AU3642500A - Method of incorporating drugs into a polymer component of stents - Google Patents

Method of incorporating drugs into a polymer component of stents Download PDF

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AU3642500A
AU3642500A AU36425/00A AU3642500A AU3642500A AU 3642500 A AU3642500 A AU 3642500A AU 36425/00 A AU36425/00 A AU 36425/00A AU 3642500 A AU3642500 A AU 3642500A AU 3642500 A AU3642500 A AU 3642500A
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polymeric material
therapeutic drug
porosigen
drug
rate
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AU738034B2 (en
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Robert P Eury
Darlene Garguilo
Plaridel Villareal
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Abbott Cardiovascular Systems Inc
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Advanced Cardiovascular Systems Inc
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Description

AUSTRALIA
PATENTS ACT 1990 DIVISIONAL APPLICATION NAME OF APPLICANT: Advanced Cardiovascular Systems, Inc.
ADDRESS FOR SERVICE: DAVIES COLLISON CAVE Patent Attorneys 1 Little Collins Street Melbourne, 3000.
INVENTION TITLE: "Method of incorporating drugs into a polymer component of stents" The following statement is a full description of this invention, including the best method of performing it known to us: -la- BACKGROUND OF THE INVENTION Field of the Invention This invention relates generally to expandable intraluminal vascular grafts, generally referred to as stents and, more particularly, concerns stents coated with a polymer component capable of carrying and 5 releasing therapeutic drugs, and a method of S. incorporating therapeutic drugs into the polymer component of such stents.
Description of Related Art Systemic administration of some therapeutic pharmaceutical drugs, in order to provide an efficacious concentration of the drugs at a localized area of interest, can produce serious systemic side effects.
15 Local administration of a therapeutic drug can be significantly more effective and produce fewer side effects than systemic delivery, particularly for i anticoagulants used for preventing thrombosis of a coronary stent, and cytostatic agents applied for reducing post-angioplasty, proliferation of vascular tissue, which is a factor when restenosis occurs following an angioplasty procedure.
There thus has been a need in modern medicine for techniques for local delivery of therapeutic drugs.
In one technique, catheters have been used to deliver therapeutic drugs in a solution used to bathe the tissue for a short period of time, which is effective for administration of thrombolytic drugs, or to inject the drug solution into the tissue surrounding the area of interest. However, the therapeutic effect of drugs delivered by this method generally is relatively short, as the drugs commonly are eliminated easily from the delivery site.
Therapeutic drugs have been incorporated into relatively permanent structures for longer term delivery of the drugs at the site of interest. For example, extravascular wraps having a relatively large quantity of a drug in a bandage structure can be applied around the exterior of an artery. Although work in animals has shown that this technique is effective for local anticoagulation with heparin, it has limited practical *.S*utility in human beings, since an invasive operation is required to place the extravascular wrap at the site of interest.
15 In another technique, coatings of therapeutic drugs have been applied to stents in order to provide sustained delivery of the drugs at the site of interest.
However, coatings thick enough to provide a therapeutically effective amount of the drug can severely compromise the function of the stent, and very thin coatings that do not impede the function of the stent, such as heparin coatings with a thickness of several microns, typically do not deliver a therapeutically effective amount of the drug.
25 It would be desirable to provide a method of incorporating a therapeutically effective amount of a therapeutic drug into an intravascular layer of polymeric material which can be applied to a relatively permanent intravascular device, such as a stent, that does not require an invasive operation for placement of the device, in a manner that would not interfere with the functioning of the stent. The present invention meets these needs.
P:\OPER\AXD48256-96.SPE 27/10/99 -3- SUMMARY OF THE INVENTION Briefly, and in general terms, the present invention provides for a polymeric material containing a therapeutic drug for application to a structure of an intravascular stent, and a method of incorporating a therapeutically effective amount of a therapeutic drug into a polymeric material for application to the structure of an intravascular stent, which when applied to the structure of the stent will not significantly increase the thickness of the stent, and thus will not interfere with the 10 function of the stent.
