye.
- embodiments of the present invention can be used to deliver many therapeutic agents to many tissues of the body.
- embodiments of the present invention can be used to deliver therapeutic agent to one or more of the following tissues: intravascular, intra-articular, intrathecal, pericardial, intraluminal and gut.
- the proposed implanted devices may permit an injection into the device, one potential problem is that an injection into an implanted device can cause at least some risk of infection for the patient in at least some instances. Also, in at least some instances the drug release rate of an implanted device can change over time, such that the release rate of the drug can be less than ideal after injection in at least some instance. At least some of the proposed implanted devices may not be implanted so as to minimize the risk of infection to the patient. For example, at least some of the proposed devices that rely on pores and capillaries may allow microbes such as bacteria to pass through the capillary and/or pore, such that infection may be spread in at least some instances. Also, work in relation to embodiments of the present invention suggests that at least some of the proposed implanted devices do not provide adequate protection from the patient's immune system, such as from macrophages and antibodies, thereby limiting the therapeutic effect in at least some instances.
- Embodiments of the present invention provide therapeutic devices to deliver therapeutic amounts of one or more of a first therapeutic agent or a second therapeutic agent for an extended time to the posterior segment of the eye, for example an extended time of at least about 1 month.
- the first therapeutic agent may comprise an anti-neoplastic agent, such as an agent to inhibit neovascularization, for example a VEGF inhibitor.
- the second therapeutic agent may comprise an anti-inflammatory, for example a cyclooxygenase (hereinafter "COX”) inhibitor.
- COX cyclooxygenase
- the therapeutic device may be helpful to reduce the frequency of negative side effects associated with direct intraocular injection such as pain, retinal detachment, hemorrhaging and infection because injections can be made less frequently and can be made into the reservoir chamber of the device rather than into the eye.
- the therapeutic device can be configured to replace the therapeutic agent when the device is implanted at least partially within the eye of the patient.
- the therapeutic device may be implanted in the eye so as to extend through the sclera of the eye, and the therapeutic device may comprise a container and a port or penetrable barrier configured to receive a quantity of therapeutic agent.
- the therapeutic agent can be placed in the container in many ways, for example by placing a solid insert through the port to the inside of the container or by injecting a formulation of the therapeutic agent through the penetrable barrier into the container.
- the first therapeutic device may comprise the first therapeutic agent and the second therapeutic agent, such that the first therapeutic agent and the second therapeutic agent can be delivered from the first therapeutic device and the second therapeutic device may not be used in many embodiments.
- the first therapeutic agent may comprise an anti-neoplastic agent such as a VEGF inhibitor
- the second therapeutic agent may comprise an anti-inflammatory such as non-steroidal anti -inflammatory, for example a cyclooxygenase inhibitor.
- the reservoir of the therapeutic device is fiushable and/or refillable. This provides the added benefit that the physician may remove the therapeutic agent from the patient by flushing the agent from the reservoir of the therapeutic device rather than waiting for the therapeutic agent to be eliminated from the patient. This removal can be advantageous in cases where the patient has an adverse drug reaction or benefit from a pause in therapy sometimes referred to as a drug holiday.
- the volume of the reservoir and release rate of the porous structure can be tuned to receive a volume of a commercially available formulation, such that the therapeutic agent can be released for an extended time.
- embodiments provide a method of treating an eye having a sclera and a vitreous humor.
- a first therapeutic amount of a first therapeutic agent is delivered to the vitreous humor of the eye, in which the first therapeutic agent effective for a first extended time.
- a second therapeutic amount of a second therapeutic agent is delivered, and the second therapeutic agent effective for a second extended time.
- the COX inhibitor comprises one or more of a salicylic acid derivative, a propionic acid derivative, an acetic acid derivative, and enolic acid (hereinafter “Oxicam”) derivative, a fenamic acid derivative, a selective COX -2 inhibitor (hereinafter “Coxibs").
- Oxicam enolic acid
- Coxibs selective COX -2 inhibitor
- the inflammatory response inhibitor comprises the acetic acid derivative and wherein the acetic acid derivative comprises one or more of Indomethacin, Sulindac, Etodolac, Diclofenac or Nabumetone.
- the inflammatory response inhibitor comprises the Enolic acid (hereinafter "Oxicam”) derivatives and wherein the Enolic acid derivative comprises one or more of Piroxicam, Meloxicam, Tenoxicam, Droxicam, Lornoxicam, or Isoxicam.
- the inflammatory response inhibitor comprises the Selective COX-2 inhibitor (hereinafter "Coxibs") and wherein the Selective COX-2 inhibitor comprises one or more of Celecoxib, Rofecoxib, Valdecoxib, Parecoxib, Lumiracoxib, or Etoricoxib.
- the first therapeutic agent is injected into the vitreous humor of the eye.
- the second therapeutic agent is injected into the vitreous humor of the eye.
- the first therapeutic agent is injected into a chamber of the container when the container is coupled to the vitreous humor and the sclera and wherein the container is configured with a porous structure and a volume to release the first therapeutic amounts of the first therapeutic agent from the chamber into the vitreous humor for the first extended time.
- the second therapeutic agent is injected into a chamber of the container when the container is coupled to the vitreous humor and the sclera.
- the first therapeutic agent comprises a VEGF inhibitor and the second therapeutic agent comprises a cyclooxygenase inhibitor.
- the cyclooxygenase inhibitor comprises a solid coupled to the container to release the second therapeutic agent for the extended time.
- the solid cyclooxygenase inhibitor is located within the chamber of the container and released through the porous structure.
- the solid cyclooxygenase inhibitor is located within a second chamber of the container and released through a second porous structure. [0037] In many embodiments, the second chamber is separated from the first chamber.
- the second chamber is coupled to the first chamber with the first porous structure and coupled to the vitreous with the second porous structure such that the first therapeutic agent passes through the first porous structure and second porous structure to reach the vitreous humor.
- the solid cyclooxygenase inhibitor is located away from the chamber and coupled to the vitreous humor.
- the container is configured to release the therapeutic amounts of the first therapeutic agent into the vitreous humor for the first extended time.
- the first therapeutic agent comprises a vascular growth inhibitor effective for the first extended time and wherein the second therapeutic agent comprises an antifibrotic agent effective for the second amount of time.
- the TNF inhibitor comprises pentoxifylline effective for the second extended time.
- the first therapeutic agent comprises a vascular growth inhibitor effective for the first extended time and wherein the second therapeutic agent comprises a dual COX/LOX inhibitor effective for the second extended time.
- the dual COX/LOX inhibitor comprises Licofelone.
- the first therapeutic agent comprises a vascular growth inhibitor effective for the first extended time and wherein the second therapeutic agent comprises an antihistamine.
- the antihistamine comprises azelastine.
- the antihistamine comprises an H3-receptor antagonist.
- the H4-receptor antagonist comprises one or more of
- inventions provide an apparatus to treat an eye having a sclera and a vitreous humor.
- a therapeutic device is configured to couple to the sclera.
- the therapeutic device comprises a first container to hold a first therapeutic agent, and the first container has a second therapeutic agent with in the container to release therapeutic amounts of the second therapeutic agent into the vitreous humor for a second extended time when the therapeutic device is inserted into the eye.
- an apparatus to treat an eye having a sclera and a vitreous humor comprises a first container to hold a first therapeutic agent and a second container to hold a second therapeutic agent.
- the first container is configured to release first therapeutic amounts of the first therapeutic agent into the vitreous humor for a first extended time
- the second container is configured to release second therapeutic amounts of the second therapeutic agent into the vitreous humor for a second extended time.
- an apparatus to treat an eye having a sclera and a vitreous humor comprises a first therapeutic device and a second therapeutic device.
- the first therapeutic device and the second therapeutic device each comprises a portion to couple to the sclera having an oval cross section sized to fit an incision extending along the pars plana.
- the first therapeutic agent comprises a VEGF inhibitor and the second therapeutic agent comprises a COX inhibitor.
- the therapeutic device comprises a first chamber to receive an injection of the first therapeutic agent, and the first chamber is coupled to a first porous structure to contain the first therapeutic agent and release therapeutic amounts of the first therapeutic agent with a first release rate profile for the first extended time.
- a sustained drug delivery formulation comprising a first and second therapeutic agent wherein the first and second therapeutic agent is contained/disposed in a reservoir in at least one apparatus/therapeutic device of any one of claims 42 to 51 , and at least one of the first and second therapeutic agent has a half-life within the reservoir when implanted, the half life within the reservoir substantially greater than a corresponding half-life of the at least one of the first and second therapeutic agent when injected directly into the vitreous of an eye.
- the device can be configured by selection of the reservoir volume and a porous structure with an appropriate rate release index to achieve the desired effective half-life.
- the first therapeutic agent is a VEGF-inhibitor and the second therapeutic agent is an inflammatory response inhibitor.
- the VEGF inhibitor is selected from the group consisting of Ranibizumab, Bevacizumab and AfliberceptTM.
- Mefenamic acid Meclofenamic acid, Flufenamic acid, and Tolfenamic acid.
- the inflammatory response inhibitor is selected from the group consisting of a cyclooxygenase (COX) inhibitor, a lipoxygenase (LOX) inhibitor and a tumor necrosis factor (TNF).
- COX cyclooxygenase
- LOX lipoxygenase
- TNF tumor necrosis factor
- the lox inhibitor is selected from the group consisting of azelastine and zileuton.
- the TNF is selected from the group consisting of bupropion, pentoxifylline, infliximab, adalimumab, and etanercept.
- the concentration of the first therapeutic agent is greater than about 40 mg/ml.
- the amount of the first therapeutic agent is greater than about 50 mg.
- At least one of the first and second therapeutic agent is stabilized by adsorption onto solid substrate or macromolecule that is capable of being flushed from the eye.
- the first and second therapeutic agents are contained/disposed in one apparatus/therapeutic device.
- the first therapeutic agent is contained/disposed in a first apparatus/therapeutic device and the second therapeutic agent is contained/disposed in a second apparatus/therapeutic device.
- the first and second therapeutic agents are administered simultaneously.
- the first and second therapeutic agents are administered sequentially.
- FIG. 1 shows an eye suitable for incorporation of the therapeutic device, in accordance with embodiments of the present invention
- FIG. lA-1 shows a therapeutic device implanted at least partially within the sclera of the eye as in FIG. 1;
- FIG. lA-1-1 and 1 A-l-2 show a therapeutic device implanted under the conjunctiva and extending through the sclera to release a therapeutic agent into vitreous humor of the eye so as to treat the retina of the, in accordance with embodiments of the present invention;
- FIG. 1 A-2-2 shows a therapeutic device comprising a reservoir suitable for loading in a cannula;
- FIG. IB shows a therapeutic device configured for placement in an eye as in FIG. 1A- 1 and lA-1-1 , in accordance with embodiments of the present invention;
- FIG. 1C shows a therapeutic device configured for placement in an eye as in FIG. 1 A- 1 and 1 A- 1-1 , in accordance with embodiments of the present invention
- FIG. 1 C-A shows at least one exit port, according to embodiments of the present invention
- FIG. lC-1 shows a method of removing a binding material, according to embodiments of the present invention.
- FIG. lC-2 and inserting the therapeutic agent with a second insert having the TA bound thereon;
- FIG. lC-3 shows syringe being filled with a commercially available formulation of therapeutic agent for injection into the therapeutic device, in accordance with embodiments;
- Fig. 2 shows a first therapeutic agent contained in a first injector and a second therapeutic agent contained in a second injector to treat the patient;
- Fig. 5 shows a therapeutic device having a plurality of parallel reservoirs comprising a first reservoir and a second reservoir;
- FIG. 6A shows a therapeutic device having a plurality of reservoirs configured in series comprising a first reservoir and a second reservoir;
- FIG. 6B shows a rigid porous structure configured for sustained release with a device as in FIG. 6A;
- FIG. 6B-1 shows interconnecting channels extending from a first side to a second side of the porous structure as in FIG. 6B; [0110] FIG. 6B-2 shows a plurality of paths of the therapeutic agent along the
- interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B1 ;
- FIG. 6B-4 shows blockage of the openings with particles and the plurality of paths of the therapeutic agent along the interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B-1 ;
- FIG. 6B-5 shows an effective cross-sectional size and area corresponding to the plurality of paths of the therapeutic agent along the interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B-1 ;
- FIG. 6C shows a rigid porous structure as in FIG. 6B incorporated into a scleral tack
- FIG. 6D shows a rigid porous structure as in FIG. 6B coupled with a reservoir for sustained release
- FIG. 6E shows a rigid porous structure as in FIG. 6B comprising a hollow body or tube for sustained release
- FIG. 6F shows a rigid porous structure as in FIG. 6B comprising a non-linear helical structure for sustained release
- FIG. 6G shows porous nanostructures, in accordance with embodiments
- FIG. 7 shows a therapeutic device coupled to an injector that removes material from the device and injects therapeutic agent into the device, according to embodiments
- Fig. 7 A shows a therapeutic device having a reservoir tuned to receive an injection of a first amout of first therapeutic agent and a second amount of second therapeutic agent;
- FIG. 7A-1 shows a therapeutic device coupled to an injector needle comprising a stop that positions the distal end of the needle near the proximal end of the device to flush the reservoir with ejection of liquid formulation through the porous frit structure, in accordance with embodiments;
- FIG. 7B-2 shows an isometric view of the therapeutic device as in FIG. 7B-1 ;
- FIG. 7B-3 shows a top view of the therapeutic device as in FIG. 7B-1 ;
- FIG. 7B-5 shows a bottom view of the therapeutic device as in FIG. 7B-1 implanted in the sclera;
- Fig. 8A2 shows the therapeutic device implanted with the reservoir between the conjunctiva and the sclera, such that elongate structure extends through the sclera to couple the reservoir chamber to the vitreous humor;
- Fig. 9 shows the porous structure of therapeutic device located in channel near the opening to the chamber of the container;
- Fig. 10 shows the porous structure located within the chamber of container and coupled to the first opening of the elongate structure so as to provide the release rate profile;
- Fig. 1 1 shows a plurality of injection ports spaced apart so as to inject and exchange the liquid of chamber of the container and inject the therapeutic agent into the reservoir chamber of the container;
- Fig. 12 shows the elongate structure coupled to the container away from the center of the container and near and located near an end of the container;
- FIG. 13 shows the cumulative release of BSA protein through a sintered porous titanium cylinder; [0136] FIG. 13-1 shows the measured cumulative release of BSA of FIG. 13 measured to 180 days;
- FIG. 17 shows cumulative release of BSA through 0.1 media grade sintered porous stainless steel cylinder
- FIG. 18A shows cumulative release of BSA through 0,2 media grade sintered porous stainless steel cylinder
- FIG. 19C shows determined concentrations of ranibizumab in the vitreous humor for a first 50 uL LucentisTM injection into a 32 uL reservoir of the device and a second 50 uL injection at 90 days, in accordance with embodiments;
- FIG. 19D shows determined concentrations of ranibizumab in the vitreous humor for a first 50 uL LucentisTM injection into a 50 uL reservoir of the device and a second 50 uL injection at 90 days, in accordance with embodiments;
- FIG. 19E shows determined concentrations of ranibizumab in the vitreous humor for a first 50 uL LucentisTM injection into a 50 uL reservoir of the device and a second 50 uL injection at 130 days, in accordance with embodiments;
- FIG. 19F shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 50 uL device having a release rate index of 0.05, in accordance with embodiments;
- FIG. 19G shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 75 uL device having a release rate index of 0.05, in accordance with embodiments;
- FIG. 19H shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 100 uL device having a release rate index of 0.05, in accordance with embodiments;
- FIG. 191 shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL device having a release rate index of 0.05, in accordance with embodiments;
- FIG. 19J shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 150 uL device having a release rate index of 0.05, in accordance with embodiments;
- FIG. 19K shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 100 uL device having a release rate index of 0.1, in accordance with embodiments;
- FIG. 19L shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.105, in accordance with embodiments;
- FIG. 19M shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.095, in accordance with embodiments;
- FIG. 19N shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.085, in accordance with embodiments;
- FIG. 190 shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.075, in accordance with embodiments;
- FIG. 19P shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.065, in accordance with embodiments;
- FIG. 19R shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL concentrated LucentisTM (40 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about five days, in accordance with embodiments;
- FIG. 19S shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL standard LucentisTM (10 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about nine days, in accordance with embodiments;
- FIG. 19T shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL standard LucentisTM (10 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about five days, in accordance with embodiments;
- FIG. 20 shows a calculated time release profile of a therapeutic agent suspension in a reservoir, in accordance with embodiments.
