WO2007142916A2 - Materials formable in situ within a medical device - Google Patents
Materials formable in situ within a medical device Download PDFInfo
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- WO2007142916A2 WO2007142916A2 PCT/US2007/012639 US2007012639W WO2007142916A2 WO 2007142916 A2 WO2007142916 A2 WO 2007142916A2 US 2007012639 W US2007012639 W US 2007012639W WO 2007142916 A2 WO2007142916 A2 WO 2007142916A2
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L24/00—Surgical adhesives or cements; Adhesives for colostomy devices
- A61L24/04—Surgical adhesives or cements; Adhesives for colostomy devices containing macromolecular materials
- A61L24/046—Surgical adhesives or cements; Adhesives for colostomy devices containing macromolecular materials obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P9/00—Drugs for disorders of the cardiovascular system
- A61P9/10—Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61F—FILTERS IMPLANTABLE INTO BLOOD VESSELS; PROSTHESES; DEVICES PROVIDING PATENCY TO, OR PREVENTING COLLAPSING OF, TUBULAR STRUCTURES OF THE BODY, e.g. STENTS; ORTHOPAEDIC, NURSING OR CONTRACEPTIVE DEVICES; FOMENTATION; TREATMENT OR PROTECTION OF EYES OR EARS; BANDAGES, DRESSINGS OR ABSORBENT PADS; FIRST-AID KITS
- A61F2/00—Filters implantable into blood vessels; Prostheses, i.e. artificial substitutes or replacements for parts of the body; Appliances for connecting them with the body; Devices providing patency to, or preventing collapsing of, tubular structures of the body, e.g. stents
- A61F2/02—Prostheses implantable into the body
- A61F2/04—Hollow or tubular parts of organs, e.g. bladders, tracheae, bronchi or bile ducts
- A61F2/06—Blood vessels
- A61F2/07—Stent-grafts
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- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y10—TECHNICAL SUBJECTS COVERED BY FORMER USPC
- Y10S—TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y10S623/00—Prosthesis, i.e. artificial body members, parts thereof, or aids and accessories therefor
- Y10S623/924—Material characteristic
- Y10S623/926—Synthetic
Definitions
- the field of the invention relates to flowable precursors that form solid materials within an implanted medical device, for example an arterial prosthesis placed inside a natural blood vessel to treat an aneurysm.
- AAA Abdominal Aortic Aneurysms
- aorta Abdominal Aortic Aneurysms
- the pressure of the blood pushes against the weakened wall, causing it to enlarge.
- Blood pools in the enlarged area, usually without forming a firm clot.
- AAA is usually the result of degeneration in the media of the arterial wall, resulting in a slow and continuous dilatation of the lumen of the vessel.
- Ruptured AAA is about the 13th-leading cause of death in the United States, causing an estimated 15,000 deaths per year. While more than 500,000 Americans have been diagnosed with aortic aneurysms, less than 100,000 are treated due to shortcomings of current devices and the risk of open surgical procedures.
- AAA Clips and open surgery have been the traditional interventional treatments for AAA. More recently, less invasive techniques have been attempted, such as introducing a coil into the aneurysm that triggers blood clotting. Of those AAA' s that are repaired, only about 30,000 procedures are minimally invasive. Other approaches have involved placing endografts across the aneurysm, so that blood can flow through the lumen of the graft and reduce the pressure on the aneurysm wall to prevent its enlargement and rupture. Stents have been used with the endografts to facilitate their placement and stabilize them in the patient. Conventional endograft devices, however, can be a poor fit for aneurysms, which can have complex three-dimensional geometries. Further, aneurysms can change shape over time leading to failure of an implanted graft and/or stent.
- an endograft equipped with suitable expandable members may be securely positioned with a lumen or lumens that allow blood to flow through the aorta and isolation of the aneurisrnal sac.
- the aneurismal sac without blood flowing into it, is less likely to rupture and may remodel to a less dangerous condition, e.g., by collapsing around the endograft that bridges the sac.
- Other expandable and tillable devices for treating an AAA are described, for instance, in U.S. Pat. No. 6,312,462, in U.S. Pat. Pub. No. 2004/0204755 published October 14 2004, and in U.S. Application Serial No. US2006/0025853A1 filed on July 22, 2005 which are hereby incorporated herein by reference to the extent that they do not contradict explicit disclosure of this specification.