According to one aspect of the invention, there is provided a method of incorporating a therapeutically effective amount of a therapeutic drug into a polymeric material for application to an intravascular stent, the method comprising the steps of: forming solid particles of a therapeutic drug to have a maximum cross-sectional dimension of about 10 microns; and uniformly dispersing said solid particles of said therapeutic drug in said polymeric material such that said particles of said therapeutic drug form up to 70% by weight of the total weight of the therapeutic drug and the polymeric *...material; and uniformly dispersing a porosigen in said polymeric material together with said therapeutic drug.
According to another aspect of the invention, there is provided a polymeric material containing a therapeutic drug for application to an intravascular stent for carrying and delivering said therapeutic drug within a blood vessel in which said intravascular stent is placed, comprising: a polymeric material having a relatively low thermal processing temperature; particles of a therapeutic drug incorporated in said polymeric material; and a porosigen incorporated in said polymeric material.
P:\OPER\AXD48256-96.SPE 27/10199 3A Accordingly, the present invention provides for a polymeric material containing a therapeutic drug, for application to a thin reinforcement or structural member of the stent on at least one side, for carrying and releasing the therapeutic drug. The thin reinforcement provides the structural strength required for maintaining the patency of the vessel in which the stent is placed, and the polymer coating provides the stent with the capacity for carrying and releasing therapeutic drugs at the location of the stent of the vessel in which the stent is placed. The polymer coating can be formed to include pores or to contain a material which will dissolve or degrade to form pores in the polymeric material, can be multi-layered to permit "the combination of a plurality of different drug containing materials in a single stent, and can include a rate-controlling membrane to allow for controlled retention and delivery of selected drugs within the affected blood vessel upon implantation. Depending upon the construction and lamination of S" the stent, drugs can be released simultaneously or sequentially, on the exterior surface of the stent to a blood vessel wall, and directly into the bloodstream, as desired.
The present invention also provides for a method of incorporating a therapeutic drug into a polymeric material. In one preferred embodiment of the method of the invention, a layer of polymeric material is manufactured by combining the selected polymeric material with a relatively high loading of the therapeutic drug in a thermal process, such as coextrusion of the therapeutic drug with the polymeric material, for example, although other thermal processes such as molding or calendaring may also be suitable. The polymeric material preferably is selected to have a relatively low processing temperature, at which the drug of interest is thermally unstable. In another preferred embodiment of the method of the invention, particularly where the drug of interest :is thermally unstable and a low temperature processing polymer is not suitable, the layer of the selected 15 polymeric material can be formed by solvent casting or by coating the polymeric material with the selected therapeutic drug. In either a thermal process, such as coextrusion, or a low or ambient temperature process, *o..such as solvent casting, the therapeutic drug can be dispersed and incorporated into a polymer as small particles, preferably having a maximum cross-sectional dimension of about 10 microns.
These and other aspects and advantages of the invention will become apparent from the following detailed description, and the accompanying drawings, which illustrate by way of example aspects of the invention.
BRIEF DESCRIPTION OF THE DRAWINGS Fig. 1 is a cross-sectional view of an extrusion apparatus for use in combining a therapeutic drug with a polymer component of a stent according to the method of the invention; Fig. 2 is a diagrammatic view of a laminating apparatus that can be used for laminating the reinforcement member of the stent on one side with a drug-loaded polymeric film; and Fig. 3 is a diagrammatic view of a lamination apparatus that can be used for laminating the reinforcement member of the stent on two sides with a drug-loaded polymeric film.
DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS Local administration of therapeutic drugs to avoid the serious side effects that can result from systemic administration of some therapeutic drugs can result in limitation of the effective duration of the drug to a relatively short period of time, due to S. 15 elimination of the therapeutic drug from the delivery site. Administration of therapeutic drugs to a blood vessel by a relatively permanent intravascular device to *provide a longer effective duration of localized drug *therapy also poses the problem of providing a therapeutically effective amount of the drug without substantially increasing the thickness of the device, *which increased thickness could injure or block the vessel when the device is deployed.
The invention accordingly is embodied in a 25 polymeric material containing a therapeutically effective amount of a therapeutic drug that can be combined with the reinforcement structure of an intravascular stent, and a method of incorporating the therapeutic drug into the polymeric material and forming the polymeric material as a thin layer containing a therapeutically effective amount of the therapeutic drug, to be incorporated in the stent without significantly increasing the thickness of the stent.