- FIG. 21 shows cumulative release for AvastinTM with therapeutic devices comprising substantially similar porous frit structures and a 16 uL reservoir and a 33 uL reservoir;
- FIG. 22A shows cumulative release for AvastinTM with porous frit structures having a thickness of 0.049"
- FIG. 22B-1 shows cumulative release for AvastinTM with porous frit structures having a thickness of 0.029"
- FIG. 22B-2 shows rate of release for AvastinTM with porous frit structures having a thickness of 0.029" as in FIG. 22B-1 ;
- FIG. 23A- 1 shows cumulative release to about 90 days for AvastinTM with a reservoir volume of 20 uL as in FIG. 23A;
- FIG. 23B shows rate of release as in FIG. 23 A;
- FIG. 23B-1 shows rate of release as in FIG. 23 A- 1 ;
- FIG. 24A-1 shows cumulative release to about 90 days release for AvastinTM with a 0.1 media grade porous frit structure as in FIG. 24A;
- FIG. 24B shows rates of release of the devices as in FIG. 24A;
- FIG. 24B-1 shows rates of release of the devices as in FIG. 24A-1 ;
- FIG. 25A shows cumulative release for fluorescein through a 0.2 media grade porous frit structure
- FIG. 25A-1 shows cumulative release to about 90 days for fluorescein through a 0.2 media grade porous frit structure as in FIG. 25A;
- FIG. 25B shows rates of release of the devices as in FIG. 25A;
- FIG. 25D shows rates of release of the devices as in FIG. 25C;
- FIG. 25E shows cumulative relase to about thirty days for LucentisTM for 30 uL devices having a RRI's from about 0.015 to about 0.090;
- FIG. 25F shows rates of release of the devices as in FIG. 25E;
- FIGS. 26A and 26B show scanning electron microscope images from fractured edges of porous frit structures so as to show the structure of the porous structure to release the therapeutic agent, in accordance with embodiments;
- FIGS. 27A and 27B show scanning electron microscope images from surfaces of porous frit structures, in accordance with embodiments;
- FIG. 28 shows a pressure decay test and test apparatus for use with a porous structure so as to identify porous frit structures suitable for use with therapeutic devices in accordance with embodiments described herein;
- embodiments of the present invention can be used to deliver many therapeutic agents to many tissues of the body.
- embodiments of the present invention can be used to deliver therapeutic agent for an extended period to one or more of the following tissues: intravascular, intra articular, intrathecal, pericardial, intraluminal and gut.
- the therapeutic agents and devices as described herein can be used to deliver combinations of therapeutic agents for an extended time.
- the combined therapeutic agents can be used to treat many disease of the eye, for example age related macular degeneration
- Embodiments of the present invention provide sustained release of a therapeutic agent to the posterior segment of the eye or the anterior segment of the eye, or combinations thereof.
- the release rate index encompasses (PA/FL) where P comprises the porosity, A comprises an effective area, F comprises a curve fit parameter corresponding to an effective length and L comprises a length or thickness of the porous structure.
- the units of the release rate index (RRI) comprise units of mm unless indicated otherwise and can be determined by a person of ordinary skill in the art in accordance with the teachings described hereon.
- a therapeutic agent referred to with a trade name encompasses one or more of the formulation of the therapeutic agent commercially available under the tradename, the active ingredient of the commercially available formulation, the generic name of the active ingredient, or the molecule comprising the active ingredient.
- first and second identify components of combinations and can be in any order, for example reversed, or simultaneous, in accordance with the teachings and embodiments described herein.
- the therapeutic agent may comprise small molecules such as of a corticosteroid and analogues thereof.
- the therapeutic corticosteroid may comprise one or more of triamcinolone, triamcinolone acetonide, dexamethasone, dexamethasone acetate, fluocinolone, fluocinolone acetate, or analogues thereof.
- the therapeutic agent may comprise a therapeutic agent suitable for treatment of dry AMD such as one or more of SirolimusTM (Rapamycin), CopaxoneTM (Glatiramer Acetate), OtheraTM, Complement C5aR blocker, Ciliary Neurotrophic Factor, Fenretinide or
- the delivery profile may be configured in many ways to obtain a therapeutic benefit from the sustained release device.
- an amount of the therapeutic agent may be inserted into the container at monthly intervals so as to ensure that the concentration of therapeutic device is above a safety protocol or an efficacy protocol for the therapeutic agent, for example with monthly or less frequent injections into the container.
- the sustained release can result in an improved delivery profile and may result in improved results.
- the concentration of therapeutic agent may remain consistently above a threshold amount, for example 0.1 ug/mL, for the extended time.
- the insertion method may comprise inserting a dose into the container of the therapeutic device.
- a dose for example, a single injection of LucentisTM may be injected into the therapeutic device.
- the duration of sustained delivery of the therapeutic agent may extend for twelve weeks or more, for example four to six months from a single insertion of therapeutic agent into the device when the device is inserted into the eye of the patient.
- the therapeutic agent may be delivered in many ways so as to provide a sustained release for the extended time.
- the therapeutic device may comprise a therapeutic agent and a binding agent.
- the binding agent may comprise small particles configured to couple releasably or reversibly to the therapeutic agent, such that the therapeutic agent is released for the extended time after injection into the vitreous humor.
- the particles can be sized such that the particles remain in the vitreous humor of the eye for the extended time.
- the therapeutic agent may be delivered with a device implanted in the eye.
- the drug delivery device can be implanted at least partially within the sclera of the eye, so as to couple the drug delivery device to the sclera of the eye for the extended period of time.
- the therapeutic device may comprise a drug and a binding agent.
- the drug and binding agent can be configured to provide the sustained release for the extended time.
- a membrane or other diffusion barrier or mechanism may be a component of the therapeutic device to release the drug for the extended time.
- the therapeutic device can be refilled in many ways.
- the therapeutic agent can be refilled into the device in the physician's office.
- the therapeutic device may comprise many configurations and physical attributes, for example the physical characteristics of the therapeutic device may comprise at least one of a drug delivery device with a suture, positioning and sizing such that vision is not impaired, and biocompatible material.
- the device may comprise a reservoir capacity from about 0.005 cc to about 0.2 cc, for example from about 0.01 cc to about 0.1 cc, and a device volume of no more than about 2 cc.
- a vitrectomy may be performed for device volumes larger than 0.1 cc.
- the length of the device may not interfere with the patient's vision and can be dependent on the shape of the device, as well as the location of the implanted device with respect to the eye.
- the length of the device may also depend on the angle in which the device is inserted.
- a length of the device may comprise from about 4 to 6 mm. Since the diameter of the eye is about 24 mm, a device extending no more than about 6 mm from the sclera into the vitreous may have a minimal effect on patient vision.
- Embodiments may comprise many combinations of implanted drug delivery devices.
- the therapeutic device may comprise a drug and binding agent.
- the device may also comprise at least one of a membrane, an opening, a diffusion barrier, a diffusion mechanism so as to release therapeutic amounts of therapeutic agent for the extended time.
- FIG. 1 shows an eye 10 suitable for incorporation of the therapeutic device.
- the eye has a cornea 12 and a lens 22 configured to form an image on the retina 26.
- the cornea can extend to a limbus 14 of the eye, and the limbus can connect to a sclera 24 of the eye.
- a conjunctiva 16 of the eye can be disposed over the sclera.
- the lens can accommodate to focus on an object seen by the patient.
- the eye has an iris 18 that may expand and contract in response to light.
- the eye also comprises a choroid 28 disposed the between the sclera 24 and the retina 26.
- the retina comprises the macula 32.
- the eye comprises a pars plana 25, which comprises an example of a region of the eye suitable for placement and retention, for example anchoring, of the therapeutic device 100 as described herein.
- the pars plana region may comprise sclera and conjuncitva disposed between the retina and cornea.
- the therapeutic device can be positioned so as to extend from the pars plana region into the vitreous humor 30 to release the therapeutic agent.
- the therapeutic agent can be released into the vitreous humor 30, such that the therapeutic agent arrives at the retina and choroids for therapeutic effect on the macula.
- the vitreous humor of the eye comprises a liquid disposed between the lens and the retina.
- the vitreous humor may comprise convection currents to deliver the therapeutic agent to the macula.
- FIG. 1 A-l shows a therapeutic device 100 implanted at least partially within the sclera 24 of the eye 10 as in FIG. 1.
- the therapeutic device may comprise a retention structure, for example a protrusion, to couple the device to the sclera.
- the therapeutic device may extend through the sclera into vitreous humor 30, such that the therapeutic device can release the therapeutic agent into the vitreous humor.
- FIGS. lA-1-1 and lA-l-2 shows a therapeutic device 100 implanted under the conjunctiva 16 and extending through the sclera 24 to release a therapeutic agent 1 10 into vitreous humor 30 of the eye 10 so as to treat the retina of the eye.
- the therapeutic device 100 may comprise a retention structure 120 such as a smooth protrusion configured for placement along the sclera and under the conjunctiva, such that the conjunctiva can cover the therapeutic device and protect the therapeutic device 100.
- the conjunctiva may be lifted away, incised, or punctured with a needle to access the therapeutic device.
- the eye may comprise an insertion of the tendon 27 of the superior rectus muscle to couple the sclera of the eye to the superior rectus muscle.
- the device 100 may be positioned in many locations of the pars plana region, for example away from tendon 27 and one or more of posterior to the tendon, posterior to the tendon, under the tendon, or with nasal or temporal placement of the therapeutic device.
- the implant can be positioned in the eye in many ways, work in relation to embodiments suggests that placement in the pars plana region can release therapeutic agent into the vitreous to treat the retina, for example therapeutic agent comprising an active ingredient composed of large molecules.
- Therapeutic agents 110 suitable for use with device 100 includes many therapeutic agents, for example as listed in Table 1A, herein below.
- the therapeutic agent 110 of device includes many therapeutic agents, for example as listed in Table 1A, herein below.
- the therapeutic agent 100 may comprise one or more of an active ingredient of the therapeutic agent, a formulation of the therapeutic agent, a commercially available formulation of the therapeutic agent, a physician prepared formulation of therapeutic agent, a pharmacist prepared formulation of the therapeutic agent, or a commercially available formulation of therapeutic agent having an excipient.
- the therapeutic agent may be referred to with generic name or a trade name, for example as shown in Table 1A.
- FIG. 1 A-2 shows structures of therapeutic device 100 configured for placement in an eye as in FIGS. lA-1 , lA-1-1 and lA-1-2.
- the device may comprise retention structure 120 to couple the device 100 to the sclera, for example a protrusion disposed on a proximal end of the device.
- the device 100 may comprise a container 130 affixed to the retention structure 120.
- An active ingredient, for example therapeutic agent 1 10 can be contained within a reservoir 140, for example a chamber 132 defined by a container 130 of the device.
- the container 130 may comprise a porous structure 150 comprising a porous material 152, for example a porous glass frit 154, and a barrier 160 to inhibit release of the therapeutic agent, for example non- permeable membrane 162.
- the non-permeable membrane 162 may comprise a substantially non-permeable material 164.
- the non-permeable membrane 162 may comprise an opening 166 sized to release therapeutic amounts of the therapeutic agent 110 for the extended time.
- the porous structure 150 may comprise a thickness 150T and pore sizes configured in conjunction with the opening 166 so as to release therapeutic amounts of the therapeutic agent for the extended time.
- the container 130 may comprise reservoir 140 having a chamber with a volume 142 sized to contain a therapeutic quantity of the therapeutic agent 110 for release over the extended time.
- the non-permeable membrane 162, the porous material 152, the reservoir 140, and the retention structure 120 may comprise many configurations to deliver the therapeutic agent 1 10.
- the non-permeable membrane 162 may comprise an annular tube joined by a disc having at least one opening formed thereon to release the therapeutic agent.
- the porous material 152 may comprise an annular porous glass frit 154 and a circular end disposed thereon.
- the reservoir 140 may be shape-changing for ease of insertion, i.e. it may assume a thin elongated shape during insertion through the sclera and then assume an extended, ballooned shape, once it is filled with therapeutic agent.
- the porous structure 150 can be configured in many ways to release the therapeutic agent in accordance with an intended release profile.
- the porous structure may comprise a porous structure having a plurality of openings on a first side facing the reservoir and a plurality of openings on a second side facing the vitreous humor, with a plurality of interconnecting channels disposed there between so as to couple the openings of the first side with the openings of the second side, for example a sintered rigid material.
- the porous structure 150 may comprise one or more of a permeable membrane, a semi-permeable membrane, a material having at least one hole disposed therein, nano-channels, nano-channels etched in a rigid material, laser etched nano-channels, a capillary channel, a plurality of capillary channels, one or more tortuous channels, tortuous microchannels, sintered nano- particles, an open cell foam or a hydrogel such as an open cell hydrogel.
- 1A-2-1 shows therapeutic device 100 loaded into an insertion cannula 210 of an insertion apparatus 200, in which the device 100 comprises an elongate narrow shape for insertion into the sclera, and in which the device is configured to expand to a second elongate wide shape for retention at least partially in the sclera;
- FIG. IB shows therapeutic device 100 configured for placement in an eye as in FIG. lA-1 and lA-1-1.
- the device comprises retention structure 120 to couple to the sclera, for example flush with the sclera, and the barrier 160 comprises a tube 168.
- An active ingredient 112 comprising the therapeutic agent 110 is contained within tube 168 comprising non- permeable material 164.
- a porous material 152 is disposed at the distal end of the tube 168 to provide a sustained release of the therapeutic agent at therapeutic concentrations for the extended period.
- the non-permeable material 164 may extend distally around the porous material 152 so as to define an opening to couple the porous material 152 to the vitreous humor when the device is inserted into the eye.
- the tube 168 and retention structure 120 may be configured to receive a glass rod, which is surface treated, and the glass rod can be injected with therapeutic agent . When the therapeutic agent has finished elution for the extended time, the rod can be replaced with a new rod.
- the device 100 may comprise therapeutic agent and a carrier, for example a binding medium comprising a binding agent to deliver the therapeutic agent.
- a carrier for example a binding medium comprising a binding agent to deliver the therapeutic agent.
- the therapeutic agent can be surrounded with a column comprising a solid support that is eroded away.
- FIG. 1C shows a therapeutic device configured for placement in an eye as in FIG. 1A- 1 and 1 A-l-1.
- a binding medium 192 comprising a binding agent 190 such as glass wool may be loaded with therapeutic agent 1 10 prior to injection into the device through an access port 180.
- the device 100 may comprise binding, leak, and barrier functions to deliver the therapeutic agent for the extended time.
- the binding medium 192 and therapeutic agent 1 10 can be aspirated to replace the binding medium and therapeutic agent.
- the binding medium can be at least one of flushed or replaced when at least majority of the therapeutic agent has been released, such that additional therapeutic agent can be delivered from a second, injected binding medium comprising therapeutic agent.
- a membrane 195 can be disposed over the periphery of the therapeutic device 100.
- the membrane 195 may comprise methyleellulose, regenerated cellulose, cellulose acetate, nylon, polycarbonate, poly(tetrafluoroethylene) (PTFE), polyethersulfone, and polyvinylidene difluoride (PVDF).
- the therapeutic device may comprise barrier 160 shaped such that opening 166 comprises an exit port.
- the therapeutic agent may be released through at least one of a diffusion mechanism or convection mechanism.
- the number, size, and configuration of exit ports may determine the release rate of the therapeutic agent.
- the exit port may comprise a convection port, for example at least one of an osmotically driven convection port or a spring driven convection port.
- the exit port may also comprise a tubular path to which the therapeutic agent may temporarily attach, and then be released under certain physical or chemical conditions.
- FIG. 1C-A shows at least one exit port 167 , the exit port can be disposed on the device 100 to allow liquid to flow from inside the device outward, for example when fluid is injected into an injection port 182 of the device or when an insert such as a glass frit is inserted into the device.
- the therapeutic device may comprise an access port 180 for injection and/or removal, for example a septum. Additionally or in the alternative, when the therapeutic device is refilled, the contents of the device may be flushed into the vitreous of the eye.
- FIG. lC-1 shows a method of removing a binding agent 194.
- a needle 189 coupled to a syringe 188 of an injector 187 can be inserted into an access port 180 of the therapeutic device 100.
- the binding agent 194 can be aspirated with a needle.
- FIG. 1 C-2 shows a method of inserting the therapeutic agent 1 10 with a second binding agent 190 having the therapeutic agent 1 10 bound thereon.
- the therapeutic agent can be injected into a container 130 of the device for sustained release over the extended time.
- FIG. lC-3 shows syringe being filled with a formulation of therapeutic agent for injection into the therapeutic device.
- the needle 189 coupled to syringe 188 of injector 187 can be used to draw therapeutic agent 110 from a container 1 IOC.
- the container 1 IOC may comprise a commercially available container, such as a bottle with a septum, a single dose container, or a container suitable for mixing formulations.
- a quantity 1 10V of therapeutic agent 1 10 can be drawn into injector 187 for injection into the therapeutic device 100 positioned within the eye.
- the quantity 110V may comprise a predetermined quantity, for example based on the volume of the container of the therapeutic device 110 and an intended injection into the vitreous humor.
- the formulation 1 1 OF may be a concentrated or diluted formulation of a commercially available therapeutic agent, for example AvastinTM.