- a filler for an expandable member should have certain characteristics.
- certain embodiments of the technique are directed to a method of forming a material in situ in a biocompatible expandable member comprising, for instance, increasing a volume of an expandable member of a medical device within a patient by delivering a water soluble polymer precursor in a flowable aqueous solution into the expandable member.
- Functional groups on the polymer precursor undergo a single or combined mechanisms, such as covalent bonding, ionic complex, thermal transition, to form a solid and nonbiodegradable material having a swellability of less than about, e.g., 20% v/v and having a Young's modulus of at least about 1 kPa or at least about 10 kPa or at least about 100 kPa or at least about 1 MPa or at least about lOMPa within about 30 seconds to about 30 minutes of initiating a chemical reaction of the functional groups to form the solid material, e.g., by free radical initiation or mixing another precursor having reactive functional groups with the first precursor, hi some embodiments, the polymeric precursor comprises at least 100 MW or at least 4,000 MW of polyethylene oxide and acrylate functional groups.
- One variation includes using two precursors with molecular weights that are different by a factor of about 10, with the smaller precursor optionally having a molecular weight of less than about 2000 or less than about 1000.
- Materials formed by these techniques may have aqueous solvent intermixed therein, and may include intermixed buffering agents.
- Another variation includes changing the concentration of reactant solutions to obtain the hardened material.
- Some embodiments of the invention relate to a medical device comprising an expandable member that comprises an aqueous buffered solution and a solid and nonbiodegradable polymeric material having a Young's modulus of at least about 1OkPa or at least about 100 kPa or at least about 1 MPa or at least about lOMPa and a swellability of less than about, e.g., 20% v/v.
- An aqueous buffered solution or components of such a solution may be dispersed through the material or partially partitioned from the material.
- Figure IA depicts a polymer precursor with two functional groups.
- Figure IB depicts two types of polymer precursors with chemically distinct backbones and similar functional groups.
- Figure 1C depicts a polymer precursor with two types of functional groups.
- Figure ID depicts a multi -armed polymer precursor with four functional groups.
- Figure IE depicts two polymer precursors of different molecular weights.
- Figure 1 F depicts a multi-armed polymer precursor with two types of functional groups.
- Figure IG depicts two polymer precursors with two types of functional groups.
- Figure 2 depicts a polymer precursor with a polyethylene glycol backbone and acrylate functional groups.
- Figure 3 depicts a polymer precursor with a polyethylene glycol backbone and methacrylate functional groups.
- Figure 4 depicts a polymer precursor with methacrylate functional groups.
- Figure 5 depicts a polymer precursor with a polypropylene backbone and methacrylate functional groups.
- One ⁇ embodiment of the invention is a system for forming polymeric materials in situ within an implantable medical device. As explained above, some implants can be stabilized in the body by introducing an implant with an expandable member that can be inflated with polymer precursors that form a solid material.
- the polymer precursors and resultant solid material may be chosen in light of a variety of considerations, including solubility in aqueous solution, viscosity, reaction time, heat of polymerization, shelf life, pot life, bonding to the medical device, and mechanical properties after polymerization such as tensile strength, low-swellability, compressive strength, stiffness, elasticity, brittleness, stability, and durability.
- Functional groups on the precursors may be chosen to address these and other design considerations.
- Other components of the system may be chosen to adjust these characteristics or to provide additional control over other pertinent factors, e.g., pH, durability, radiopacity, bonding to plastic, bonding to metal, and biocompatibility.
- an endograft comprising a thin, double- walled balloon can be placed across the AAA with an inner lumen of the endograft providing for blood flow through the endograft.
- the balloon is filled in-situ with flowable polymeric precursors that polymerize and harden into a solid material.
- the hardened material is conformed to the specific shape of the patient's aneurysm and provides stability, a leakproof seal, and prevents migration of the endograft.
- the polymer precursor is a polymer that has reactive functional groups that form covalent bonds with particular functional groups on other polymer precursors to thereby form a polymeric material.