As is illustrated in the drawings, in one preferred embodiment, a selected therapeutic drug is preferably intimately mixed with the selected polymeric material so as to uniformly disperse the therapeutic drug P:\OPER\AXD\48256-96.SPE -27/10/99 -6in the polymeric material. The specific method of uniformly dispersing the therapeutic drug in the polymer can vary, and depends upon the stability of the therapeutic drug to thermal processing. However, in a preferred embodiment, the therapeutic drug is uniformly dispersed in the polymeric material by coextruding small solid particles of the selected therapeutic drug with the selected polymeric material, as is illustrated in Fig. 1. Such an extrusion apparatus 10 typically includes a hopper into which the polymeric material and small particles of the selected therapeutic drug are added together, and into which a porosigen can also be added. The extruder also typically includes a lead screw 14 that drives and intimately mixes the *e ingredients together, to uniformly disperse the small particles of the therapeutic drug and a porosigen in the polymeric material. The barrel 16 of the extruder preferably is heated by temperature controlled heaters 18 surrounding the barrel in stages. A motor 20 and associated gears are provided to drive the lead screw, and a cooling system 22 also is typically provided. This method of intimately mixing the therapeutic drug **.and polymeric material can yield a relatively high and uniformly distributed loading of the therapeutic drug in the polymer.
.::While a currently preferred loading of the therapeutic drug is no more than about 40% by weight, drug loadings as high as by weight depending upon the specific application and interaction of the polymer with the drug, have been achieved by this method. The drug-loaded polymer can be extruded into an appropriate shape, or subsequently can be calendared to produce a drug-loaded polymer film having a smooth surface, with the therapeutic drug uniformly distributed in the film.
The selected therapeutic drug can, for example, be anticoagulant, antiplatelet or antithrombin agents such as heparin, D-phe-pro-arg-chloromethylketone -7- (synthetic antithrombin), dipyridamole, hirudin, recombinant hirudin, thrombin inhibitor (available from the Biogen Company), or c7E3 (an antiplatelet drug from the Centocore Company); cytostatic or antiproliferative agents such as angiopeptin (a somatostatin analogue from the Ibsen Company), angiotensin-converting enzyme inhibitors such as Captopril (available from the Squibb Company), Cilazapril (available from the Hoffman-LaRoche Company), or Lisinopril (available from the Merck Company) calcium channel blockers (such as Nifedipine), colchicine, fibroblast growth factor (FGF) antagonists, fish oil (omega 3-fatty acid), low molecular weight S. heparin (available from the Wyeth and Glycomed Companies), histamine antagonists, Lovastatin (an 15 inhibitor of HMG-CoA reductase, a cholesterol lowering drug from the Merck Company), methotrexate, monoclonal antibodies (such as to PDGF receptors), nitroprusside, phosphodiesterase inhibitors, prostacyclin and prostacyclin analogues, prostaglandin inhibitor (available from the Glaxo Company), Seramin (a PDGF antagonist), serotonin blockers, steroids, thioprotease inhibitors, and triazolopyrimidine (a PDGF antagonist) Other therapeutic drugs which may be appropriate include alpha-interferon and genetically engineered epithelial 25 cells, for example.
The particles of the desired therapeutic drug preferably are formed by air milling of crystals of the therapeutic drug to form microgranules of the therapeutic drug. This method is preferred because it typically produces no heat and generally does not lead to contamination of the therapeutic drug. The particles of the desired therapeutic drug can also be formed by recrystallization, ball milling or grinding, as long as generation of heat and possible contamination are closely controlled.
The particles of the desired therapeutic drug preferably are formed to have a maximum cross-sectional dimension of about 10 microns. An average particle size of less than 10 microns, and a uniform distribution of the particles of the therapeutic drug in the polymeric material, are critical to provision of a therapeutically effective amount of the therapeutic drug in the layer of polymeric material to be applied to the structure of the stent, because the layer of polymeric material typically can be as thin as 25 microns. The size and distribution of the particles of the therapeutic drug also can affect the physical properties of the polymer.