- AvastinTM a commercially available therapeutic agent
- the osmolarity and tonicity of the vitreous humor can be within a range from about 290 to about 320.
- a commercially available formulation of AvastinTM may be diluted so as to comprise a formulation having an osmolarity and tonicity substantially similar to the osmolarity and tonicity of the vitreous humor, for example within a range from about 280 to about 340, for example about 300 mOsm.
- the therapeutic agent 1 10 may comprise an osmolarity and tonicity substantially similar to the vitreous humor, the therapeutic agent 1 10 may comprise a hyper osmotic solution relative to the vitreous humor or a hypo osmotic solution relative to the vitreous humor.
- a person or ordinary skill in the art can conduct experiments based on the teachings described herein so as to determine empirically the formulation and osmolarity of the therapeutic agent to provide release of therapeutic agent for an extended time.
- LucentisTM active ingredient ranibizumab
- aqueous solution with 10 mM histidine HC1, 10% a, a-trehalose dihydrate, 0.01% polysorbate 20, at pH 5.5.
- the LucentisTM formulation can be substantially similar to the formulation of the United States.
- the sustained release formulation of Lucentis in development by Genentech and/or Novartis may comprise the therapeutic agent injected in to the device 100.
- the sustained release formulation may comprise particles comprising active ingredient.
- AvastinTM (bevacizumab) is approved as an anticancer drug and in clinical trials are ongoing for AMD.
- the commercial solution is a pH 6.2 solution for intravenous infusion.
- AvastinTM is supplied in 100 mg and 400 mg preservative-free, single-use vials to deliver 4 mL or 16 mL of AvastinTM (25 mg/mL).
- the 100 mg product is formulated in 240 mg ⁇ , ⁇ -trehalose dihydrate, 23.2 mg sodium phosphate (monobasic, monohydrate), 4.8 mg sodium phosphate (dibasic, anhydrous), 1.6 mg polysorbate 20, and Water for Injection, USP.
- the 400 mg product is formulated in 960 mg ⁇ , ⁇ -trehalose dihydrate, 92.8 mg sodium phosphate (monobasic, monohydrate), 19.2 mg sodium phosphate (dibasic, anhydrous), 6.4 mg polysorbate 20, and Water for Injection, USP.
- the commercial formulations are diluted in lOOmL of 0.9% sodium chloride before administration and the amount of the commercial formulation used varies by patient and indication. Based on the teachings described herein, a person of ordinary skill in the art can determine formulations of AvastinTM to inject into therapeutic device 100. In Europe, the AvastinTM formulation can be substantially similar to the formulation of the United States.
- Triamcinolone used in injectable solutions, the acetonide and the hexacetonide.
- the acetamide is approved for intravitreal injections in the U.S.
- the acetamide is the active ingredient in TRIVARIS
- the formulation of therapeutic agent may injected into therapeutic device 100 may comprise many known formulations of therapeutic agents, and the formulation therapeutic agent comprises an osmolatiry suitable for release for an extended time from device 100.
- Table IB shows examples of osmolarity (Osm) of saline and some of the commercially formulations of Table 1A.
- the formulations listed in Table IB are substantially iso- osmotic and isotonic with respect to the vitreous of the eye and suitable for injection into the therapeutic device
- the formulation of the therapeutic agent injected into the therapeutic device can be hypertonic (hyper-osmotic) or hypotonic (hypo-osmotic) with respect to the tonicity and osmolarity of the vitreous.
- a hyper-osmotic formulation may release the active ingredient of the therapeutic agent into the vitreous somewhat faster initially when the solutes of the injected formulation equilibrate with the osmolatiry of the vitreous
- a hypo-osmotic formulation such as AvastinTM may release the active ingredient of the therapeutic agent into the vitreous somewhat slower initially when the solutes of the injected formulation equilibrate with the eye.
- a person of ordinary skill in the art can conduct experiments based on the teaching described herein to determine empirically the appropriate reservoir chamber volume and porous structure for a formulation of therapeutic agent disposed in the reservoir chamber, so as to release therapeutic amounts of the therapeutic agent for an extended time and to provide therapeutic concentrations of therapeutic agent in the vitreous within a range of therapeutic concentrations that is above the minimum inhibitory concentration for the extended time.
- the therapeutic device may comprise at least one structure configured to provide safety precautions.
- the device may comprise at least one structure to prevent at least one of macrophage or other immune cell within the reservoir body; bacterial penetration; or retinal detachment.
- the therapeutic device may be configured for other applications in the body.
- Other routes of administration of drugs may include at least one of intraocular, oral, subcutaneous, intramuscular, intraperitoneal, intranasal, dermal, intrathecal, intravascular, intra articular, pericardial, intraluminal in organs and gut or the like.
- Conditions that may be treated and/or prevented using the drug delivery device and method described herein may include at least one of the following: hemophilia and other blood disorders, growth disorders, diabetes, leukemia, hepatitis, renal failure, HIV infection, hereditary diseases such as cerebrosidase deficiency and adenosine deaminase deficiency, hypertension, septic shock, autoimmune diseases such as multiple sclerosis, Graves disease, systemic lupus erythematosus and rheumatoid arthritis, shock and wasting disorders, cystic fibrosis, lactose intolerance, Crohn's disease, inflammatory bowel disease, gastrointestinal or other cancers, degenerative diseases, trauma, multiple systemic conditions such as anemia, and ocular diseases such as, for example, retinal detachment, proliferative retinopathy, proliferative diabetic retinopathy, degenerative disease, vascular diseases, occlusions, infection caused by penet
- therapeutic agents 1 10 that may be delivered by the therapeutic device 100 are described in Table 1A and may include Triamcinolone acetonide, Bimatoprost (Lumigan), Ranibizumab (LucentisTM), Travoprost (Travatan, Alcon), Timolol (Timoptic, Merck), Levobunalol (Betagan, Allergan), Brimonidine (Alphagan, Allergan), Dorzolamide (Trusopt, Merck), Brinzolamide (Azopt, Alcon).
- hydroxyamphetamine hydroxyamphetamine
- sypathomimetics such as epinephrine
- antineoplastics such as carmustine, cisplatin and fluorouracil
- immunological drugs such as vaccines and immune stimulants
- hormonal agents such as estrogens, estradiol, progestational, progesterone, insulin, calcitonin, parathyroid hormone and peptide and vasopressin hypothalamus releasing factor
- beta adrenergic blockers such as timolol maleate, levobunolol Hcl and betaxolol Hcl
- growth factors such as epidermal growth factor, fibroblast growth factor, platelet derived growth factor, transforming growth factor beta, somatotropin and fibronectin
- carbonic anhydrase inhibitors such as dichlorophenamide, acetazolamide and methazolamide and other drugs such as prostaglandins, antiprostaglandins and pros
- the therapeutic agent 1 10 may comprise one or more of the following: Abarelix, Abatacept, Abciximab, Adalimumab, Aldesleukin, Alefacept, Alemtuzumab, Alpha- 1- proteinase inhibitor, Alteplase, Anakinra, Anistreplase, Antihemophilic Factor, Antithymocyte globulin, Aprotinin, Arcitumomab, Asparaginase, Basiliximab, Becaplermin, Bevacizumab, Bivalirudin, Botulinum Toxin Type A, Botulinum Toxin Type B, Capromab, Cetrorelix, Cetuximab, Choriogonadotropin alfa, Coagulation Factor IX, Coagulation factor Vila, Collagenase, Corticotropin, Cosyntropin, Cyclosporine, Daclizumab, Darbepoetin alfa, Defibrot
- the therapeutic agent 1 10 may comprise one or more of compounds that act by binding members of the immunophilin family of cellular proteins.
- Immunophilin binding compounds include but are not limited to the "limus” family of compounds.
- limus compounds that may be used include but are not limited to cyclophilins and FK506-binding proteins (FKBPs), including sirolimus (rapamycin) and its water soluble analog SDZ-RAD, tacrolimus, everolimus, pimecrolimus, CCI-779 (Wyeth), AP23841 (Ariad), and ABT-578 (Abbott Laboratories).
- FKBPs FK506-binding proteins
- the limus family of compounds may be used in the compositions, devices and methods for the treatment, prevention, inhibition, delaying the onset of, or causing the regression of angiogenesis-mediated diseases and conditions of the eye, including choroidal neovascularization.
- the limus family of compounds may be used to prevent, treat, inhibit, delay the onset of, or cause regression of AMD, including wet AMD.
- Rapamycin may be used to prevent, treat, inhibit, delay the onset of, or cause regression of angiogenesis-mediated diseases and conditions of the eye, including choroidal neovascularization. Rapamycin may be used to prevent, treat, inhibit, delay the onset of, or cause regression of AMD, including wet AMD.
- the therapeutic agent 1 10 may comprise one or more of: pyrrolidine, dithiocarbamate (NF.kappa.B inhibitor); squalamine; TPN 470 analogue and fumagillin; PKC (protein kinase C) inhibitors; Tie-1 and Tie-2 kinase inhibitors; inhibitors of VEGF receptor kinase; proteosome inhibitors such as Velcade.TM.
- integrin antagonists such as rosiglitazone or troglitazone; interferon, including .gamma.-interferon or interferon targeted to CNV by use of dextran and metal coordination; pigment epithelium derived factor (PEDF); endostatin; angiostatin; tumistatin; canstatin; anecortave acetate; acetonide; triamcinolone; tetrathiomolybdate; RNA silencing or RNA interference (RNAi) of angiogenic factors, including ribozymes that target VEGF expression; Accutane.TM.
- PEDF pigment epithelium derived factor
- endostatin angiostatin
- tumistatin canstatin
- anecortave acetate acetonide
- triamcinolone tetrathiomolybdate
- RNAi RNA silencing or RNA interference (RNAi) of angiogenic factors, including rib
- angiostatin angiostatin; tumistatin; canstatin; anecortave acetate; acetonide; triamcinolone;
- the therapeutic device may comprise a container configured to hold at least one therapeutic agent, the container comprising a chamber to hold the at least one therapeutic agent with at least one opening to release the at least one therapeutic agent to the vitreous humor and porous structure 150 placed within the at least one opening.
- the porous structure 150 may comprise a fixed tortuous, porous material such as a sintered metal, a sintered glass or a sintered polymer with a defined porosity and tortuosity that controls the rate of delivery of the at least one therapeutic agent to the vitreous humor.
- the rigid porous structures provide certain advantages over capillary tubes, erodible polymers and membranes as a mechanism for controlling the release of a therapeutic agent or agents from the therapeutic device.
- the device can also be tuned to release the therapeutic agent based on the half life of the therapeutic agent in the eye.
- the device volume and release rate index comprise parameters that can be tuned together based on the volume of formulation injected and the half life of the therapeutic agent in the eye. The following equations can be used to determine therapeutic device parameters suitable for tuning the device.
- the max value of Cv will correspond to conditions that maximize the Rate from the device.
- the maximum Cv is found at the the value of x that provides the maximum rate.
- the above equations provide approximate optimized values that, when combined with numerical simulations, can provide optimal values of Vr and PA/TL. The final optimum value can depend on additional parameters, such as the filling efficiency.
- the therapeutic device can be tuned to the volume of formulation injected into the device with a device reservoir volume and release rate index within about +/- 50% of the optimal values, for example +/- 30% of the optimal values.
- the maximum volume of the reservoir can be limited to no more than about twice the optimal volume.
- the porous structure tuned with the reservoir may comprise one or more of a porous frit, a permeable membrane, a semi-permeable membrane, a capillary tube or a tortuous channel, nano-structures, nano-channels or sintered nano-particles, and a person of ordinary skill in the art can determine the release rate characteristics, for example a release rate index, so as to tune the one or more porous structures and the volume to receive the quantity of the formulation and release therapeutic amounts for an extended time.
- the corresponding Cv is about 3.19 ug/mL at 180 days based on the Rate of drug released from the device at 180 days and the rate of the drug from the vitreous (k corresponding to a half life of about 9 days).
- a device with a container reservoir volume of 63 uL and RRI of 0.044 will also provide the optimal Cv at 180 days since the ratio of Vr to PA/TL is also optimal.
- the therapeutic device can be tuned to provide therapeutic amounts of drug at a targeted time, for example 180 days, with many values of the reservoir volume and many values of the release rate index near the optimal values, for example within about +/- 50% of the optimal values.
- the volume of the reservoir can be substantially fixed, the volume of the reservoir can vary, for example within about +/- 50% as with an expandable reservoir such as a balloon reservoir.
- the half life of the drug in the vitreous humor of the eye can be determined based on the therapeutic agent and the type of eye, for example human, rabbit or monkey, such that the half life may be determined based on the species of the eye, for example.
- the half life of the therapeutic agent in the vitreous humor can be shorter than for human eyes, for examply by a factor of about two in at least some instances.
- the half-life of the therapeutic agent LucentisTM (ranibizumab) can be about nine days in the human eye and about two to four days in the rabbit and monkey animal models.
- the half life in the vitreous humor of the human eye can be about two to three hours and can be about one hour in the monkey and rabbit animal models.
- the therapeutic device can be tuned to receive the volume of formulation based on the half life of the therapeutic agent in the human vitreous humor, or an animal vitreous humor, or combinations thereof. Based on the teachings described herein, a person of ordinary skill in the art can determine empirically the half life of the therapeutic agent in the eye based on the type of eye and the therapeutic agent, such that the revervoir and porous structure can be tuned together so as to receive the volume of formulation and provide therapeutic amounts for the extended time.
- the thereapeutic agents and devices as described herein can be used to deliver combinaitons of therapeutic agents for an extended time.
- the combined therapeutic agents can be used to treat many disease of the eye, for example age related macular degeneration
- Combination therapy to treat AMD may be can be used to treat a patient through the different disease stages.
- an inflammatory and oxidative stress takes a role in the development of the early and intermediate stage of the disease.
- the advanced stage may comprise enhanced by the VEGF activity and inflammatory components.
- CNV choroidal neovascularization
- a patient with early stage AMD who is at risk for advancing to intermediate or advanced AMD may benefit from an anti inflammatory treatment such as complement inhibitor alone or in combination with an anti oxidant. If the disease advances to CNV the same device may be injected with AntiVEGF alone or in combination with any antiinflammatory agent. Subsequently when the CNV is under sucessful control an agent to control local inflammation such as COX inhibitor can be injected to the device to reduce the chances for fibrosis and recurrence.
- an anti inflammatory treatment such as complement inhibitor alone or in combination with an anti oxidant.
- AntiVEGF alone or in combination with any antiinflammatory agent.
- COX inhibitor can be injected to the device to reduce the chances for fibrosis and recurrence.
- An AMD patient may go through few different disease stages, and one or more
- the therapeutic agent injected into device 100 can be injected based on a response of the patient to treatment.
- An inflammatory component is present while CNV is regressing and may
- An antiinflammatory can be injected into to inhibit scar formation.
- Oxidative stress may cause both early stage AMD and can be associated with the
- injection into therapeutic device 100 include one or more of:
- the combination therapy to treat AMD may comprise one or more of injecting the therapeutic agent 110 directly into the vitreous humor from a needle, injecting the therapeutic agent into therapeutic device 100 to store the therapeutic agent in device 100, injecting the therapeutic agent into the device 100 and through a porous structure to deliver a bolus of therapeutic agent 110 and store therapeutic agent 110 in device 100, injecting a first therapeutic agent 1 10 into a first device 100 and a second therapeutic agent 1 10 into a second thereapeutic device 100.
- Table 2 shows combinations treatments in accordance with embodiments.
- Fig. 2 shows a first therapeutic agent 1 10A contained in a first injector 187 and a second therapeutic agent HOB contained in a second injector 187 to treat the patient.
- the first therapeutic agent 11 OA can be combined with the second therapeutic agent 1 1 OB to treat the eye.
- the first therapeutic agent 1 10A and the second therapeutic agent HOB can be injected into the vitreous humor of the eye.
- the first therapeutic agent 110A may comprise a therapeutic agent to inhibit neoplasia, for example to inhibit neovascularization such as a VEGF inhibitor.
- the second therapeutic agent HOB may comprise an antiinflammatory, for example a steroid or a non-steroidal antiinflammatory such as a COX inhibitor. While the first therapeutic agent and the second therapeutic agent can be delivered in many ways, the first therapeutic agent and the second therapeutic agent may each be injected directly into the vitreous humor with a needle of the injector.
- Fig. 4 shows a plurality of therapeutic devices implanted into the eye to deliver therapeutic amounts of first therapeutic agent 110A and second therapeutic agent HOB.
- the plurality of therapeutic devices comprises a first therapeutic device 100 and a second therapeutic device 100.
- the first therapeutic device 100 can be configured with a volume and release rate index to provide sustained release of the first therapeutic agent when the first therapeutic agent 11 OA is injected into first device 100 implanted in the eye
- the second therapeutic device 100 can be configured with a second volume and second release rate index to provide sustained release of the second therapeutic agent HOB when the second device 100 is implanted in the eye.