- the polymer precursor may be any polymer or a synthetic polymer. Synthetic is a term that refers to molecules not naturally produced by a human cell and excludes, for example, collagen regardless of how it is made or how it is chemically modified. Some polymer precursors may be essentially synthetic meaning that they are at least about 90% by molecular weight synthetic with the balance of the precursor being chemical groups with a biological motif, e.g., a sequence of amino acids degradable by particular enzymes. Polymer precursors may be selected to be free of amino acids, or peptide bonds, or saccharide units, or polysaccharides.
- Polymer precursors may comprise a variety of polymeric groups. Some precursors are water soluble, meaning that the precursors are soluble in aqueous solution at a concentration of at least about 1 gram per liter. Some precursors comprise polyethylene oxide (PEO, -(CH 2 CH 2 O) n -), which is useful to impart water solubility and desirable viscosity in solution and mechanical properties when formed into a polymeric material. Some polymer precursors comprise, e.g., about 100 to about 500,000 MW of PEO; the ordinary artisan will understand that all values and subranges within these explicitly articulated values are included, e.g., about 600 Daltons, about 15,000 Daltons, about 500 to about 100,000 Daltons, about 5,000 to about 50,000 Daltons.
- PEO polyethylene oxide
- Some precursors include comparable amounts of polymers related to PEO, e.g., polypropylene oxide (PPO, - CH 2 (GHy 2 O) n -), other polyalkylene oxide, or a copolymer of PEO-PPO, e.g., about 100 to about 250,000 Daltons.
- PEO polypropylene oxide
- - CH 2 (GHy 2 O) n - other polyalkylene oxide
- a copolymer of PEO-PPO e.g., about 100 to about 250,000 Daltons.
- Water-soluble precursors may also be formed directly from, or after derivitization of, other polymers, e.g., poly(acrylic acid), polyvinyl alcohol), polyvinyl chloride, polyacrlonitrile, polyallyamine, polyacrylates, polyurethanes, polycarbomethylsilane, polydimethylsiloxane, polyvinylcaprolactam, polyvinylpyrrolidone, or a combination of these.
- a nonwater soluble polymer may be decorated with water soluble groups to enhance its water solubility to make a water soluble polymer precursor, e.g., by adding carboxyls, hydroxyls, or polyethylene glycols.
- water soluble monomers examples include 2(2- ethoxyethoxy) ethyl acrylate, ethoxylated (15) trimethylolpropane triacrylate, ethoxylated (30) bisphenol a diacrylate, ethoxylated (30) bisphenol a dimethacrylate, ethoxylated(20) trimethylolpropane triacrylate, metallic diacrylate, methoxy polyethylene glycol (350) monoacrylate, methoxy polyethylene glycol (350) monomethacrylate, methoxy polyethylene glycol (550) monoacrylate, methoxy polyethylene glycol (550) monomethacrylate, polyethylene glycol (200) diacrylate, polyethylene glycol (400) diacrylate, polyethylene glycol (400) dimethacrylate, polyethylene glycol (600) diacrylate, polyethylene glycol (600) dimethacrylate, and polypropylene glycol monomethacrylate.
- Polymer precursors may be linear or be branched.
- the precursor may have 3 or more termini, e.g., at least 3, or about 3 to about 12, artisans will immediately appreciate that all ranges and values within the explicitly stated ranges are disclosed.
- a variety of techniques and sources for obtaining multi-armed precursors and attaching functional groups to them are known, e.g., as in the Aldrich catalog or Nektar or Shearwater Polymers or from Sartomer, Inc. catalogs, as well as in the literature for these arts.
- Some embodiments include two or more precursors with distinct average molecular weights or two or more types of precursors. Different types of precursors have distinct chemical formulae. A single type of polymer may be incorporated into two polymeric precursors having two distinct average molecular weights. Molecular weight averages for a solution of precursors may be determined as is customary in these arts, e.g., by weight or number averaging. Accordingly, a molecular weight for a precursor represents an average molecular weight for a plurality of precursors.
- a precursor's functional groups may be, for example, polymerizable or reactive by electrophile-nucleophile combination.
- the groups may be reactive with identical groups, e.g., as in free radical polymerization of acrylates, or with complementary groups, e.g., as in electrophilic-nucleophilic reactions.
- Polymerizable groups include, e.g., ethylenically unsaturated groups, groups polymerizable by free-radical chemistry, condensation chemistry, or addition chemistry.