In a preferred aspect of the method of the invention, the polymeric material in which the therapeutic drug is incorporated has a relatively low processing temperature, such as polycaprolactone, having 15 a processing temperature of approximately 80 0
C,
poly(ethylene-co-vinyl acetate) or poly(vinyl acetate), having processing temperatures of approximately 100 0 C, or silicone gum rubber, having a processing temperature of about 40 0 C, for example. Other polymers having similar relatively low processing temperatures also may be suitable. Other polymers which may be suitable include non-degradable polymers capable of carrying and delivering therapeutic drugs, and biodegradable, bioabsorbable polymers capable of carrying and delivering 25 therapeutic drugs, such as poly-DL-lactic acid (DL-PLA), and poly-L-lactic acid (L-PLA), polyorthoesters, polyiminocarbonates, aliphatic polycarbonates, and polyphosphazenes.
Alternatively, the therapeutic drug can be compounded with the polymer by calendaring the ingredients, such as in a two-roll mill, for example.
This method also can yield a relatively high and uniformly distributed loading of the therapeutic drug in the polymer.
A porosigen also can be incorporated in the drug-loaded polymer by adding the porosigen to the polymer along with the therapeutic drug to form a porous, drug-loaded polymeric membrane. A porosigen is defined herein for purposes of this application as any moiety, such as microgranules of sodium chloride, lactose, or sodium heparin, for example, which will dissolve or otherwise will be degraded when immersed in body fluids to leave behind a porous network in the polymeric material. The pores left by such porosigens typically can be a large as 10 microns. The pores formed by porosigens such as polyethylene glycol (PEG), polyethylene oxide/polypropylene oxide (PEO/PPO) copolymers, for example, also can be smaller than one micron, although other similar materials which form phase separations from the continuous drug-loaded polymeric matrix and can later be leached out by body fluids also S 15 can be suitable for forming pores smaller than one micron. While currently it is preferred to apply the polymeric material to the structure of a stent during the time that the therapeutic drug and porosigen material are 'contained within the polymeric material, to allow the porosigen to be dissolved or degraded by body fluids when the stent is placed in a blood vessel, alternatively the porosigen can be dissolved and removed from the polymeric material to form pores in the polymeric material prior to placement of the polymeric material combined with the 25 stent within a blood vessel.
If desired, a rate-controlling membrane also can be applied over the drug-loaded polymer, to limit the release rate of the therapeutic drug. Such a ratecontrolling membrane can be useful for delivery of water soluble substances as to which a nonporous polymer film would completely prevent diffusion of the drug. The rate-controlling membrane can be added by applying a coating from a solution, or a lamination, as described previously. The rate-controlling membrane applied over the polymeric material can be formed to include a uniform dispersion of a porosigen in the rate-controlling membrane, and the porosigen in the rate-controlling membrane can be dissolved to leave pores in the ratecontrolling membrane typically as large as 10 microns, or as small as 1 micron, for example, although the pores also can be smaller than 1 micron. The porosigen in the rate-controlling membrane can be, for example, sodium chloride, lactose, sodium heparin, polyethylene glycol, polyethylene oxide/polypropylene oxide copolymers, and mixtures thereof.
The drug-loaded polymer can be laminated to the surface of a stent. The inner reinforcement structure to which the drug-loaded polymer is laminated preferably is formed from a thin sheet of metal, such as stainless :steel, although other metals such as platinum-iridium alloy, molybdenum-rhenium alloy, tantalum, gold, combinations thereof and other similar materials also may be suitable. The inner metal reinforcement structure of the stent preferably is laminated with polymer films on each side, with at least one coating of a polymer film.
Alternatively, the reinforcement structure also can be coated on one side, if desired. At least one laminating polymeric film capable of absorbing and releasing therapeutic drugs is placed on at least one side of the reinforcement member of the stent, and the laminating polymeric film is heated to its appropriate processing 25 temperature to bond the laminating polymeric film to the surface of the inner stent member to form a laminated stent member.
When the structural reinforcement member 30 of the stent is to be laminated on one side only, the reinforcement member and polymer film can be bonded by a typical two-ply fusion lamination system 32, as is illustrated in Fig. 2. The two-ply laminating stack typically includes an idler roll 34 receiving a sheet of the reinforcement members 30, and a lay-on roll 36 receiving the drug-loaded polymeric film 28. The reinforcement member 30 and drug-loaded polymeric film 28 are pressed into intimate contact between the lay-on roll -11and the heating and combining drum 38, and can be heated by the drum and take-off heat roll 40, where the reinforcement member and drug-loaded film laminate can be utilized for further processing in making the drug-loaded stent.