- Fig. 5 shows a therapeutic device having a plurality of parallel reservoirs comprising a first reservoir 140A and a second reservoir 140B.
- First reservoir 140A comprises a first container 130A having a first chamber 132A coupled to a first porous structure 150X.
- Second reservoir 140B comprises a second container 130B having a second chamber 132B coupled to a second porous structure 150Y.
- a first injector 187A can comprise a first amount of therapeutic agent 1 10A and can be coupled to first reservoir 140A to deliver therapeutic amounts of first therapeutic agent 110A.
- a second injector 187B can comprise a second amount of second therapeutic agent 110B and can be coupled to second reservoir 140B to deliver therapeutic amounts of second therapeutic agent HOB.
- the first container and the second container can be tuned to the amount of therapeutic agent injected into the repsective container as described herein.
- the first chamber 132A can be configured with a volume and the first porous structure 150X configured release rate index so as to provide sustained release of the first therapeutic agent 11 OA when the first therapeutic agent 11 OA is injected into first device 100 implanted in the eye.
- the second chamber 132B can be configured with a second volume and the second porous structure 150Y can be configured with a second release rate index so as to provide sustained release of the second therapeutic agent 1 10B when the second therapeutic agent 1 10B is injected into device 100 implanted in the eye.
- Barrier 160 may extend between first chamber 132A and second chamber ⁇ 32 ⁇ . Based on the teahings described herein a person of ordinary skill in the art can detrmine the volume and release rate index of each chamber so as to release the therapeutic agent for the extended time.
- Fig. 6A shows a therapeutic device having a plurality of reservoirs configured in series comprising a first reservoir 140A and a second reservoir 140B.
- First reservoir 140A comprises a first container 130A having a first chamber 132A coupled to a first porous structure 150X.
- Second reservoir 140B comprises a second container 130B having a second chamber 132B coupled to a second porous structure 150Y.
- a injector 187 can comprise a first amount of therapeutic agent 110A and can be coupled to first reservoir 140A to inject therapeutic amounts of first therapeutic agent 110A.
- Second injector 132B can comprise a second amount of second therapeutic agent 1 10B comprising a solid located within second reservoir 140B so as to deliver therapeutic amounts of first therapeutic agent 1 10A.
- the first container can be tuned to the amount of therapeutic agent injected into chamber 132A.
- the first chamber 132A can be configured with a volume and the first porous structure 150X configured release rate index so as to provide sustained release of the first therapeutic agent 110A when the first therapeutic agent 1 1 OA is injected into first device 100 implanted in the eye.
- the second chamber 132B can be configured with a second volume and the second porous structure 150Y configured with a second release rate index so as to provide sustained release of the solid second therapeutic agent HOB and first therapeutic agent 1 10A.
- the first porous strucure 150X may extend between first chamber 132A and second chamber 132B, and the porosity and RRI of the first porous structure 150X can be smaller than the porosity and RRI of the second porous structure 150Y such that release rate of the first therapeutic agent 11 OA is substantial lly determined based on the porosity and RRI of the first porous structure and the release rate of the second therapeutic agent is determined substantially based on the porosity and RRI of the second porous structure.
- antiinflammatory for example a non-steroidal anti-inflammatory such as a COX inhibitor, for example such as celocoxib.
- a person of ordinary skill in the art could conduct experiments and simulations to determine the first release rate index, volume of the first chamber, and the first injected amount so as to release the first therapeutic agent 1 10A for a first extended time, and determine the second release rate index, volume of the second chamber, and the second amount of second therapeutic agent 11 OB so as to release the first therapeutic agent 1 10A for the first extended time the second therapeutic agent 1 10B for the second extended time.
- FIG. 6B shows a rigid porous structure as in FIG. 6A.
- the rigid porous structure 158 comprises a plurality of interconnecting channels 156.
- the porous structure comprises a sintered material composed of interconnected grains 155 of material.
- the interconnected grains of material define channels that extend through the porous material to release the therapeutic agent.
- the channels may extend around the sintered grains of material, such that the channels comprise interconnecting channels extending through the porous material.
- the channels of the rigid porous structure comprise a resistance to flow of an injected solution or suspension through a thirty gauge needle such that ejection of said solution or suspension through the rigid porous structure is substantially inhibited when said solution or suspension is injected into the reservoir of the therapeutic device.
- these embodiments may optionally comprise an evacuation vent or an evacuation reservoir under vacuum or both to facilitate filling or refilling of the reservoir.
- the reservoir and the porous structure can be configured to release therapeutic amounts of the therapeutic agent in many ways.
- the reservoir and the porous structure can be configured to release therapeutic amounts of the therapeutic agent corresponding to a concentration of at least about 0.1 ug per ml of vitreous humor for an extended period of at least about three months.
- the reservoir and the porous structure can be configured to release therapeutic amounts of the therapeutic agent corresponding to a concentration of at least about 0.1 ug per ml of vitreous humor and no more than about 10 ug per ml for an extended period of at least about three months.
- the therapeutic agent may comprise at least a fragment of an antibody and a molecular weight of at least about 10k Daltons.
- the hydrogel can be formed within the channels and may comprise an acrylamide gel.
- the hydrogel comprises a water content of at least about 70%.
- the hydrogel may comprise a water content of no more than about 90% to limit molecular weight of the therapeutic agent to about 30k Daltons.
- the hydrogel comprises a water content of no more than about 95% to limit molecular weight of the therapeutic agent to about 100k Daltons.
- the hydrogel may comprise a water content within a range from about 90% to about 95% such that the channels of the porous material are configured to pass LucentisTM and substantially not pass AvastinTM [0278]
- the rigid porous structure may comprise a composite porous material that can readily be formed in or into a wide range of different shapes and configurations.
- the mold can be oriented vertically with the open other end disposed upwardly, and metal powder having a particle size of less than 20 micrometers can be introduced into the cavity through the open end of the mold while vibrating the mold to achieve substantially uniform packing of the metal powder in the cavity.
- a cap can be placed on the open other end of the mold, and pressure is applied to the mold and thereby to the metal powder in the cavity to cause the metal powder to cohere and form a cup-shaped powdered metal structure having a shape corresponding to the mold.
- the shaped powdered metal structure can be removed from the mold, and sintered to obtain a porous sintered metal porous structure.
- the release rate of therapeutic agent through a porous body may be described by diffusion of the of the therapeutic agent within the porous structure with the channel parameter, and with an effective diffusion coefficient equal to the diffusion coefficient of the therapeutic agent in the liquid that fills the reservoir multiplied by the Porosity and a Channel Parameter of the porous body:
- F Channel parameter that may correspond to a tortuosity parameter of channels of porous structure
- A Area of porous structure
- the channel parameter multiplied by the thickness (length) of the porous structure can determine the effective length that the therapeutic agent travels along the interconnecting channels from the reservoir side to the vitreous side.
- the channel parameter (F) of about 1.5 corresponds to interconnecting channels that provide an effective increase in length traveled by the therapeutic agent of about 50%, and for a 1 mm thick porous structure the effective length that the therapeutic agent travels along the interconnecting channels from the reservoir side to the vitreous side corresponds to about 1.5 mm.
- the channel parameter (F) of at least about 2 corresponds to interconnecting channels that provide an effective increase in length traveled by the therapeutic agent of about 100%, and for a 1 mm thick porous structure the effective length that the therapeutic agent travels along the interconnecting channels from the reservoir side to the vitreous side corresponds to at least about 2.0 mm.
- the porous structure comprises many interconnecting channels that provide many alternative paths for release of the therapeutic agent, blockage of some of the channels provides no substantial change in the effective path length through the porous structure as the alternative interconnecting channels are available, such that the rate of diffusion through the porous structure and the release of the therapeutic agent are substantially maintained when some of the channels are blocked.
- the value for the diffusion coefficient of the therapeutic agent (TA) in water at the temperature of interest may be used.
- MW refers to the molecular weight of either BSA or the test compound and ⁇ is the viscosity of water, and Table 3 lists diffusion coefficients of proteins of interest. Table 3. Diffusion Coefficients
- the small molecule may comprise a glucocorticoid such as triamcinolone acetonide having a molecular weight of about 435.
- Porosity can be determined from the weight and macroscopic volume or can be measured via nitrogen gas adsorption [0287]
- the porous structure may comprise a plurality of porous structures, and the area used in the above equation may comprise the combined area of the plurality of porous structures.
- the channel parameter may comprise a fit parameter corresponding to the tortuosity of the channels.
- the curve fit parameter F which may correspond to tortuosity of the channels can be determined based on experimental measurements.
- the parameter PA/FL can be used to determine the desired sustained release profile, and the values of P, A, F and L determined.
- the rate of release of the therapeutic agent corresponds to a ratio of the porosity to the channel parameter, and the ratio of the porosity to the channel parameter can be less than about 0.5 such that the porous structure releases the therapeutic agent for the extended period.
- the ratio of the porosity to the channel parameter is less than about 0.1 or for example less than about 0.2 such that the porous structure releases the therapeutic agent for the extended period.
- the channel parameter may comprise a value of at least about 1, such as at least about 1.2.
- the value of the channel parameter may comprise at least about 1.5, for example at least about 2, and may comprise at least about 5.
- the channel parameter can be within a range from about 1.1 to about 10, for example within a range from about 1.2 to about 5.
- the area in the model originates from the description of mass transported in units of flux; i.e., rate of mass transfer per unit area.
- rate of mass transfer per unit area i.e., rate of mass transfer per unit area.
- the area corresponds to one face of the disc and the thickness, L, is the thickness of the disc.
- the effective area is a value in between the area where therapeutic agent enters the porous body and the area where therapeutic agent exits the porous body.
- a model can be derived to describe the release rate as a function of time by relating the change of concentration in the reservoir to the release rate described above.
- This model assumes a solution of therapeutic agent where the concentration in the reservoir is substantially uniform.
- Solving the differential equation and rearrangement yields the following equations describing the concentration in the reservoir as a function of time, t, and volume of the reservoir, V R , for release of a therapeutic agent from a solution in a reservoir though a porous structure.
- the concentration in reservoir is the dissolved concentration in equilibrium with the solid (i.e., the solubility of the therapeutic agent).
- the concentration in the reservoir is constant with time, the release rate is zero order, and the cumulative release increases linearly with time until the time when the solid is exhausted.
- Therapeutic concentrations for many ophthalmic therapeutic agents may be determined experimentally by measuring concentrations in the vitreous humor that elicit a therapeutic effect. Therefore, there is value in extending predictions of release rates to predictions of concentrations in the vitreous.
- a one-compartment model may be used to describe elimination of therapeutic agent from eye tissue.
- the model predicts an initial concentration of 333 ug/mL for a bolus injection of 0.5 mg LucentisTM into the eye of a monkey. This concentration decays to a vitreous concentration of 0.1 ug/mL after about a month.
- vitreous concentration decreases with a rate constant equal to D PA / FL V R and, hence, is dependent on the properties of the porous structure and the volume of the reservoir.
- the vitreous concentration will also be time-independent.
- the release rate will depend on the properties of the porous structure via the ratio, PA / FL , but will be independent of the volume of the reservoir until the time at which the drug is exhausted.
- the channels of the rigid porous structure can be sized in many ways to release the intended therapeutic agent.
- the channels of the rigid porous structure can be sized to pass therapeutic agent comprising molecules having a molecular weight of at least about 100 Daltons or for example, at least about 50k Daltons.
- the channels of the rigid porous structure can be sized to pass therapeutic agent comprising molecules comprising a cross-sectional size of no more than about 10 nm.
- the channels of the rigid porous structure comprise
- the rigid porous structure comprises grains of rigid material and wherein the interconnecting channels extend at least partially around the grains of rigid material to pass the therapeutic agent through the porous material.
- the grains of rigid material can be coupled together at a loci of attachment and wherein the interconnecting channels extend at least partially around the loci of attachment.
- the porous structure and reservoir may be configured to release the glucocorticoid for an extended time of at least about six months with a therapeutic amount of glucocorticoid of corresponding to an in situ concentration within a range from about 0.05 ug/mL to about 4 ug/mL, for example from 0.1 ug/mL to about 4 ug/mL, so as to suppress inflammation in the retina-choroid.
- the porous structure comprises a sintered material.
- the sintered material may comprise grains of material in which the grains comprise an average size of no more than about 20 um.
- the sintered material comprises a wettable material to inhibit bubbles within the channels of the material.
- the sintered material comprises at least one of a metal, a ceramic, a glass or a plastic.
- the sintered material may comprises a sintered composite material, and the composite material comprises two or more of the metal, the ceramic, the glass or the plastic.
- the metal comprises at least one of Ni, Ti, nitinol, stainless steel including alloys such as 304, 304L, 316 or 316L, cobalt chrome, elgiloy, hastealloy, c-276 alloy or Nickel 200 alloy.
- the sintered material may comprise a ceramic.
- the sintered material may comprise a glass.
- the plastic may comprise a wettable coating to inhibit bubble formation in the channels, and the plastic may comprise at least one of polyether ether ketone (PEEK), polyethylene, polypropylene, polyimide, polystyrene, polycarbonate, polyacrylate, polymethacrylate, or polyamide.
- PEEK polyether ether ketone
- the rigid porous structure may comprise a plurality of rigid porous structures coupled to the reservoir and configured to release the therapeutic agent for the extended period.
- additional rigid porous structure can be disposed along the container, for example the end of the container may comprise the porous structure, and an additional porous structure can be disposed along a distal portion of the container, for example along a tubular sidewall of the container.
- the therapeutic device can be tuned to release therapeutic amounts of the therapeutic agent above the minimum inhibitory concentration for an extended time based on bolus injections of the therapeutic agent.
- the volume of the chamber of the reservoir can be sized with the release rate of the porous structure based on the volume of the bolus injection.
- a formulation of a therapeutic agent can be provided, for example a known intravitreal injection formulation.
- the therapeutic agent can be capable of treating the eye with bolus injections, such that the formulation has a corresponding period between each of the bolus injections to treat the eye.
- the bolus injections may comprise monthly injections.
- Each of the bolus injections comprises a volume of the formulation, for example 50 uL.
- Each of the bolus injections of the therapeutic agent may correspond to a range of therapeutic concentrations of the therapeutic agent within the vitreous humor over the time course between injections, and the device can be tuned so as to release therapeutic amounts of the therapeutic agent such that the vitreous concentrations of the released therapeutic agent from the device are within the range of therapeutic concentrations of the corresponding bolus injections.
- the therapeutic agent may comprise a minimum inhibitory concentration to treat the eye, for example at least about 3 ug/mL, and the values of the range of therapeutic concentrations can be at least about 3 ug/mL.
- the therapeutic device can be configured to treat the eye with an injection of the monthly volume of the formulation into the device, for example through the penetrable barrier.
- the reservoir of the container has a chamber to contain a volume of the therapeutic agent, for example 35 uL, and a mechanism to release the therapeutic agent from the chamber to the vitreous humor.
- the volume of the container and the release mechanism can be tuned to treat the eye with the therapeutic agent with vitreous concentrations within the therapeutic range for an extended time with each injection of the quantity corresponding to the bolus injection, such that the concentration of the therapeutic agent within the vitreous humor remains within the range of therapeutic concentrations and comprises at least the minimum inhibitory concentration.
- the extended time may comprise at least about twice the corresponding period of the bolus injections.
- the release mechanism comprises one or more of a porous frit, a sintered porous frit, a permeable membrane, a semi-permeable membrane, a capillary tube or a tortuous channel, nano-structures, nano-channels or sintered nano-particles.
- the amount of formulation released to the eye through the porous structure upon injection can decrease along with the concentration of active ingredient of the therapeutic agent within the reservoir, and the release rate index can be increased appropriately so as to provide thereapeutic amounts of therapeutic agent for the extended time.
- the volume of the reservoir of the container can be greater than the volume corresponding to the bolus injection, so as to provide therapeutic amounts for at least about five months, for example 6 months, with an injection volume corresponding to a monthly injection of LucentisTM.
- the formulation may comprise commercially available LucentisTM, 50 uL, and the reservoir may comprise a volume of about 100 uL and provide therapeutic vitreous concentrations of at least about 3 ug/mL for six months with 50 uL of LucentisTM injected into the reservoir.
- the chamber may comprise a substantially fixed volume and the release rate mechanism comprises a substantially rigid structure to maintain release of the therapeutic agent above the minimum inhibitory concentration for the extended time with each injection of a plurality of injections.
- FIG. 6B-1 shows interconnecting channels 156 extending from first side 150S1 to second side 150S2 of the porous structure as in FIG. 6B.
- the interconnecting channels 156 extend to a first opening 158A1, a second opening 158A2 and an Nth opening 158AN on the first side 150S1.
- the interconnecting channels 156 extend to a first opening 158B1, a second opening 158B2 and an Nth opening 158BN on the second side 150S2.
- Each of the openings of the plurality of channels on the first side is connected to each of the openings of plurality of channels on the second side, such that effective length traveled along the channels is greater than thickness 150T.