- Examples of functional groups are: acrylates, methacrylates, butyl acrylate, methyl methacrylate, butyl methacrylate, hydroxyethyl methacrylate, polypropylene glycol diglycidal ether, polyethylene glycol diglycidyl ether, N-acryloxysuccinimide, glycidyl methacrylate, and hexamethylene diisocyanate.
- Examples of electrophilic or nucleophilic functional groups include succinimide esters, maleic acids, isocyanates, maleic acids, carbodiimides, aldehydes, azos, diazos, thiocyanates, carboxyls, amines, thiols, and hydroxyls.
- the functional groups on a precursor may be the same or of different types, with each type of functional group being a chemically distinct group. Different types of precursors may have the same or different types of functional groups, provided that the precursors react to form a polymeric material.
- acrylates may advantageously be used because acrylates are generally water soluble but do not react with water.
- a polyurethane precursor will react with water.
- acrylamide monomers are generally toxic, while water soluble acrylates have a low toxicity and are more acceptable for biomedical applications involving implantation.
- Figure IA depicts a polymer precursor with two functional groups that have the same chemical formula, with the functional groups being reactable to form a solid material, e.g., by free radical polymerization.
- Figure IB shows two types of polymer precursors with chemically distinct backbones that both have the same type of functional group, with the two precursors being reactable with each other to form a solid material.
- Figure 1C depicts a set of polymer precursors with different functional groups that can react to form a solid material, e.g., by free radial polymerization or electrophilic- nucleophilic reaction.
- Figure ID depicts an exemplary polymer precursor having a PEG backbone and acrylate functional groups.
- Figure 3 depicts an exemplary polymer precursor having a PEG backbone and methacrylate functional groups.
- Figure 4 depicts an exemplary polymer precursor having methacrylate functional groups reacted with a diglycol.
- Figure 5 depicts an exemplary polymer precursor having a polypropylene backbone and methacrylate functional groups
- Some embodiments employ combinations of polymer precursors with large variations in molecular weight.
- a small precursor can be relatively more mobile than an end of a larger precursor so that fewer living chains are terminated without reaction.
- a small precursor can be used to control physical properties of a material generated from the larger precursor, e.g., to adjust stiffness or other properties controlled by the number and distance between chain crosslinks.
- a lower molecular weight precursor can enhance the stiffness of a polymeric material by providing shorter distances between crosslinks.
- some embodiments include a first precursor with a molecular weight of about 30,000 to about 300,000 and a second precursor with a molecular weight between about 100 and about 3,000.
- a precursor with a molecular weight that is about 10 to about 100 times less than the molecular weight of a second precursor or, alternatively, less than the molecular weight of all the other precursors in the system.
- a first precursor having free radical polymerizable functional groups can be mixed with a relatively lower molecular weight precursor having free radical polymerizable functional groups.
- polymeric precursors When polymeric precursors are reacted, they form polymer segments in the polymeric material.
- a 30,000 MW bifunctional polymer precursor can form a polymer segment of 30,000 MW in the material.
- the time required for polymer precursors to react may be controlled by the choice of functional groups, precursor size, pH, initiator, catalyst, or accelerants. In general, a time of between about 30 seconds to about 30 minutes for polymerization is desired so that the precursor solution or solutions may be introduced into the medical device without undue increases in viscosity and without unduly extending the procedure time required for the precursors to form a firm material that permits users to close the patient.
- the time to polymerization may be measured outside a patient by observing the time from activation of precursors in a solution or suspension until the solution or suspension is no longer flowable.
- Activation of the precursors refers to the event that triggers their reaction with each other, e.g., initiating a free radical polymerization or mixing electrophilic and nucleophilic groups at a reactive pH.
- Bonding of the polymeric material to the device may be controlled by selecting precursor functional groups and/or precursors to bond the expandable member, or members that receive the precursors or mixed precursors. Bonding to plastic and metal may be enhanced by using suitable functional groups, e.g., sodium acrylates or other metallic acrylates.
- the material formed upon reaction of polymer precursors should have adequate mechanical properties to keep the device stable within the patient. Thus materials that are stiff enough to resist deformation caused by forces applied to the device after implantation are advantageous.