When the reinforcement member is to be laminated on both sides, the reinforcement member 30 and drug-loaded polymeric film layers 28, 29 can be bonded together by typical three-ply fusion lamination rolls, as is illustrated in Fig. 3. Such a three-ply fusion lamination system 42 typically can include a first preheat roll system 44 for receiving and preheating one drug-loaded polymeric film 28, a second preheat roll system 46 for receiving and preheating the sheet of 15 reinforcement members 30, and a lay-on roll 48 for 9go• pressing the reinforcement member and first drug-loaded polymeric laminating film together in intimate contact against the heating-and-combining drum 50. A third preheat roll system 52 can be provided for receiving and preheating the second drug-loaded polymeric laminating film 29, and a lay-on roll 54 presses the second drugloaded polymeric laminating film and reinforcement member together in intimate contact against the drum. The reinforcement member and two layers of laminating film 25 can be further heated by the drum and take-off heat roll 56, and removed for further processing in making the drug-loaded stent. Other laminating systems that combine the reinforcement member with one or more of the drugloaded polymeric laminating films also may be suitable.
Alternatively, the polymeric film can be applied by solvent casting, or by adhering the film to the surface of the inner stent member with a biocompatible adhesive.
Any excess polymer extending beyond the desired edges of orifices or the outside edges of the stent preferably is removed, typically by cutting with a laser (not shown), such as a continuous C02 laser, a pulsed yttrium aluminum garnet (YAG) laser, or an excimer laser, P:\OPER\AXD\48256-96.SPE 27/10/99 12for example, although the excess polymer also can be removed by stamping and the like.
It thus has been demonstrated that the invention provides for a polymeric material containing a therapeutically effective amount of a therapeutic drug that can be combined with a reinforcement structure of an intravascular stent, and a method of incorporating the therapeutic drug into the polymeric material for combination with the stent, and for forming the polymeric material as a thin layer containing a therapeutically effective amount of the therapeutic drug to be incorporated in the stent without significantly increasing the thickness of the stent.
Throughout this specification and the claims which follow, ooo* *unless the context requires otherwise, the word "comprise", and variations such as "comprises" and "comprising", will be understood to imply the inclusion of a stated integer or step or group of integers or steps but not the exclusion of any other soot •g00 integer or step or group of integers or steps.
It will be apparent fromr the foregoing that while particular forms of the invention have been illustrated and described, various modifications can be made without departing from the scope of the invention. Accordingly, it is not intended that the invention be limited, except as by the appended claims.

Claims (32)

  1. 2. The method of claim i, wherein said step of forming solid particles of said therapeutic drug comprises air milling crystals of said therapeutic drug. The method of claim i, wherein said step of forming solid particles of said therapeutic drug comprises recrystallizing crystals of said therapeutic drug.
  2. 4. The method of claim i, wherein said step of forming solid particles of said therapeutic drug comprises ball milling crystals of said therapeutic drug. The method of claim 1, wherein said step of forming solid particles of said therapeutic drug comprises grinding crystals of said therapeutic drug. -14-
  3. 6. The method of claim 1, wherein said therapeutic drug is selected from the group consisting of heparin, D-phe-pro-arg-chloromethylketone, dipyridamole, hirudin, recombinant hirudin, thrombin inhibitor, angiopeptin, angiotensin converting enzyme inhibitors, calcium channel blockers, colchicine, fibroblast growth factor antagonists, fish oil, omega 3-fatty acid, low molecular weight heparin, histamine antagonists, inhibitors of HMG-CoA reductase, methotrexate, monoclonal 10 antibodies, nitroprusside, phosphodiesterase inhibitors, prostacyclin and prostacyclin analogues, prostaglandin inhibitor, PDGF antagonists, serotonin blockers, steroids, thioprotease inhibitors, triazolopyrimidine, alpha-interferon, and genetically engineered epithelial cells, and mixtures thereof.