- the channel parameter can be within a range from about 1.1 to about 10, such that the effective length is within a range from about 1.1 to 10 times the thickness 150T.
- the channel parameter can be about 1 and the porosity about 0.2, such that the effective length corresponds to at least about 5 times the thickness 150T.
- FIG. 6B-2 shows a plurality of paths of the therapeutic agent along the
- the plurality of paths comprises a first path 156P1 extending from the first side to the second side, a second path 156P2 extending from the first side to the second side and a third path 156P3 extending from the first side to the second side, and many additional paths.
- the effect length of each of first path PI, second path P2 and third path P3 is substantially similar, such that each opening on the first side can release the therapeutic agent to each interconnected opening on the second side.
- the substantially similar path length can be related to the sintered grains of material and the channels that extend around the sintered material.
- the porous structure may comprise randomly oriented and connected grains of material, packed beads of material, or combinations thereof.
- the channel parameter can be related to the structure of the sintered grains of material and corresponding
- interconnecting channels porosity of the material, and percolation threshold.
- Work in relation to embodiments shows that the percolation threshold of the sintered grains may be below the porosity of the porous frit structure, such that the channels are highly inter-connected.
- the sintered grains of material can provide interconnected channels, and the grains can be selected to provide desired porosity and channel parameters and RRI as described herein.
- the channel parameter and effective length from the first side to the second side can be configured in many ways.
- the channel parameter can be greater than 1 and within a range from about 1.2 to about 5.0, such that the effective length is within a range about 1.2 to 5.0 times the thickness 150T, although the channel parameter may be greater than 5, for example within a range from about 1.2 to 10.
- the channel parameter can be from about 1.3 to about 2.0, such that the effective length is about 1.3 to 2.0 times the thickness 150T.
- experimental testing has shown the channel parameter can be from about 1.4 to about 1.8, such that the effective length is about 1.4 to 1.8 times the thickness 150T, for example about 1.6 times the thickness.
- FIG. 6B-3 shows blockage of the openings with a covering 156B and the plurality of paths of the therapeutic agent along the interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B-1.
- a plurality of paths 156PR extend from the first side to the second side couple the first side to the second side where one of the sides is covered, such that the flow rate is maintained when one of the sides is partially covered.
- FIG. 6B-4 shows blockage of the openings with particles 156PB and the plurality of paths of the therapeutic agent along the interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B-1.
- FIG. 6B-5 shows an effective cross-sectional size 150DE and area 150EFF corresponding to the plurality of paths of the therapeutic agent along the interconnecting channels extending from a first side to a second side of the porous structure as in FIGS. 6B and 6B-1.
- the effective cross sectional area of the interconnecting channels corresponds to the internal cross-sectional area of the porous structure disposed between the openings of the first side and the openings of the second side, such that the rate of release can be substantially maintained when the channels are blocked on the first side and the second side.
- the rigid porous structure can be shaped and molded in many ways for example with tubular shapes, conical shapes, discs and hemispherical shapes.
- the rigid porous structure may comprise a molded rigid porous structure.
- the molded rigid porous structure may comprises at least one of a disk, a helix or a tube coupled to the reservoir and configured to release the therapeutic agent for the extended period.
- FIG. 6C shows a rigid porous structure as in FIG. 6B incorporated into a scleral tack 601 as described in U.S. Pat. No. 5,466,233.
- the scleral tack comprises a head 602, a central portion 603 and a post 604.
- the post may comprise the reservoir 605 and the rigid porous structure 606 as described above.
- the porous structure may comprise a molded conical structure having a sharp tip configured for insertion into the patient. Alternatively or in combination, the tip may be rounded.
- FIG. 6E shows a plurality of rigid porous structures as in FIG. 6B incorporated with a drug delivery device for sustained release as described in U.S. Pat. No. 5,972,369.
- the therapeutic device comprises a reservoir 613 to contain the therapeutic agent and an impermeable and non-porous outer surface 614.
- the reservoir is coupled to a rigid porous structure 615 that extends to a distal end 617.
- the rigid porous structure comprises an exposed area 616 on the distal end to release the therapeutic agent, and the impermeable and non-porous outer surface may extend to the distal end.
- FIG. 6D shows a rigid porous structure as in FIG. 6B incorporated with a delivery device for sustained release as described in U.S. Pat. Pub. 2003/0014036 Al .
- the drug delivery device comprises an inlet port 608 on the proximal end and a hollow body 609 coupled to the inlet port.
- the hollow body comprises many openings 612 that allow a solution injected into the inlet port to pass from the hollow body into a balloon 610.
- the balloon comprises a distal end 611 disposed opposite the injection port.
- the balloon comprises a plurality of the rigid porous structures 607, as described above.
- Each of the plurality of porous rigid structures comprises a first surface exposed to the interior of the balloon and a second surface configured to contact the vitreous.
- the calculated area can be the combined area of the plurality of porous rigid structures as noted above.
- FIG. 6G shows porous nanostructures, in accordance with embodiments.
- the porous structure 150 may comprise a plurality of elongate nano-channels 156NC extending from a first side 150S1 of the porous structure to a second side 150S2 of the porous structure.
- the porous structure 150 may comprise a rigid material having the holes formed thereon, and the holes may comprise a maximum dimension across such as a diameter.
- the diameter of the nano- channels may comprise a dimension across, for example from about 10 nm across, to about 1000 nm across, or larger.
- the channels may be formed with etching of the material, for example lithographic etching of the material.
- the channels may comprise substantially straight channels such that the channel parameter F comprises about 1, and the parameters area A, and thickness or length L correspond to the combined cross-sectional area of the channels and the thickness or length of the porous structure.
- the porous structure 150 may comprise interconnecting nano-channels, for example formed with a sintered nano-material.
- the injection of therapeutic agent into the device 100 as described herein can be performed before implantion into the eye or alternatively when the therapeutic device is implanted into the eye.
- FIG. 7 shows a therapeutic device 100 coupled to an injector 701 that removes material from the device and injects therapeutic agent 702 into the device.
- the injector picks up spent media 703 and refills the injector with fresh therapeutic agent.
- the therapeutic agent is injected into the therapeutic device.
- the spent media is pulled up into the injector.
- the injector may comprise a stopper mechanism 704.
- the injector 701 may comprise a first container 702C to contain a formulation of therapeutic agent 702 and a second container 703C to receive the spent media 703.
- the needle 189 may comprise a double lumen needle with a first lumen coupled to the first container and a second lumen coupled to the second container, such that spent media 703 passes from the container reservoir of device 100 to the injector.
- a valve 703V for example a vent, can be disposed between the second lumen and the second container.
- valve When the valve is open and therapeutic agent is injected, spent media 703 from the container reservoir of the therapeutic device 100 passes to the second container of the injector, such that at least a portion of the spent media within the therapeutic device is exchanged with the formulation.
- a portion of the therapeutic agent passes from the reservoir of the therapeutic device into the eye.
- a first portion of formulation of therapeutic agent can be injected into therapeutic device 100 when the valve is open such that the first portion of the formulation is exchanged with material disposed within the reservoir; the valve is then closed and a second portion of the formulation is injected into therapeutic device 100 such that at least a portion of the first portion passes through the porous structure into the eye.
- a portion of the second portion of injected formulation may pass through the porous structure when the second portion is injected into the eye.
- the second portion of formulation injected when the valve is closed may correspond to a volume of formulation that passes through the porous structure into the vitreous humor to treat the patient immediately.
- Fig. 7 A shows a therapeutic device having a reservoir 140 tuned to receive an injection of a first amout of first therapeutic agent 1 10A and a second amount of second therapeutic agent 110B.
- the first amount of first therapeutic agent 11 OA and the second amount of second therapeutic agent 1 10B can be mixed together and injected from injector 187.
- Reservoir 140 comprises container 130 having chamber 132 coupled to porous structure 150. The container can be tuned with the volume and RRI of the porous structure to receive the first amount of first therapeutic agent 1 10A and second amount of second therapeutic agent 1 10B injected into chamber 132 with the first amount.
- the stop can be sized and positioned along an axis of the needle such that the needle tip extends a stop distance 189SD into the reservoir as defined by the length of the needle from the stop to the tip and the thickness of the penetrable barrier, in which the stop distance is within a range from about 0.5 to about 2 mm.
- the reservoir may extend along an axis of the therapeutic device distance within a range from about 4 to 8 mm.
- a volume comprising a quantity of liquid formulation within a range from about 20 to about 200 uL, for example about 50 uL can be injected into the therapeutic device with the needle tip disposed on the distal end.
- FIG. 7A-2 shows a therapeutic device comprising a penetrable barrier coupled to a needle 189 of an injector 701 to inject and remove material from the device such that the liquid in the reservoir 130 is exchanged with the injected formulation.
- the needle comprises at least one lumen and may comprise a concentric double lumen needle 189DL with a distal end coupled to the inner lumen to inject formulation of the therapeutic agent into the therapeutic device and a proximal vent 189V to receive liquid into the needle when the formulation is injected.
- the vent may correspond to an opening on the distal end of the inner lumen of the needle and the outer lumen may comprise a proximal opening to inject therapeutic agent formulation into a proximal portion of the container reservoir.
- FIG. 7B-1 shows a side cross-sectional view of therapeutic device 100 comprising a retention structure having a cross-section sized to fit in an elongate incision.
- the retention strucutre shown can be combined with one or more therapeutic agents as described herein.
- the volume and RRI can be tuned to receive a quantity of the first therapeutic agent by injection
- the second therapeutic agent 1 10B may comprise a solid located in the chamber 132.
- the release rate index and volume of chamber 132 can be sized to receive a quantity of first therapeutic agent 1 10A.
- the release rate index can be sized to release therapeutic amounts of the second therapeutic agent 1 10B for a second extended time.
- the elongate cross section 120NE of the narrow portion 120N can be sized in many ways to fit the incision.
- the elongate cross section 120NE comprises a first dimension longer than a second dimension and may comprise one or more of many shpes such as dilated slot, dilated slit, lentoid, oval, ovoid, or elliptical.
- the dilated slit shape and dilated slot shape may correspond to the shape sclera tissue assumes when cut and dilated.
- the lentoid shape may correspond to a biconvex lens shape.
- the elongate cross-section of the narrow portion may comprise a first curve along an first axis and a second curve along a second axis different than the first curve.
- the container reservoir may comprise a cross-sectional profile.
- FIG. 7B-2 shows an isometric view of the therapeutic device as in FIG. 7B-1.
- FIG. 7B-3 shows a top view of the therapeutic device as in FIG. 7B-1.
- FIG. 7B-4 shows a side cross sectional view along the short side of the retention structure of the therapeutic device as in FIG. 7B-1.
- FIG. 7B-5 shows a bottom view of the therapeutic device as in FIG. 7B-1 implanted in the sclera.
- the width 712 of the blade 710 may comprise about 3 mm such that the incision comprises an opening having a perimeter of about 6 mm so as to seal the incision with the narrow portion 160P.
- perimeter 160P of barrier 160 may comprise a size slightly larger than the incision and the perimeter of the narrow portion.
- the retention structure comprises a narrow section 120N having a short distance 120NS and a long distance 120NL so as to fit in an elongate incision along the pars plana of the eye.
- the retention structure comprises an extension 122.
- the extension of the retention structure 120E comprises a short distance across 122S and a long distance across 122S, aligned with the short distance 122NS and long distance 122NL of the narrow portion 120N of the retention structure 120.
- the narrow portion 120 may comprise an indentation 1201 sized to receive the sclera.
- FIGS. 8A and 8A1 show a side cross sectional view and a top view, respectively, of therapeutic device 100 for placement substantially between the conjunctiva and the sclera.
- the therapeutic agent 110 as described herein can be injected when device 100 is implanted.
- the therapeutic device 100 comprises container 130 as described herein having penetrable barrier 184 as described herein disposed on an upper surface for placement against the conjunctiva.
- An elongate structure 172 is coupled to container 130.
- Elongate structure 172 comprises a channel 174 extending from a first opening coupled to the chamber of the container to a second opening 176 on a distal end of the elongate structure.
- the porous structure 150 as described herein is located on the elongate structure 172 and coupled to the container 130 so as to release therapeutic agent for an extended period, and a retention structure 120 comprising an extension protruding outward from the container 130 to couple to the sclera and the conjunctiva.
- the container may comprise barrier 160 as described herein that defines at least a portion of the reservoir, and the container may comprise a width, for example a diameter.
- the barrier 160 may comprise a rigid material, for example rigid silicone or rigid rubber, or other material as described herein, such that the volume of the chamber of container 130 comprises a
- the length can be sized within a range, for example within a range from about 2 to about 1 4 mm, for example within a range from about 4 to 10 mm and can be about 7 mm, for example.
- the penetrable barrier may comprise a septum disposed on a proximal end of the container, in which the septum comprises a barrier that can be penetrated with a sharp object such as a needle for injection of the therapeutic agent.
- the porous structure may comprise a cross sectional area sized to release the therapeutic agent for the extended period.
- the elongate structure 172 can be located near a center of the container 130, or may be eccentric to the center. [0340] The elongate structure 172 can be inserted into the sclera at the pars plana region as described herein.
- the barrier 160 can have a shape profile for placement between the conjunctiva and sclera.
- the lower surface can be shaped to contact the sclera and may comprise a concave shape such as a concave spherical or toric surface.
- the upper surface can be shaped to contact the conjunctivae and may comprise a convex shape such as a convex spherical or toric surface.
- the barrier 160 may comprise an oval, an elliptical, or a circular shape when implanted and viewed from above, and the elongate structure 172 can be centered or eccentric to the ellipse.
- the cross sectional diameter of the elongate structure 172 can be sized to decrease the invasiveness of device 100, and may comprise a diameter of no more than about 1 mm, for example no more than about 0.5 mm, for example no more than about 0.25 mm such that the penetrate sclera seals substantially when elongate structure 172 is removed and the eye can seal itself upon removal of elongate structure 172.
- the elongate structure 172 may comprise a needle, and channel 174 may comprise a lumen of the needle, for example a 30 Gauge needle.
- the porous structure 150 may comprise a first side a described herein coupled to the reservoir and a second side to couple to the vitreous.
- the first side may comprise a first area 150 as described herein and the second side may comprise a second area.
- the porous structure may comprise a thickness as described herein.
- the porous structure many comprise a diameter.
- the porous structure may comprise a release rate index, and the chamber of container 130 that defines the volume of reservoir 140 can be sized such that the porous structure and the volume are tuned to receive and amount of therapeutic agent injected with a volume of formulation of therapeutic agent and tuned to release therapeutic amounts for an extended time. Many release rate mechanisms as described herein can be used to tune the release rate and volume to the quantity of therapeutic agent injected as described herein.
- the volume of the reservoir 140 defined by the chamber of the container may comprise from about 5 uL to about 2000 uL of therapeutic agent, or for example from about 10 uL to about 200 uL of therapeutic agent.
- the porous structure may comprise a needle stop that limits penetration of the needle.
- the porous structure may comprise a plurality of channels configured for the extended release of the therapeutic agent.
- the porous structure may comprise a rigid sintered material having characteristics suitable for the sustained release of the material.
- Fig. 8A2 shows the therapeutic device 100 implanted with the reservoir between the conjunctiva and the scleara, such that elongate structure 172 extends through the sclera to couple the reservoir chamber to the vitreous humor.
- the porous structure 150 can be located in the viteous humor, or located between the conjunctiva and sclera, or may extend through the sclera, or combinations thereof.
- Fig. 10 shows the porous structure 150 located within the chamber of container 150 and coupled to the first opening of the elongate structure 172 so as to provide the release rate profile.
- the porous structure can cover the opening of elongate structure 172 such that therapeutic amounts are released for the extended time as described herein.
- Fig. 1 1 shows a plurality of injection ports spaced apart so as to inject and exchange the liquid of chamber of the container 130 and inject the therapeutic agent into the reservoir chamber of the container 130.
- the penetrable barrier 184 may comprise a first penetrable barrier located in a first access port formed in the barrier 160 and a second penetrable barrier located in a second access port formed in the barrier 160, and the first barrier can be separated from the second barrier by at least about 1 mm.
- the injector 701 as described above can be configured to coupled to the reservoir placed between the conjunctiva and the sclera as describe herein.
- the injector 701 can be coupled to a double lumen needle 189L such that a second lumen 189B injects therapeutic agent 1 10 from a chamber 702C into device 100, and the first lumen can be spaced apart from the second lumen with the distance extending therebetween sized to position the first lumen in the first septum as described above and the second lumen in the second septum as described above.
- the second container 703C can be coupled to a first lumen 189A that extends to the chamber of the reservoir container and receives liquid from device 100, such that liquid of device 100 is exchanged when the chamber of the reservoir container is postioned between the conjunctiva and the sclera.
- the switching valve 703V to exchange an intended amount of liquid and an intended amout of the formulation the therapeutic agent 1 10, and inject an intended amount of therapeutic agent injected into device 100, for example such that a bolus amount of therapeutic agent can be injected from device 100 as described above.