- Embodiments include materials with a Young's modulus of at least about 500 kPa, or 1000 kPa, or in a range of about 500 kPa to about 5O 5 OOO kPa; artisans will immediately appreciate that other values may be suitable and that all values and ranges within the explicitly articulated ranges are disclosed. Modulus is measured as follows: Cylindrical shaped samples of the crosslinked polymer are created by injecting the polymeric mixture into a silicone tubing of a known inner diameter.
- Certain embodiments are non-hydrogels. Certain embodiments are polymers formed from the precursors and functional groups set forth herein, as well as combinations thereof, e.g., polyacrylates, polymethacrylates, and polymethylmethacrylates. Materials that have a high ultimate stress and strain and which still have a modulus above about 100 kPa) are preferred. Materials that do not show substantial hydration upon being placed in an aqueous environment and also do not exhibit substantial degradation in physical properties over time are preferred.
- the material formed upon reaction of polymer precursors should have adequate durability to keep the device stable within the patient over time. Some embodiments of the material effectively maintain their mechanical properties over a period of at least 5, 10, 15, 20, or 30 years. Some embodiments of the polymeric material are essentially not biodegradable in an animal body, i.e. are not subject to effective hydrolytic and/or enzymatic degradation that leads to a loss of mechanical strength in an animal body in a typical tissue, i.e., as measurable by implantation subcutaneously, intramuscularly, or intravascularly in an animal model such as a rat or a rabbit. Examples of nonbiodedgrabale polymeric materials are polyacrylates, polymethacrylates, and polymethylmethacrylates. Examples of biodegradable materials are fibrin glue, hyaluronic acid, collagen, polylactic acid, and many polyesters.
- the polymeric material may be designed to have limited swellability in aqueous solution.
- a limited degree of swelling advantageously prevents the polymeric material from applying pressure to its surroundings after formation, even if water is present.
- limited intake of water through swelling can help to keep the material immobile in the patient.
- Certain embodiments of the polymeric materials have a swelling in aqueous solution of less than 20% v/v, 10% v/v, 5% v/v, or l%v/v, as measured by exposing the polymeric material to a 300-330 milliOsmolar, pH 7.4 buffered water solution after the polymeric material essentially reaches its full compressive strength and observing its change in weight after it has been allowed to swell in an unconstrained state for 24 hours, with the volume swelling being calculated from the change in weight.
- Viscosity of solutions of the polymer precursors can be controlled by adjusting factors such as the type of polymer, the polymer concentration, solubility of the polymer, and the polymer's molecular weight.
- the viscosity of a precursor solution should be low enough to allow the solution to be forced down a tube, e.g., a hollow tube guidewire, that allows inflation of an endograft using medically safe pressures.
- Some medical devices use such tubes to inflate balloons on endoscopic devices, e.g., for angioplasty or temporary occlusion of a blood vessel.
- viscosities of less than about 500 centipoise, less than about 100 centipoise, or less than about 10 centipoise, are preferable.
- the viscosity may be adjusted for use in conventionally-sized tubes, with conventional operating pressures of less than about 25 atmospheres.
- Some embodiments of the precursors are chosen with functional groups that are reactable at an approximately physiological pH and/or osmolality. These characteristics are useful, for instance, for employing physiological buffers to solubilize the precursors, push the precursors into place, or to flush a portion of the device with precursors or polymeric material in place.
- buffers for one or more of the solutions may be chosen to have a first pH before mixing and a second pH after mixing.
- a first precursor solution may have a low pH in a low buffering strength buffer to minimize reaction of the precursors and a second solution with a relatively higher buffering strength may be mixed with the first solution to achieve a second pH that is favorable for reaction of the precursors.
- ester linkages are observed to be more stable at somewhat acidic pH (e.g., about pH 4) and so a particular pH may be selected for certain components for reasons of stability.
- a physiological pH of e.g., about 7 to about 8
- a different pH may be chosen, e.g., from about 4 to about 9.
- Radio-opaque components may be introduced with polymeric precursors to allow visualization of the polymeric material after it is formed.
- radio-opaque materials are PANTOP AQUE, barium sulfate, tantalum powder, (all water insoluble), ISOVUE, OXILAN, iodapamide, omnipaque, metrizamide, iopentol, iohexol, iophenoxic acid, ioversol, gadodiamide, and sodium tyropanoate.