  4. 7. The method of claim 1, wherein said polymeric material has a relatively low thermal processing temperature. e*
  5. 8. The method of claim 1, wherein said polymeric material has a thermal processing temperature of not more than approximately 100 0 C.
  6. 9. The method of claim 1, wherein said polymeric material is selected from the group consisting of polycaprolactone, poly(ethylene-co-vinyl acetate), poly(vinyl acetate), silicone gum rubber, poly-DL-lactic acid (DL-PLA), poly-L-lactic acid (L-PLA), polyorthoesters, polyiminocarbonates, aliphatic polycarbonates, polyphosphazenes, and mixtures thereof. P:\OPER\AXD\48256-96.SPE 27/10199 15 The method of claim i, wherein said particles of said therapeutic drug comprise up to 40% by weight of the total weight of the therapeutic drug and the polymeric material.
  7. 11. The method of claim i, wherein said step of uniformly dispersing said solid particles of said therapeutic drug in said polymeric material comprises coextruding said particles of said therapeutic drug and said polymeric material.
  8. 12. The method of claim i, wherein said step of uniformly dispersing said solid particles of said therapeutic drug in said polymeric material comprises calendaring said particles of said therapeutic drug and said polymeric material together.
  9. 13. The method of claim 1, wherein said step of uniformly dispersing said solid particles of said therapeutic drug in said polymeric material comprises solvent casting said particles of said therapeutic drug together with said polymeric material.
  10. 14. The method of claim 1, wherein said step of uniformly dispersing a porosigen in said polymeric material together with said therapeutic drug comprises coextruding said porosigen together with said therapeutic drug and said polymeric material. The method of claim 14, further including the step of dissolving said porosigen in said polymeric material to leave pores in said polymeric material.
  11. 16. The method of claim 15, wherein said pores have a maximum cross-sectional dimension of about 10 microns.
  12. 17. The method of claim 15, wherein said pores have a maximum cross-sectional dimension of about one micron. P:\OPER\AXD\48256-96.SPE 27M1O99 16-
  13. 18. The method of claim 1, wherein said porosigen is selected from the group consisting of sodium chloride, lactose, sodium heparin, polyethylene glycol, polyethylene oxide/polypropylene oxide copolymers, and mixtures thereof.
  14. 19. The method of claim 1, further including the step of applying a rate-controlling membrane over said polymeric material to control the release rate of said therapeutic drug from said polymeric material.
  15. 20. The method of claim 19, wherein said step of applying a rate-controlling membrane over said polymeric material comprises forming said rate-controlling membrane to include a uniform dispersion of a porosigen in said rate-controlling membrane.
  16. 21. The method of claim 20, further including the step of dissolving said porosigen in said rate-controlling membrane to leave pores in said rate-controlling membrane. "22. The method of claim 20, wherein said porosigen in said rate-controlling membrane is selected from the group consisting of sodium chloride, lactose, sodium heparin, polyethylene glycol, polyethylene oxide/polypropylene oxide copolymers, and mixtures thereof.
  17. 23. The method of claim 1, further including tae step of forming said polymeric material containing said therapeutic drug as a sheet at least about 25 microns thick.
  18. 24. The method of claim 23, further including the step of laminating said sheet of polymeric material containing said therapeutic drug to an intravascular stent structure. P:\OPER\AXD\48256-96.SPE 27/10199 -17- The method of claim 24, further including the step of removing excess polymeric material laminated to said intravascular stent structure.
  19. 26. A polymeric material containing a therapeutic drug for application to an intravascular stent for carrying and delivering said therapeutic drug within a blood vessel in which said intravascular stent is placed, comprising: a polymeric material having a relatively low thermal processing temperature; particles of a therapeutic drug incorporated in said polymeric material; and a porosigen incorporated in said polymeric material.
  20. 27. The polymeric material of claim 26, wherein said polymeric material has a thermal processing temperature no greater than about 100 0 C.
  21. 28. The polymeric material of claim 26, wherein said polymeric material is selected from the group consisting of polycaprolactone, poly(ethylene-co-vinyl acetate), poly(vinyl acetate), silicone gum rubber, poly-DL-lactic acid (DL-PLA), poly-L-lactic acid (L-PLA), polyorthoesters, polyiminocarbonates, aliphatic polycarbonates, polyphosphazenes, and mixtures thereof.