- a portion of the formulation of therapeutic agent injected into device 100 can be retaind in device 100 for release for an extended time.
- the injector 701 can be used to exchange a liquid comprising a first therapeutic agent such as an antineoplastic agent, for example a VEGF inhibitor, and a second therapeutic agent such as a COX inhibitor, for example the ketorolac, such that the first and second therapeutic agent are injected together and exchanged with a liquid in the reservoir.
- a first therapeutic agent such as an antineoplastic agent, for example a VEGF inhibitor
- a second therapeutic agent such as a COX inhibitor, for example the ketorolac
- the reservoir can be located between the sclera and the conjunctiva, or within the vitreous, or combinations thereof.
- Fig. 12 shows the elongate structure 172 coupled to the container 130 away from the center of container 130 and near and located near an end of the container.
- the first therapeutic device may comprise a device having the reservoir located in the vitreous humor and th second therapeutic device may comprise a device having the reservoir located between the conjunctiva and the sclera, in accordance with embodiments as described herein.
- a first theapeutic agent comprising an anti-neoplasia agent, such as an anti-neoplasia agent,
- antineovascular agent for example a VEGF inhibitor such as a Lucentis
- an antiinflammatory such as steroid comprising triamcinolone actendie.
- triamcinolone acetonide suspension is described supra in Examples 10 and 11 and
- the first reservoir may comprise a volume of about 125 uL and an RRI of about 0.1 such that the first reservoir is tuned to receive a 50 uL injection of Lucentis and provide a concentration of about 3 ug/mL in the vitreous humor.
- the second reservoir may comprise Triamcinolone Acetonide having an RRI of 1.2, as described in Example 1 1, supra.
- the second reservoir may be configured in parallell or in series as described herein, and provide trimcinolone acetonide for about 400 days over the course of at least 2 sequential 50 uL injections of Lucentis at day 0 and day 180, for example.
- the amount of triamcinolone acetate suspension in the second chamber can be may be increased so as to comprise about a 20 uL reservoir volume loaded with 0.8 mg using a commercial drug product (40 mg/mL triamcinolone acetonide), such that the trimcinolone acetonide can be delivered in therapeuti amounts for an extended time of at least about 800 days, corresponding to about four sequential 50 uL injections of LucentisTM at six month intervals.
- the IC50 of triamcinolone can be about 1.5nM, depending on the target assay such as such as one or more of VEGF-induced cell proliferation, or receptor binding.
- the amount of Ranibizumab in the first chamber can be agent may be increased, for example to about 2.5 mg, for example, such that the amount Ranibizumab delivered in therapeuti amounts for an extended time, and the RRI can be adjusted accordingly for example the RRI can be about 0.02 and provide about 10 ug/mL of Ranibizumab at about 6 months.
- EXAMPLE B VEGF INHIBITORS COMBINED WITH COX INHIBITORS.
- a first theapeutic agent comprising an anti-neoplasia agent, such as an anti-neoplasia agent,
- antineo vascular agent for example a VEGF inhibitor such as a Lucentis
- a non-steroidal antiinflammatory such as a COX inhibitor
- the release of the small molecule cyclcoxib through the porous frit structure 150 can be similar to triamcinolone acetonide as described supra in Examples 10 and 11 and corresponding Fig. 20.
- the first reservoir may comprise a volume of about 125 uL and an RRI of about 0.1 such that the first reservoir is tuned to receive a 50 uL injection of Lucentis and provide a concentration of about 3 ug/mL in the vitreous humor.
- the second reservoir may comprise solid celecoxib and have an RRI of 1.2, similar to that described in Example 11, supra.
- the second reservoir may be configured in parallell or in series as described herein, and provide therapeutic amounts of celecoxib.
- the amount of celecoxib solid in the second chamber can be may be increased so as to provide therapeutic amounts of celecoxib for the extended time. Based on the teahings described herein a person of ordinary skill in the art can determine the concentration of cycloscoxib in the vitreous humor to achieve therapeutic inhibition of COX for the treatment of one or more stages of AMD, and the RRI, reservoir volume and amount of solid can be determined.
- the IC50 of cyclcoxib can be approximately 40 nM, about 40 times less potent than triamcinolone acetonide.
- the celecoxib can be relased from a separate chamber, for example from a separate device, and the amount of celecoxib solid released from the separate device may comprise about 20 mg released over about 200 days, for example.
- Table 3A shows examples of COX inhibitors that can be injected into the therapeutic device.
- the COX inhibitor may comprise celecoxib, keotolac or bromefenac.
- the RRIs, volumes and conentrations are shown to release therapeutic amounts for the times indicated time, and the vitreous concentrations are shown above the IC 50 concentrations.
- Ketorolac has an initial steady state release rate profile from the suspension for 318 days with a vitreous concentration of about 0.9 ug/mL, followed by release of the reminain Ketorolac solution for about 70 days above about 0.07 ug/mL, for a total time above 0.07 of about 400 days.
- a person of ordinary skill in the art can determine many COX inhibitors suitable for release through the release mechanism with the antineoplastic agnet such as the VEGF inhibitor, for example Lucentis.
- the COX inhibitor can be combined with the VEGF inhibitor in the chamber of the therapeutic device and released together through the porous frit structure.
- the RRI of 0.02 shown for ketolac can be used with ranibizumab as described above, such that therapeutic amounts can be delivered for at least about 120 days, for example at least about 180 days.
- the formulation may comprise Ranibizumab and ketorolac intjected together into the therapeutic device.
- the values of RRI' s and concentrations of Ranibizumab and volumes as descrbied above are suitable for combination with a ketorolac suspension.
- the concentration of Ranibizumab in the formulation can be within the range from about 10 mg/ml to the upper limit of stable solubility of about 300 to 350 mg/mL.
- Additional VEGF inhibitors and COX inhibtors suitable for combination can be determined by one of ordinary skill in the art based on the teachings described herein.
- the vitreous half-life (clearance rate of the drug from the eye) is something that can be empirically determined.
- One of ordinary skill in the art could determine based upon similar MW to triamcinolone (celecoxib 381 vs.
- the IC50 can be defined as the concentration of drug which leads to a 50% inhibition in a particular assay.
- the IC50 is approximately 15 ng/ml, corresponding to the minimum inhibitory concentration desired in the target tissue (retina, choroid). As a rough approximation, one could target above this concentration in the vitreous.
- the solubility of celecoxib in water is approximately 3ug/ml, so is this relatively "water insoluble"
- the solubility of triamcinolone acetonide is about 19 ug/mL measured at 37°C in 0.2 M potassium chloride and the diffusion coefficient of 5 e-6 cm 2 /s representative of a small molecule.
- the RRI for celecoxib can be about 600x the RRI for trimacinolone acetonide based on the above solubility and IC 50 data, for example an RRI of about 60.
- Many amounts of Ranibizumab can be used, for example within a range from about 0.5 mg to about 10 mg, for example from about 1 mg to about 5 mg, for example from about 1.5 mg to about 3 mg, and the reservoir volume and release rate index can be sized based on the teaching described herein to proved the sustained release for the extended time.
- the amount of Ranibizumab in the chamber can be about 2 mg, for example, such that the amount
- Ranibizumab delivered in therapeutic amounts for an extended time and the RRI can be adjusted accordingly for example the RRI can be about 0.02 and provide about 10 ug/mL of Ranibizumab at leat about 6 months.
- Examples 1-4 are described in priority U.S. Provisional Pat. App. Ser. No. 61/371,168, filed 5 August 2010; U.S. App. Ser. No. 12/696,678, filed January 29, 2010, entitled “Posterior Segment Drug Delivery", published as U.S. Pat. App. Pub. No. 2010/0255061 (attorney docket not. 026322-003750US); and PCT/US2010/022631, published 5 August 2010 as WO2010/088548, entitled "Posterior Segment Drug Delivery”.
- Example 5 Release of protein through a cylindrical sintered porous titanium cylinder [0368] Reservoirs were fabricated from syringes and sintered porous titanium cylinders (available from Applied Porous Technologies, Inc., Mott Corporation or Chand Eisenmann Metallurgical). These were sintered porous cylinders with a diameter of 0.062 inches and a thickness of 0.039 inches prepared from titanium particles. The porosity is 0.17 with mean pore sizes on the order of 3 to 5 micrometers. The porous cylinder is characterized as 0.2 media grade according to measurements of bubble point. The porous cylinders were press-fit into sleeves machined from Delrin.
- the sleeves exposed one entire planar face to the solution in the reservoir and the other entire planar face to the receiver solution in the vials, corresponding to an area of 1.9 square millimeters.
- the tips were cut off of 1 mL polypropylene syringes and machined to accept a polymer sleeve with outer diameter slightly larger than the inner diameter of the syringe.
- the porous cylinder / sleeve was press-fit into the modified syringe.
- FIG. 13 shows the measured cumulative release of BSA through a sintered porous titanium disc and a prediction from the model describing release through a porous body.
- the Channel Parameter of 1.7 was determined via a least squares fit between the measured data and the model (MicroSoft Excel). Since the porous cylinder has equal areas exposed to the reservoir and receiving solution, the Channel Parameter suggests a tortuosity of 1.7 for porous titanium cylinders prepared from 0.2 media grade.
- FIG. 13-1 shows the measured cumulative release of BSA of FIG. 13 measured to 180 days.
- the Channel Parameter of 1.6 was determined via a least squares fit between the measured data and the model (MicroSoft Excel). This corresponds to a Release Rate Index of 0.21 mm. Since the porous cylinder has equal areas exposed to the reservoir and receiving solution, the Channel Parameter corresponds to an effective path length channel parameter of 1.6 and suggests a tortuosity of 1.6 for porous titanium cylinders prepared from 0.2 media grade.
- Example 6 Release of protein through masked sintered porous titanium cylinders
- Reservoirs were fabricated from syringes and porous sintered titanium cylinders similar to that described in Example 5.
- the porous sintered titanium cylinders (available from Applied Porous Technologies, Inc., Mott Corporation or Chand Eisenmann Metallurgical) had a diameter of 0.082 inch, a thickness of 0.039 inch, a media grade of 0.2 and were prepared from titanium particles.
- the porosity is 0.17 with mean pore sizes on the order of 3 to 5 micrometers.
- the porous cylinder is characterized as 0.2 media grade according to
- the porous cylinders were press fit into sleeves machined from Delrin.
- the sleeves exposed one entire planar face to the solution in the reservoir and the other entire planar face to the receiver solution in the vials, corresponding to an area of 3.4 square millimeters.
- the tips were cut off of 1 mL polycarbonate syringes and machined to accept a polymer sleeve with outer diameter slightly larger than the inner diameter of the syringe.
- the porous cylinder / sleeve was press fit into the modified syringe.
- a kapton film with adhesive was affixed to the surface exposed to the receiving solution to create a mask and decrease the exposed area.
- the diameter of the mask was 0.062 inches, exposing an area of 1.9 square millimeters to the receiving solution.
- the diameter of the mask was 0.027 inches, exposing an area of 0.37 square millimeters.
- Three conditions were run in this study: 1) 0.062 inch diameter mask, 100 uL donor volume, at room temperature in order to compare with reservoirs with unmasked porous cylinders in Example 5; 2) 0.062 inch diameter mask, 60 uL donor volume, at 37°C; and 3) 0.027 inch diameter mask, 60 uL donor volume, at 37°C.
- the syringes were filled with a solution containing 300 mg/mL bovine serum albumin (BSA, Sigma, A2153-00G) in phosphate buffered saline (Sigma, P3813), similar to Example 5.
- BSA bovine serum albumin
- phosphate buffered saline Sigma, P3813
- 0.02 wt% of sodium azide Sigma, 438456-5G was added as a preservative to both the BSA solution placed in the reservoirs and the PBS placed in the receiving vials and both solutions were filtered through a 0.2 micron filter. This time, the amount of BSA solution dispensed into the syringe was weighed and the amount expressed through the porous cylinder was determined by rinsing and measuring the amount of BSA in the rinse.
- the amount dispensed was 1 13 +/- 2 uL (Condition 1) and 66 +/- 3 uL (Condition 2). Subtracting off the amount in the rinse yielded a final reservoir volume of 103 +/- 5 uL (Condition 1) and 58 +/- 2 uL (Condition 2).
- the reservoirs were then placed into 5 mL vials containing 1 mL PBS at 37°C in a heating block. At periodic intervals, the reservoirs were moved to new vials containing PBS and the BSA concentrations were determined in the receiving solutions using the method described in Example 5.
- FIG. 16 shows the cumulative release of BSA protein through a masked sintered porous titanium cylinder at Condition 3 (0.027 inch diameter mask, 60 uL donor volume, at 37°C).
- This mask achieves a release rate corresponding to an effective area in between the area exposed to the reservoir and the area exposed to the receiver solution.
- a combination of the results in FIGS. 15 and 16 demonstrate that slower release is achieved using a mask that exposes a smaller area to the receiver solution.
- Example 7 Release of protein through sintered porous stainless steel cylinder (media grade 0.1) [0378]
- Prototype devices were fabricated from tubing and sintered porous stainless steel cylinders (available from Applied Porous Technologies, Inc., Mott Corporation or Chand Eisenmann Metallurgical) which are cylindrical with diameter 0.155 inch and thickness 0.188 inch prepared from 316L stainless steel particles.
- the porous cylinder is characterized as 0.1 media grade according to measurements of bubble point. This study was performed with these large, off-the-shelf porous cylinders with an area of 12 mm 2 in order to characterize the resistive properties of 0.1 media grade stainless steel.
- FIG. 17 displays the measured cumulative release of BSA through the 0.1 media grade stainless steel sintered titanium discs.
- Prototype devices were fabricated from tubing and sintered porous stainless steel cylinders (available from Applied Porous Technologies, Inc., Mott Corporation or Chand
- Eisenmann Metallurgical which are cylindrical with diameter 0.031 inch, and thickness 0.049 inch prepared from 316L stainless steel particles.
- the porous cylinder is characterized as 0.2 media grade according to measurements of bubble point. This porous cylinder was obtained as a custom order with properties determined from a previous study with a large diameter 0.2 media grade porous stainless steel cylinder (data no shown) and predictions based on the model described herein. The area of each face of this porous cylinder is 0.5 mm 2 .
- FIG. 18A displays the measured cumulative release of BSA through the 0.2 media grade sintered porous stainless steel cylinder.
- a single parameter of Porosity divided by Channel Parameter was determined to be 0.12 by least squares fit of the model to the data. Since the sintered porous structure is cylindrical, the Channel Parameter can be interpreted as effective length of the interconnecting channels that may correspond the Tortuosity, T. Using the Porosity of 0.17 determined by the vendor, the effective length of the channel that may correspond to the Tortuosity was determined to be 1.4. Furthermore, this corresponds to a PA/FL ratio (Release Rate Index) of 0.0475 mm.
- FIG. 18B displays the measured cumulative release of BSA through the 0.2 media grade sintered porous stainless steel cylinder for 180 days.
- a single parameter of Porosity divided by Channel Parameter was determined to be 0.10 by least squares fit of the model to the data. Since the sintered porous structure is cylindrical, the Channel Parameter can be interpreted an effective length of the inter-connecting channels that may correspond to the Tortuosity, T. Using the Porosity of 0.17 determined by the vendor, the effective channel length of the inter-connecting channels that may correspond to the Tortuosity was determined to be 1.7. Furthermore, this corresponds to a PA/FL ratio (Release Rate Index) of 0.038 mm.
- Example 9 Calculations of LucentisTM concentrations in the vitreous
- the vitreous concentrations of a therapeutic agent can be predicted based on the equations described herein.
- Table 4 shows the values of the parameters applied for each of Simulation 1, Simulation 2, Simulation 3, Simulation 4, and Simulation 5.
- the half-life and vitreous volume correspond to a monkey model (J. Gaudreault et al.., Preclinical
- the parameter PA/FL can be varied to determine the release rate profile.
- a person of ordinary skill in the art can determine empirically the area, porosity, length and channel fit parameter for extended release of the therapeutic agent for the extended period based on the teachings described herein. Table 4A.
- the average concentration of LucentisTM is about 46 ug/ml.
- the minimum therapeutic concentration of LucentisTM is about 0.1 ug/mL, which may correspond to about 100% VGEF inhibition (Gaudreault et al.).
- Table 4B indicates that a bolus injection of 0.5 mg LucentisTM maintains a vitreous concentration above 0.1 ug/mL for about a month whether using the measured or calculated Cmax. This is consistent with monthly dosing that has been shown to be therapeutic in clinical studies.
- Tables 4C1, 4C2, 4C3 4C4, and 4C5 show the calculated concentration of Lucentis 1M in the vitreous humor for Simulation 1, Simulation 2, Simulation 3, Simulation 4, and
- the ability of the device to release therapeutic agent for an extended time can be described by an effective device half-life.
- the effective device half-life is 29 days for delivery of LucentisTM.