- Components may be introduced to enhance imaging, for example, according to X-ray, magnetic resonance imaging, and tomography, e.g., spiral computer tomography techniques.
- Some embodiments of the functional groups are free radical polymerizable groups that may advantageously be exposed to initiators and/or catalysts to, for example, enhance reaction kinetics or mechanical properties of the polymeric material.
- Initiators are required to start polymerization in many systems, and include, for example, thermal, chemical, and light-activated initiators. Initiators may be used to activate the polymer precursors to polymerize and form the polymeric material. Initiator concentration can affect variables such as polymerization time, temperature, and mechanical properties of the polymeric material.
- metal ions may be used either as an oxidizer or a reducer.
- certain metal ions may be used in combination with a peroxide or hydroperoxide to initiate polymerization.
- Some suitable metal ions have at least two states separated by only one difference in charge, e.g., ferric/ferrous; cupric/cuprous; ceric/cerous; cobaltic/cobaltous; vanadate V vs. IV; permanganate; and manganic/manganous.
- Peroxygen containing compounds such as peroxides and hydroperoxides, including hydrogen peroxide, t-butyl hydroperoxide, t- butyl peroxide, benzoyl peroxide, cumyl peroxide, may also be used.
- Thermal initiating systems may also be used, for example, commercially available low temperature free radical initiators that initiate tree radical crosslmking reactions at or near physiological body temperatures. Some examples are sodium persulfate (50° C), ammonium persulfate (50° C), glucose oxidase-glucose-ferrous sulfate (initiated around 37° C in presence of dissolved oxygen).
- Photoinitiators are also known for initiation of polymerization, e.g., DAROCUR 2959 (initiated around 360 nm), IRGACURE 651 (initiated around 360 ran), eosin- triethanol amine (initiated around 510 nm), methylene blue-triethanol amine (initiated around 632 nm), and the like.
- Catalysts, co-catalysts, and chain extenders may be used to further control reaction of the polymer precursors or to extend shelf life.
- small amounts of vinyl pyrrolidinone e.g., around 1-10 ⁇ l per ml
- Inhibitors such as hydroquinone may be added to prevent premature polymerization of polymer precursors during storage.
- Tetramethylethylenediamine (TEMED) is a catalyst useful in many polymerizations, e.g., in an ammonium persulfate/TEMED or riboflavin/TEMED catalyzed reaction.
- Some initiators can be chosen that require little or no oxygen, e.g., riboflavin-based initiator systems. Systems that are not substantially inhibited by the presence of oxygen and that can enable the reaction to proceed at physiological temperature may be chosen.
- aqueous solution facilitates preparation of a solution with a controlled viscosity by including water.
- an aqueous solution as opposed to, e.g., an organic solvent, provides safety benefits in case some amount of the solution should be exposed to the patient or user.
- the presence of water also serves to reduce the mass of polymerizable precursors used, and thus improves the toxicological profile of the precursors, should they be accidentally discharged into the body.
- an aqueous solvent for the precursors is avoids potential compatibility problems with materials used in the expandable device, such as degradation of the material or potentially unwanted changes to its mechanical properties, e.g., softening by partial salvation.
- aqueous solutions do not solvate biomaterials used for an expandable member of a medical device.
- the aqueous solvent may be interspersed through the polymeric material, e.g., in pore spaces, or some portion of the solvent may be partitioned away from the material.
- the solvent may be buffered with a buffering agent or agents to control pH of the solution.
- the amount of aqueous solvent to mix with the other components of the system may be adjusted to achieve a desired viscosity in light of the properties of the hardened material.
- Some embodiments include between about 0.5 parts to about 10 parts by weight of polymeric precursor compared to the weight of the aqueous solvent; artisans in this field will immediately appreciate that all ranges and values within this range are disclosed.
- the polymer precursors may be used to fill an expansion member of an implantable medical device.
- the medical device may be, for example, suited for minimally invasive surgery (MIS) techniques, e.g., guidable through vasculature of a human patient using a guidewire introduced into the patient for that purpose.