  22. 29. The polymeric material of claim 26, wherein said particles of said therapeutic drug have a maximum cross- sectional dimension of up to 10 microns. P:\OPER\AXD\48256-96.SPE 27110/99 -18- The polymeric material of claim 26, wherein said therapeutic drug is a drug selected from the group consisting of heparin, D-phe-pro-arg-chloromethylketone, dipyridamole, hirudin, recombinant hirudin, thrombin inhibitor, angiopeptin, angiotensin converting enzyme inhibitors, calcium channel blockers, colchicine, fibroblast growth factor antagonists, fish oil, omega 3-fatty acid, low molecular weight heparin, histamine S" antagonists, inhibitors of HMG-CoA reductase, methotrexate, monoclonal antibodies, nitroprusside, phosphodiesterase inhibitors, prostacyclin and prostacyclin analogues, prostaglandin inhibitor, PDGF antagonists, serotonin blockers, steroids, thioprotease inhibitors, triazolopyrimidine, alpha- interferon, and genetically engineered epithelial cells, and mixtures thereof.
  23. 31. The polymeric material of claim 26, wherein said particles of said therapeutic drug comprise up to 70% by weight of the total weight of the therapeutic drug and the polymeric material.
  24. 32. The polymeric material of claim 26, wherein said particles of said therapeutic drug comprise up to 40% by weight of the total weight of the therapeutic drug and the polymeric material.
  25. 33. The polymeric material of claim 26, wherein said porosigen is selected from the group consisting of sodium chloride, lactose, sodium heparin, polyethylene glycol, polyethylene oxide/polypropylene oxide copolymers, and mixtures thereof. P:\OPER\AXD\48256-96.SPE 2710199 -19-
  26. 34. The polymeric material of claim 36, wherein said polymeric material comprises a surface defining pores with a maximum cross-sectional dimension of less than about 10 microns. The polymeric material of claim 26, further including a rate-controlling membrane.
  27. 36. The polymeric material of claim 35, wherein said rate- S""controlling membrane is formed to include a uniform distribution of a porosigen, said porosigen being selected from the group consisting of sodium chloride, lactose, sodium heparin, polyethylene glycol, polyethylene oxide/polypropylene oxide copolymers, and mixtures thereof.
  28. 37. The polymeric material of claim 35, wherein said rate- controlling membrane comprises a surface defining pores with a maximum cross-sectional dimension of about 10 microns.
  29. 38. The polymeric material of claim 35, wherein said rate- controlling membrane comprises a surface defining pores with a maximum cross-sectional dimension of about one micron.
  30. 39. The polymeric material of claim 26, wherein said polymeric material containing said therapeutic drug is formed as a sheet at least about 25 microns thick. The polymeric material of claim 39, wherein said sheet of polymeric material containing said therapeutic drug further is laminated to an intravascular stent structure.
  31. 41. A method of incorporating a therapeutic drug into a polymeric material substantially as hereinbefore described with reference to the drawings and Examples. P;\OPER\AXD\48256-96.SPE -25/5/00J 20
  32. 42. A polymeric material incorporating a therapeutic drug substantially as hereinbefore described with reference to the drawings and Examples. DATED this 25th day of MAY,2000 **ADVANCED CARDIOVASCULAR SYSTEMS, INC. by DAVIES COLLISON CAVE Patent Attorneys for the applicant
AU36425/00A 1995-03-30 2000-05-25 Method of incorporating drugs into a polymer component of stents Ceased AU738034B2 (en)

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FR2673843B1 (en) * 1991-03-14 1995-01-13 Centre Nat Rech Scient IMPLANTABLE, BIORESORBABLE PHARMACEUTICAL COMPOSITION BASED ON POLY (LACTIC ACID), INTENDED TO IMPLEMENT A LOCAL INTERNAL ANTIBOTHERAPY.
US5342348A (en) * 1992-12-04 1994-08-30 Kaplan Aaron V Method and device for treating and enlarging body lumens
EP0604022A1 (en) * 1992-12-22 1994-06-29 Advanced Cardiovascular Systems, Inc. Multilayered biodegradable stent and method for its manufacture

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