- the device can be configured by selection of the reservoir volume and a porous structure with an appropriate PA/FL to achieve the desired effective half-life.
- CNV laser photocoagulation treatment-induced Grade IV choroidal neovascularization
- Table 4D shows predictions of LucentisTM vitreous concentrations for the lowest total amount of LucentisTM investigated (intravitreal injection of 5 ug on days 1, 6, 1 1, 16, 21 and 26), using the equations described herein and pharmacokinetic parameters listed in Table 4A. This data indicates that it is not necessary to achieve the high Cmax of a 0.5 mg single bolus injection in order to be therapeutic.
- FIG. 19A compares this predicted profile with that predicted for the device in Example 8. This data further supports that the release profile from a device in accordance with embodiments of the present invention may be therapeutic for at least about 6 months.
- the single injection of 500 ug corresponds to a 50 uL bolus injection of LucentisTM that can given at monthly intervals, and the range of therapeutic concentrations of LucentisTM (ranibizumab) in the vitreous extends from about 100 ug/mL to the minimum inhibitory (therapeutic) concentration of about 0.1 ug/mL at about 1 month, for example.
- LucentisTM injections 5 ug each, can be administered so as to provide a concentration in the vitreous of at least about 1 ug/mL, and the therapeutic benefit of the injections assessed as described herein.
- Table 4D
- concentration profiles of a therapeutic agent comprising Lucentis were determined as shown below based on the teachings described herein and with drug half-life of nine days for LucentisTM in the human eye.
- the examples shown below for injections of the commercially available formulation LucentisTM and the nine day half life show unexpected results, and that a volume of formulation corresponding to a montly bolus injection into the device as described herein can provide therapeutic benefit for at least about two months.
- the device volume and the porous structure can be be tuned to receive the predetermined volume of formulation and provide sustained rease for an extended time. Additonal tuning of the device can include the half-life of the therapeutic agent in the eye, for example nine days for
- LucentisTM LucentisTM
- minmimum inhibitory concentration of the therapeutic agent as deteremined based on the teachings as described herein.
- FIG. 19B shows determined concentrations of LucentisTM in the vitreous humor for a first 50 uL injection into a 25 uL device and a second 50 uL injection at 90 days.
- the calculations show that the 50 uL dosage of the monthly FDA approved bolus injection can be used to treat the eye for about 90 days, and that the injections can be repeated to treat the eye, for example at approximately 90 day intervals.
- the LucentisTM may comprise a predetermined amount of the commercially available formulation injected into the device.
- the commercially available formulation of LucentisTM has a concentration of ranibizumab of 10 mg/mL, although other concentrations can be used for example as described herein below with reference to a 40 mg/mL solution of injected ranibizumab.
- the predetermine amount corresponds to the amount of the monthly bolus injection, for example 50 uL.
- the therapeutic device may comprise a substantially fixed volume container reservoir having a volume of 25 uL, such that a first 25 uL portion of the 50 uL injection is contained in the reservoir for sustained and/or controlled release and a second 25 uL portion of the 50 uL injection is passed through the porous structure and released into the vitreous with a 25 uL bolus.
- the filling efficiency of the injection into the device may comprise less than 100%, and the reservoir volume and injection volume can be adjusted based on the filling efficiency in accordance with the teachings described herein.
- the filling efficiency may comprise approximately 90%, such that the first portion comprises approximately 22.5 uL contained in the chamber of the container reservoir and the second portion comprises approximately 27.5 uL passed through the device for the 50 uL injected into the therapeutic device.
- the initial concentration of LucentisTM in the vitreous humor corresponds to about 60 ug/mL immediately following injection into the reservoir device.
- the concentration of LucentisTM in the vitreous humor decreases to about 3.2 ug/mL at 90 days.
- a second 50 uL injection of LucentisTM approximately 90 days after the first injection increases the concentration to about 63 ug/mL.
- FIG. 19C shows determined concentrations of LucentisTM in the vitreous humor for a first 50 uL injection into a 32 uL device and a second 50 uL injection at a time greater than 90 days.
- the calculations show that the 50 uL dosage of the monthly FDA approved bolus injection can be used to treat the eye for about 90 days, and that the injections can be repeated to treat the eye, for example at approximately 90 day intervals.
- the LucentisTM may comprise a predetermined amount of the commercially available formulation injected into the device. The predetermine amount corresponds to the amount of the monthly bolus injection, for example 50 uL.
- the therapeutic device may comprise a substantially fixed volume container reservoir having a volume of 32 uL, such that a first 32 uL portion of the 50 uL injection is contained in the reservoir for sustained and/or controlled release and a second 18 uL portion of the 50 uL injection is passed through the porous structure and released into the vitreous with an 18 uL bolus.
- the filling efficiency of the injection into the device may comprise less than 100%, and the reservoir volume and injection volume can be adjusted based on the filling efficiency in accordance with the teachings described herein. For example, the filling efficiency may comprise approximately 90%, such that the first portion comprises
- the initial concentration of LucentisTM in the vitreous humor corresponds to abbut 45 ug/mL immediately following injection into the reservoir device.
- the concentration of LucentisTM in the vitreous humor decreases to about 4 ug/mL at 90 days.
- a second 50 uL injection of LucentisTM approximately 90 days after the first injection increases the concentration to about 50 ug mL.
- the concentration of LucentisTM in the vitreous humor decreases to about 4 ug/mL at 180 days after the first injection and 90 days after the second injection.
- FIG. 19D shows determined concentrations of LucentisTM in the vitreous humor for a first 50 uL injection into a 50 uL device and a second 50 uL injection at 90 days.
- the calculations show that the 50 uL dosage of the monthly FDA approved bolus injection can be used to treat the eye for about 90 days, and that the injections can be repeated to treat the eye, for example at approximately 90 day intervals.
- the LucentisTM may comprise a predetermined amount of the commercially available formulation injected into the device.
- the filling efficiency of the injection into the device may comprise less than 100%, and the reservoir volume and injection volume can be adjusted based on the filling efficiency in accordance with the teachings described herein.
- the filling efficiency may comprise
- the initial concentration of LucentisTM in the vitreous humor corresponds to about 11 ug/mL immediately following injection into the reservoir device.
- the concentration of LucentisTM in the vitreous humor decreases to about 5.8 ug/mL at 90 days.
- a second 50 uL injection of LucentisTM approximately 90 days after the first injection increases the concentration to about 17 ug/ mL.
- the concentration of LucentisTM in the vitreous humor decreases to about 5,8 ug/mL at 180 days after the first injection and 90 days after the second injection.
- FIG. 19E shows determined concentrations of Lucentis in the vitreous humor for a first 50 uL injection into a 50 uL device and a second 50 uL injection at 90 days. The calculations show that the 50 uL dosage of the monthly FDA approved bolus injection can be used to treat the eye for about 130 days, and that the injections can be repeated to treat the eye, for example at approximately 120 day intervals.
- the LucentisTM may comprise a
- the filling efficiency of the injection into the device may comprise less than 100%, and the reservoir volume and injection volume can be adjusted based on the filling efficiency in accordance with the teachings described herein.
- the filling efficiency may comprise approximately 90%, such that the first portion comprises approximately 45 uL contained in the chamber of the reservoir container and the second portion comprises approximately 5 uL passed through the device for the 50 uL of LucentisTM injected into the therapeutic device.
- the initial concentration of LucentisTM in the vitreous humor corresponds to about 1 1 ug/mL immediately following injection into the reservoir device.
- concentration of LucentisTM in the vitreous humor decreases to about 4 ug/mL at 133 days.
- a second 50 uL injection of LucentisTM approximately 130 days after the first injection increases the concentration to about 15 ug/ mL.
- the concentration of LucentisTM in the vitreous humor decreases to about 4 ug/mL at 266 days after the first injection and 90 days after the second injection.
- FIGS. 19B to 19P make reference to injections of commercially available off the shelf formulations of LucentisTM
- therapeutic device 100 can be similarly configured to release many formulations of the therapeutic agents as described herein, for example with reference to Table 1 A and the Orange Book of FDA approved formulations and similar books of approved drugs in many countries, unions and jurisdictions such as the European Union.
- FIG. 19F shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 50 uL device having a release rate index of 0.05.
- the concentration of ranibizumab in the vitreous humor peaks at around 9 ug/mL and is at or above 4 ug/mL for about 145 days.
- the concentration remains above about 1 ug/mL for about 300 days.
- the concentration is about 0.6 ug/mL at 360 days, and can be suitable for treatment with a single injection up to one year, based on a minimum inhibitory concentration of about 0.5.
- the minimum inhibitory concentration can be determined empirically by a person of ordinary skill in the art based on the teachings described herein.
- FIG. 19G shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 75 uL device having a release rate index of 0.05.
- the concentration of ranibizumab in the vitreous humor peaks at around 6.5 ug/mL and is at or above 4 ug/mL for about 140 days. The concentration remains above about 1 ug/mL for about 360 days.
- FIG. 19H shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 100 uL device having a release rate index of 0.05.
- the concentration of ranibizumab in the vitreous humor peaks at around 5 ug/mL and is at or above 4 ug/mL for about 1 16 days.
- the concentration remains above about 1 ug/mL for more than 360 days and is about 1.5 ug/mL at 360 days.
- FIG. 19J shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 150 uL device having a release rate index of 0.05.
- the concentration of ranibizumab in the vitreous humor peaks at around 3.5 ug/mL and does not equal or exceed 4 ug/mL.
- the concentration remains above about 1 ug/mL for more than 360 days and is about 1.5 ug/mL at 360 days.
- FIG. 19K shows determined concentrations of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 100 uL device having a release rate index of 0.1. These determined concentrations are similar to the determined concentrations of FIG. 19F, and show that the release rate index of the porous structure can be tuned with the device volume to provide therapeutic concentration profile for an extended time. For example, by doubling the volume of the reservoir so as to half the concentration of therapeutic agent in the vitreous, the release rate index can be doubled so as to provide a similar therapeutic concentration profile.
- the concentration of ranibizumab in the vitreous humor peaks at around 9 ug/mL and is at or above 4 ug/mL for about 145 days. The concentration remains above about 1 ug/mL for about 300 days. The concentration is about 0.6 ug/mL at 360 days.
- FIGS. 19L to 19P show examples of release rate profiles with 125 uL reservoir devices having the RRI vary from about 0.065 to about 0.105, such that these devices are tuned to receive the 50 uL injection of LucentisTM and provide sustained release above a minimum inhibitory concentration for at least about 180 days. These calculations used a drug half life in the vitreous of 9 days to determine the profiles and 100% efficiency of the injection.
- FIG. 19L shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.105.
- the concentration of ranibizumab in the vitreous at 180 days is about 3.128 ug/mL.
- FIG. 19M shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.095.
- the concentration of ranibizumab in the vitreous at 180 days is about 3.174 ug/mL.
- FIG. 19N shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.085.
- the concentration of ranibizumab in the vitreous at 180 days is about 3.185 ug/mL.
- FIG. 190 shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.075.
- the concentration of ranibizumab in the vitreous at 180 days is about 3.152 ug/mL.
- 19P shows determined concentration profiles of ranibizumab in the vitreous humor for a 50 uL LucentisTM injection into a 125 uL reservoir device having a release rate index of 0.065.
- the concentration of ranibizumab in the vitreous at 180 days is about 3.065 ug/mL.
- the optimal RRI for the concentration of ranibizumab at 180 days for a reservoir volume of 125 uL and a 50 uL injection of LucentisTM can be calculated based on the equations as described herein, and is about 0.085. Although the optimal value is 0.085, the above graphs show that the reservoir and release rate index can be tuned to provide therapeutic amounts of ranibizumab above a minimum inhibitory concentration of 3 ug/mL with many values of the RRI and reservoir volume, for example values within about +/-30% to +/-50% of the optimal values for the predetermined quantity of LucentisTM formulation.
- Table 4E shows values of parameters used to determine the ranibizumab
- the therapeutic concentration profiles of examples of FIGS. 19B to 19P were determined with a nine day half-life of the drug in the vitreous humor of the human eye.
- the therapeutic concentration profiles can be scaled in accordance with the half life of the therapeutic agent in the eye. For example, with an eighteen day half life, the concentration in these examples will be approximately twice the values shown in the graph at the extended times, and with a 4.5 day half-life, the concentrations will be approximately half the values shown with the extended times.
- a drug half life of eighteen days instead of nine days will correspond to a concentration of about 1.4 ug/mL at 360 days instead of about 0.6 ug/mL as shown in FIGS. 19F and 19K.
- This scaling of the concentration profile based on drug half life in the vitreous can be used to tune the volume and sustained release structures of the therapeutic device, for example in combination with the minimum inhibitory concentration.
- a person of ordinary skill in the art can determine the release rate index and volume of the therapeutic agent based on the volume of formulation injected into the device and minimum inhibitory concentration. This tuning of the device volume and release rate index based on the volume of formulation injected can produce unexpected results. For example, with a clinically beneficial minimum inhibitory concentration of about 4 ug/mL, a single bolus injection corresponding to a one month injection can provide a therapeutic benefit for an unexpected three or more months, such as four months. Also, for a clinically beneficial minimum inhibitory concentration of at least about 1.5 ug/mL, a single bolus injection corresponding to a one month injection can provide a therapeutic benefit for an unexpected twelve or more months.
- concentration can be determined empirically based on clinical studies as described herein.
- FIGS. 19F to 19K assumed a filling efficiency of one hundred percent, a person of ordinary skill in the art based on the teachings as described herein can determine the release rate profiles for filling efficiencies less than 100%, for example with 90% filling efficiency as shown above. Such filling efficiencies can be achieved with injector apparatus and needles as described herein, for example with reference to FIGS. 7, 7A, 7A1 and 7A2. [0415] FIG.
- 19Q shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL concentrated LucentisTM (40 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about nine days.
- 19R shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL concentrated LucentisTM (40 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about five days.
- FIG. 19S shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL standard LucentisTM (10 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about nine days.
- FIG. 19T shows determined concentrations of ranibizumab in the vitreous humor for a 10 uL standard LucentisTM (10 mg/mL) injection into a 10 uL device having a release rate index of 0.01 and in which the ranibizumab has a half life in the vitreous humor of about five days.
- FIG. 20 shows a calculated time release profile of a therapeutic agent suspension in a reservoir as in Example 10.
- a device with a 10 uL reservoir volume and Release Rate Index of 1.2 mm can produce substantially constant drug concentration amounts in the human vitreous for approx. 400 days. Additional experimental and clinical studies based on the teachings described herein can be conducted to determine the release rate profile in situ in human patients, and the drug reservoir volume and release rate index configured appropriately for therapeutic benefit for a target time of drug release. The substantially constant drug concentration amounts can provide substantial therapy and decrease side effects. Similar studies can be conducted with many suspensions of many therapeutic agents as described herein, for example suspensions of corticosteroids and analogues thereof as described herein.
- Example 12 Measured of release rate profiles for AvastinTM through the porous frit structures coupled to reservoirs of different sizes and dependence of release rate profile on reservoir size.
- FIG. 21 shows a release rate profiles of therapeutic devices comprising substantially similar porous frit structures and a 16 uL reservoir and a 33 uL reservoir.
- the release rate index of each frit was approximately 0.02.
- the release rate for two therapeutic devices each comprising a 16 uL reservoir and two therapeutic devices each comprising a 33 uL reservoir are shown.
- the device comprising the 33 uL reservoir released the AvastinTM at approximately twice the rate of the device comprising 16 uL reservoir.
- Example 13 Measured release rate profiles for AvastinTM through the porous frit structures.
- FIG. 22A shows cumulative release for AvastinTM with porous frit structures having a thickness of 0.049".
- the experiments used 25 mg/mL AvastinTM; Frit #2 (0.031 x 0.049", media grade 0.2 um, 316L SS, Mott Corporation); Machined polycarbonate surrogate with screw; Reservoir Volume 37 uL;37C.
- the device number and corresponding RRI's for each tested device are listed in Table 5B below. The determined RRI based on measurements is 0.02, consistent with the model for release of the therapeutic agent as described herein.
- the RRI for each device can be used to determine the release of the therapeutic agent, and the porous structure can be further characterized with gas flow as described herein to determine the RRI prior to placement in the patient.
- FIG. 22B 1 shows cumulative release for Avastin with porous frit structures having a thickness of 0.029".
- the experiments used 25 mg/mL AvastinTM; Frit #3 (0.038 x 0.029", media grade 0.2 um, 316L SS, Mott Corporation); Machined polycarbonate surrogate with screw; Reservoir Volume 37 uL; 37C.
- the device number and corresponding RRPs for each tested device are listed in Table 5C below.
- the determined RRI based on measurements is 0.034, consistent with the model for release of the therapeutic agent as described herein.
- the RRI for each device can be used to determine the release of the therapeutic agent, and the porous structure can be further characterized with gas flow as described herein to determine the RRI prior to placement in the patient.
- FIG. 22B2 shows rate of release for Avastin with porous frit structures having a thickness of 0.029" as in FIG. 22B 1.