- MIS devices having an inflatable or expandable member or are provided in, for example, PCT Application Pub. No. WO 00/51522, U.S. Pat. Nos. 5,334,024, 5,330,528, 6,312,462, 6,964,667, 7,001,431, in U.S. Pat. Pub. No. 2004/0204755 published October 14 2004, and U.S. Patent Serial No. US2006/0025853A1 filed on July 22, 2005 ⁇ which are hereby incorporated by reference herein to the extent that they do not contradict what is explicitly disclosed herein.
- An expandable member undergoes an increase in volume resulting from introduction of a flowable material into the member.
- An expandable member may be, for example, a balloon, a double-walled balloon, or an inflatable cuff.
- the expandable member may include either compliant materials, or non-compliant materials, or both.
- a non-compliant material generally resists deformation under physiological conditions, e.g., parylene, polytetrafluoroethylene, or polyethylene terephthalate. Examples of compliant materials are silicones, latexes, and elastic materials in general.
- a noncompliant material may be used in an expandable member by introducing the material in a shape that allows for subsequent expansion; for example, a noncompliant material be coiled or folded for delivery and expanded by uncoiling or unfolding, e.g., as a result of filling the member with a flowable precursor.
- a balloon used for placement of an implantable medical device may be a sealed, flexible, expandable member that is elastic. Balloons may take a wide variety of shapes, e.g., including spherical, ellipsoidal, tubular, cylindrical (filled between double walls with a lumen interior to the cylinder). Expandable members may include a combination of compliant materials and noncompliant materials, e.g., a noncompliant portion adjoined to a complaint portion.
- polymer precursors in a flowable form may be delivered to an expandable member wherein they are solidified into a polymeric material.
- the flowable precursors may be introduced into the expansion member to expand a flexible material to increase a volume of the member, which may be sealed after it is expanded.
- the material within the member is may be referred to as being within the patient even though the material does not directly contact a patient's tissue. Expansion of the member may force the member against a tissue of the patient to seat the device in the tissue. Hardening of the precursors into a solid material further secures the device.
- the precursor or precursors may be activated before, during, or after introduction into the expansion member.
- Activation beforehand may be accomplished by mixing a polymeric precursor with an activating agent that causes precursors to form covalent bonds, for example, as an initiator that initiates polymerization, a buffer that changes a pH of a precursor-and-initiator solution to activate the initiator, or external energy in the form of heat or light may be applied to activate a thermal or photoinitiator.
- an activating agent that causes precursors to form covalent bonds
- a buffer that changes a pH of a precursor-and-initiator solution to activate the initiator, or external energy in the form of heat or light
- electrophilic-nucleophilic reactions may be activated by mixing a precursor with electrophilic functional groups with a precursor having nucleophilic functional groups, or by using a buffer to change the pH of a premixed combination of precursors with electrophilic and nucleophilic functional groups.
- two solutions are mixed with each other ex vivo and introduced using MIS techniques into an expandable member.
- the mixture is pumped through a filling tube into the expandable member until a desired pressure is achieved, and the tubes for filling the member are withdrawn, leaving the expandable member inflated with the mixture, which is sealed entirely within the member and hardens into a solid material, e.g., a polymeric material, with the time to polymerization being greater than the amount of time required to fill the member and withdraw the filling tube.
- An example of this method is combining a first container having a polymerizable first precursor with a solution having an initiator that initiates polymerization.
- various types and sizes of precursors may be used in combination with various types of initiators. For instance, two solutions with different types and/or molecular weights of precursors may be used.
- two solutions are prepared that are separately introduced via separate filling tubes for combination within the patient, e.g., mixing for the first time in the expandable member or in a manifold disposed in the introductory device.
- a kit may be prepared with a first precursor container having about 10 grams of a 35,000 MW PEG polymeric precursor terminated with a diacrylate functional group at each of two ends.
- the first precursor container may contain a radio- opaque agent, e.g., about 10 grams sodium diatrizoate, and an initiator, e.g., about 1.8 grams of a persulfate.
- a first diluent container has about 230 ml of phosphate buffered solution at physiological pH (e.g., 7.4) and physiological osmolality, or an osmolality and buffering strength that achieves physiological pH and osmolality after combination with other components.
- a second precursor container has about 150 ml of essentially pure 600 MW PEG polymeric precursor terminated with a diacrylate functional group at each of two ends, and further comprises 100 ml of phosphate buffered solution pH 4 and a catalyst, e.g., about 1.8 ml of TEMED.