- the rate of release can be determined from the measurements and the cumulative release.
- the outliers in this data can be related to measurement error, such as contamination that provides a signal in the mBCA protein assay.
- FIG. 23A shows cumulative release for AvastinTM with a reservoir volume of 20 uL.
- the experiment used 25 mg/mL AvastinTM; Frit #6 (0.038 x 0.029", media grade 0.2 um, 316L SS, Mott Corporation); Machined polycarbonate surrogate with screw; 37C.
- the determined RRI based on measurements is 0.05 mm, consistent with the model for release of the therapeutic agent as described herein.
- FIG. 23A-1 shows cumulative release to about 90 days for AvastinTM with a reservoir volume of 20 uL as in FIG. 23A.
- the RRI of 0.053 mm corresponds substantially to the RRI of 0.05 of FIG. 23 and demonstrates stability of the release of therapeutic agent through the porous structure.
- FIG. 23B shows rate of release as in FIG. 23A.
- the release rate data show a rate of release from about 5 ug per day to about 8 ug per day. Although the initial release rate at the first day is slightly lower than subsequent rates, the rate of release is sufficiently high to provide therapeutic effect in accordance with the drug release model. Although there can be an initial period of about a few days for the release rate profile to develop, possibly related to wetting of the interconnecting channels of the porous structure, the release rate profile corresponds substantially to the release rate index (RRI) of 0.05.
- RRI release rate index
- a person of ordinary skill in the art could determine the release rate profile with additional data for an extended time of at least about one month, for example at least about three months, six months or more, so as to determine the release rate profile for an extended time.
- FIG. 23B-1 shows rate of release as in FIG. 23 A- 1.
- FIG. 24A shows cumulative release for AvastinTM with a 0.1 media grade porous frit structure. This experiment used: 25 mg/mL AvastinTM; Frit #5 (0.038 x 0.029", media grade 0.1 um, 316L SS, Mott Corporation); Machined polycarbonate surrogate with screw; Reservoir Volume 20 uL; 37C. The determined RRI based on measurements is 0.03, consistent with the model for release of the therapeutic agent as described herein.
- FIG. 24A- 1 shows cumulative to about 90 days release for AvastinTM with a 0.1 media grade porous frit structure as in FIG. 24A.
- the release rate of 0.038 mm corresponds substantially to the relase rate of 0.03 of FIG. 24A and demonstrates the stability of release of the therapeutic agent through the porous structure.
- FIG. 24B shows rate of release as in FIG. 24A.
- the release rate data show a rate of release from about 2 ug per day to about 6 ug per day. Although the initial release rate at the first day is slightly lower than subsequent rates, the rate of release is sufficiently high to provide therapeutic effect in accordance with the drug release model. Although there can be an initial period of a few days for the release rate profile to develop, possibly related to wetting of the interconnecting channels of the porous structure, the release rate profile corresponds substantially to the release rate index (RRI) of 0.03.
- RRI release rate index
- a person of ordinary skill in the art could determine the release rate profile with additional data for an extended time of at least about one month, for example at least about three months, six months or more, so as to determine the release rate profile for an extended time.
- FIG. 24B-1 shows rate of release as in FIG. 24A-1.
- Example 14 Determination of Therapeutic Device Size and Lifetime based on Minimum Inhibitory Concentration In Vivo of Therapeutic Agent
- concentration in the reservoir may correspond to the useful lifetime of the device, or time between injections of therapeutic agent into the reservoir or other replacement of the therapeutic agent.
- Table 6A shows the number days of therapeutic agent is released from the device with concentration amounts at or above the MIC. These number of days correspond to an effective lifetime of the device or effective time between injections into the device.
- the calculations show the number of days of the extended time release based the RRI and MIC for a 20 uL reservoir volume having a drug concentration disposed therein of 10 mg/ml.
- the RRI ranged from 0.01 to 0.1 and the MIC ranged from 0.1 to 10, and can be determined with experimental and clinical studies as described herein.
- the half-life of therapeutic agent in the vitreous was modeled as 9 days, based on human data.
- the Cmax indicates the maximum concentration of therapeutic agent in the vitreous humor, for example within a few days of placement or injection of the therapeutic agent in the device
- the device can maintain the concentration of therapeutic agent for about 756 days, 385 days, 224 days, and 62 day for MIC's of 0.1 , 0.5, 1, 2 and 4 ug/ml, respectively.
- the therapeutic agent may comprise LucentisTM having an MIC of about 0.5 and the device may maintain therapeutic concentrations of the agent for one year.
- These numerical data also show a concentration of therapeutic agent released from the device within a range of the current clinical bolus injections.
- the Cmax ranges from 2.1 to 1 1.9 based on the RRI from 0.01 to 0.1 respectively, such that the maximum release of therapeutic agent such as LucentisTM is within a safe range for the patient.
- a person of ordinary skill in the art can conduct experiments to determine the stability of the therapeutic agent such as LucentisTM in the reservoir, and adjust the size of the reservoir, time between injections or removal.
- the therapeutic agent can be selected and formulated so as to comprise a stability suitable for use in the therapeutic device.
- the embodiments of Table 6B include similar components to the embodiments of Table 6A and the improved time above MIC achieved with concentration of 40 mg/ml.
- the time above the MIC can be 1079, 706, 546, 385, 225, 95, for MIC's of 0.1 0.5, 1 , 2, 4, and 7 ug/ml, respectively.
- the therapeutic agent may comprise LucentisTM having an MIC of about 0.5 and the device may maintain therapeutic concentrations of the therapeutic agent for about 2 years.
- a person of ordinary skill in the art can conduct experiments to determine the stability of the therapeutic agent such as LucentisTM in the reservoir, and adjust the size of the reservoir, time between injections or removal.
- the therapeutic agent can be selected and formulated so as to comprise a stability suitable for use in the therapeutic device.
- the embodiments of Table 6B include similar components to the embodiments of Table 6A and the improved time above MIC achieved with concentration of 40 mg/ml.
- the time above the MIC can be 2706, 1737, 1347, 944, 542 and 218, for MIC's of 0.1 0.5, 1 , 2, 4, and 7 ug/ml, respectively.
- the therapeutic agent may comprise LucentisTM having an MIC of about 0.5 and the device may maintain therapeutic concentrations of the therapeutic agent for more than about 2 years.
- the Cmax ranges from 9.1 to 64.7 ug/ml based on the RRI from 0.01 to 0.1 respectively, such that the maximum release of therapeutic agent such as Lucentis is within a safe range for the patient.
- a person of ordinary skill in the art can conduct experiments to determine the stability of the therapeutic agent such as LucentisTM in the reservoir, and adjust the size of the reservoir, time between injections or removal.
- the therapeutic agent can be selected and formulated so as to comprise a stability suitable for use in the therapeutic device.
- the 50 uL reservoir may comprise an expanded configuration of the reservoir after injection of the therapeutic device.
- the reservoir and/or quantity of therapeutic agent can be adjusted so as to provide release for a desired extended time.
- the porous frit structure as described herein can be used with many therapeutic agents, and may limit release of therapeutic agent that has degraded so as to form a particulate, for example.
- Table 6D shows examples of sizes of therapeutic devices that can be constructed in accordance with the teachings described herein, so as to provide a suitable volume of the drug reservoir within the container and such devices may comprise many lengths, widths and structures as described herein.
- the frit outside diameter (hereinafter "OD") can be configured in many ways and may comprise about 1mm, for example, or about 0.5 mm.
- the length of the frit may comprise about 1 mm.
- the volume of the frit can be, for example, about 0.785 uL, or about 0.196 uL, for example.
- the volume of the reservoir can be from about 0.4 uL to about 160 uL, for example.
- the volume of the therapeutic device can be from about 0.6 uL to about 157 uL, and can be positioned in many ways, for example with a lumen and may comprise a substantially fixed volume reservoir or an expandable reservoir.
- the cross sectional width of the device may correspond to many sizes, for example many radii, and the radius can be within a range from about 0.3 mm to about 3.5 mm, for example.
- the cross-section width and corresponding diameters of the device can be within a range from about 0.6 mm to about 7 mm.
- the length of the device, including the porous structure, container and retention structure can be many sizes and can be within a range from about 2 mm to about 4 mm, for example.
- the device may comprise a substantially fixed diameter, or alternatively can be expandable, and may comprise fixed or expandable retention structures, as described herein.
- FIG. 25A shows cumulative release for fluorescein through a 0.2 media grade porous frit structure.
- the experiment used 2 mg/mL Fluorescein sodium; Frit #2 (0.031 x 0.049", media grade 0.2 um, 316L SS, Mott Corporation); Machined polycarbonate surrogate with screw; 37C.
- the fluorescein samples were assayed by UV absorbance at 492 nm with a plate reader. The determined RRI based on measurements is 0.02, consistent with the model for release of the therapeutic agents as described herein.
- FIG. 25 A- 1 shows cumulative release to about 90 days for fluorescein through a 0.2 media grade porous frit structure as in FIG. 25A.
- the mean RRI based upon the first four data points was 0.02 mm.
- the mean RRI to release for 90 days (excluding the first point) is 0.026 mm.
- FIG. 25B shows rate of release as in FIG. 25A.
- the release rate data show a rate of release from about 1.0 ug per day to about 1.8 ug per day. Although the initial release rate at the first day is slightly lower than subsequent rates, the rate of release is sufficiently high to provide therapeutic effect in accordance with the drug release model. Although there can be an initial period of about a day for the release rate profile to develop, possibly related to wetting of the interconnecting channels of the porous structure, the release rate profile corresponds substantially to the release rate index (RRI) of 0.02.
- RRI release rate index
- a person of ordinary skill in the art could determine the release rate profile with additional data for an extended time of at least about one month, for example at least about three months, six months or more, so as to determine the release rate profile for an extended time.
- FIG. 25B-1 shows rate of release as in FIG. 25A-1.
- Example 15B Measured release rate profiles for LucentisTM through the porous frit structures.
- Table 6E shows results for 39 out of 48 devices were included in the table and graphs shown below.
- the data from the in vitro studies shown in Table 6E show that LucentisTM can be delivered with the device having porous frit structure.
- the diameter ranged from 0.031" to 0.038", and the length ranged from 0.029 to 0.049.
- the media grade ranged from 0.1 to 0.3, and the RRI ranged from 0.014 to 0.090.
- the data show very low variability suitable in in vivo human treatment, with the %CV below 10% in all insances, and less than 3% for four of five device configurations measured.
- FIG. 25C shows cumulative release to about thirty days for LucentisTM through a 0.2 media grade porous frit structure having a diameter of 0.038 in and a length (thickness) of 0.029, corresponding to a release rate of 0.061 as shown in the second row of Table 6E.
- FIG. 25D shows rates of release of the devices as in FIG. 25C.
- FIG. 25E shows cumulative relase to about thirty days for LucentisTM for 30 uL devices having a RRI's from about 0.090 to about 0.015.
- FIG. 25F shows rates of release of the devices as in FIG. 25E.
- These above experimentally measured data show stable release of the LucentisTM for 30 days for a wide range of frit diameters, thickesses and media grades consistent with the release rate model of the porous structure and reservoir as described herein.
- the media grade, thickness, diameter and reservoir volume can be tuned to provide sustained release for a predetermined period of time above a predetermined targeted minimum inhibitory concentration.
- AvastinTM and Fluorescein data show that stable release can be achieved for extended times for many therapeutic agents consistent with the release model as described herein.
- FIGS. 26A and 26B show scanning electron microscope images from fractured edges of porous frit structures of 0.2 media grade and 0.5 media grade porous material, respectively.
- the commercially available samples were obtained from Mott Corporation and comprised 316L stainless steel. The samples were mechanically fractured so as to show the porous structure and interconnecting channels within the material to release the therapeutic agent.
- the micrograph images show a plurality of interconnecting channels disposed between openings of the first surface and openings of the second surface.
- FIGS. 27 A and 27B show scanning electron microscope images from surfaces of porous frit structures of media grade of 0.2 and 0.5, respectively, from the samples of Figs 26A and 26B.
- the images show a plurality of openings on the surface connected with
- Example 17 Porous Frit Structure Mechanical Flow Testing to Identify Porous Frit Structures Suitable for Use with Therapeutic Agent Delivery Devices
- the relative characteristics of sample elements can be determined by subjecting the frit to a number of mechanical tests, including but not limited to pressure decay and flow. These tests can be combined with drug release rate information, for example the RRI, so as to determine the release profile of the devices. These tests can be used with the porous structure positioned on the therapeutic device, so as to quantify flow through the porous structure of the device and determine suitable of the porous structure. Similar tests can be used to quantify the porous structure prior to mounting on the therapeutic device. At least some of the therapeutic devices can be evaluated with the gas flow of the porous structure mounted on a partially assembled therapeutic device, for example as a quality control check.
- the flow test can be performed on the partially assembled or substantially assembled therapeutic device prior to insertion of the therapeutic agent into the reservoir and prior to insertion into the patient, so as to ensure that the porous structure is suitable for release of the therapeutic agent and affixed to the device, for example a support of the therapeutic device.
- test methods above may use a mechanical connection of the test specimen to the test hardware and a number of techniques have been explored and employed.
- These fixtures include a both a means of reliably securing the specimen (such as heat recoverable tubing, elastic tubing, press fits into relatively rigid components, etc.) and a means of coupling (such as a luer, barbed fitting, quick connect coupling, etc.) that allow convenient and repeatable attachment to the test hardware.
- FIG. 28 shows a pressure decay test and test apparatus for use with a porous structure so as to identify porous frit structures suitable for use with therapeutic devices in accordance with embodiments described herein.
- One method of pressure decay testing is performed with the hardware shown schematically in FIG. 28.
- An initial pressure is applied to the system by an outside source such as a syringe, compressed air, compressed nitrogen, etc.
- the manometer may be configured to display simply the source gage pressure, or the actual differential pressure across the specimen.
- One side of the fixtured specimen is normally open to atmosphere, creating a pressure which will decay at a rate determined by the properties of the frit being tested.
- the instantaneous pressure may be measured by a pressure transducer that converts and supplies a signal to a data acquisition module (DAQ) that transfers data to a computer.
- DAQ data acquisition module
- the rate of pressure drop is then recorded and can be used for comparison to the performance of other frits or an acceptability requirement/specification.
- This comparison may be made by grossly comparing the pressure at a given time, or by directly comparing the output pressure decay curves.
- An example test procedure would pressurize the system to slightly greater than 400 mmHg as displayed by the manometer.
- the computer and DAQ are configured to begin data acquisition as the pressure drops below 400 mmHg, and a data point is taken approximately every .109 seconds. While the test can be stopped at any time, it is likely that standard discreet points along the course of pressure decay data would be selected so as to allow direct comparison of frit flow performance (e.g. time for decay from 400 mmHg to 300 mmHg, and from 400 mmHg to 200 mmHg.)
- Example 17B Pressure Decay Test to Identify Porous Structures Suitable for Use with Therapeutic Drug Delivery Devices.
- FIG. 29 shows a pressure flow test and test apparatus suitable for use with a porous structure so as to identify porous frit structures suitable for use with therapeutic devices in accordance with embodiments described herein.
- flow thru the test specimen can also be characterized.
- the source pressure is constantly regulated to a known pressure and the flow of a working fluid is allowed to flow thru a mass flow meter and then thru the fixtured test frit.
- the specific characteristics of the frit determine that rate at which the working fluid will flow through the system.
- pressure at the otherwise open end of the fixture test frit may be regulated to control the backpressure, and therefore the pressure drop across the specimen.
- a regulated compressed cylinder would supply the system with a constant source pressure of 30 psig and a constant back pressure of 1 psig.
- the test fluid would flow through the test frit at a characteristic rate (which is dependent on the pressure, but is expected to be in the 10-500 seem range) as measured by the mass flow meter.
- Example 17C Determination of Therapeutic Release Rate Based on Gas Flow
- the above partially populated table shows the amount and nature of frit data that can collected. It is contemplated to use some form of non-destructive testing (i.e. not drug release testing) so as to enable: a) QC receiving inspection testing of frits b) QC final device assembly testing
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CN103153316A (en) | 2013-06-12 |
US11679027B2 (en) | 2023-06-20 |
JP2013538082A (en) | 2013-10-10 |
AU2011285548B2 (en) | 2014-02-06 |
CN103153316B (en) | 2015-08-19 |
WO2012019139A9 (en) | 2013-03-28 |
US10617557B2 (en) | 2020-04-14 |
US20200405537A1 (en) | 2020-12-31 |
EP2600876A4 (en) | 2014-01-15 |
EP2600876A1 (en) | 2013-06-12 |
US20130274691A1 (en) | 2013-10-17 |
AU2011285548A1 (en) | 2013-03-07 |
JP6111194B2 (en) | 2017-04-05 |
CA2807537C (en) | 2018-09-18 |
EP2600876B1 (en) | 2015-04-29 |
CA2807537A1 (en) | 2012-02-09 |
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