- a user mixes the first diluent container with the first precursor container to form a first precursor solution that is mixed with the contents of the second precursor container and used to fill an expandable member.
- the precursors form a hard firm crosslinked material in approximately 2-3 minutes. The material is visible on x-ray fluoroscopy due to the sodium Diatrizoate.
- the system may be controlled to produce faster or shorter polymerization time, e.g., from about 30 seconds to about 30 minutes for either or both.
- polymerization time e.g., from about 30 seconds to about 30 minutes for either or both.
- about 1.2g of persulfate and 1.2 ml of TEMED would provide approximately a 5-6 min polymerization time.
- about 0.6g of persulfate and about 0.6 ml of TEMED in the same formulation would result in a polymerization time of about 20 minutes.
- Certain other embodiments involve using a filler material mixed with polymeric precursor(s) to form a polymeric material that includes a filler.
- a filler can be used to adjust the properties of the polymeric material, for example, the stiffness, mechanical strength, compressibility, or density.
- fillers include solid objects, e.g., beads, cylinders, microbeads, hollow materials, e.g., hollow microspheres, fibers, e.g., polylactic acid fibers, and meshes, e.g., nylon meshes.
- Such fillers may be mixed with one or both of the precursors before introduction into an implant, or the fillers may be admixed in situ.
- the precursor solutions may be used as a continuous suspending medium to hold the filler in place.
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Abstract
Description
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Priority Applications (6)
Application Number | Priority Date | Filing Date | Title |
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ES07795435T ES2906420T3 (en) | 2006-05-30 | 2007-05-29 | Formable materials in situ within a medical device |
CA002652966A CA2652966A1 (en) | 2006-05-30 | 2007-05-29 | Materials formable in situ within a medical device |
AU2007255053A AU2007255053A1 (en) | 2006-05-30 | 2007-05-29 | Materials formable in situ within a medical device |
EP07795435.2A EP2029217B1 (en) | 2006-05-30 | 2007-05-29 | Materials formable in situ within a medical device |
JP2009513234A JP2009538695A (en) | 2006-05-30 | 2007-05-29 | Materials that can be molded in situ in medical devices |
CN2007800275055A CN101489622B (en) | 2006-05-30 | 2007-05-29 | Materials formable in situ within a medical device |
Applications Claiming Priority (2)
Application Number | Priority Date | Filing Date | Title |
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US11/443,504 US7872068B2 (en) | 2006-05-30 | 2006-05-30 | Materials formable in situ within a medical device |
US11/443,504 | 2006-05-30 |
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WO2007142916A2 true WO2007142916A2 (en) | 2007-12-13 |
WO2007142916A3 WO2007142916A3 (en) | 2008-11-27 |
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PCT/US2007/012639 WO2007142916A2 (en) | 2006-05-30 | 2007-05-29 | Materials formable in situ within a medical device |
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US (2) | US7872068B2 (en) |
EP (1) | EP2029217B1 (en) |
JP (2) | JP2009538695A (en) |
CN (1) | CN101489622B (en) |
AU (1) | AU2007255053A1 (en) |
CA (1) | CA2652966A1 (en) |
ES (1) | ES2906420T3 (en) |
WO (1) | WO2007142916A2 (en) |
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Also Published As
Publication number | Publication date |
---|---|
WO2007142916A3 (en) | 2008-11-27 |
JP2014133156A (en) | 2014-07-24 |
JP5936641B2 (en) | 2016-06-22 |
US20110092613A1 (en) | 2011-04-21 |
EP2029217A4 (en) | 2012-09-26 |
AU2007255053A1 (en) | 2007-12-13 |
CN101489622A (en) | 2009-07-22 |
ES2906420T3 (en) | 2022-04-18 |
US7872068B2 (en) | 2011-01-18 |
JP2009538695A (en) | 2009-11-12 |
EP2029217B1 (en) | 2021-12-15 |
US8044137B2 (en) | 2011-10-25 |
US20070282366A1 (en) | 2007-12-06 |
CA2652966A1 (en) | 2007-12-13 |
CN101489622B (en) | 2013-04-24 |
EP2029217A2 (en) | 2009-03-04 |
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