Patent Grant
7396539
1. Field of the Invention
This invention relates to implantable medical devices such as stents. More particularly, the invention relates to coatings for stents.
2. Description of the State of the Art
Percutaneous transluminal coronary angioplasty (PTCA) is a procedure for treating heart disease. A catheter assembly having a balloon portion is introduced percutaneously into the cardiovascular system of a patient via the brachial or femoral artery. The catheter assembly is advanced through the coronary vasculature until the balloon portion is positioned across the occlusive lesion. Once in position across the lesion, the balloon is inflated to a predetermined size to radially compress against the atherosclerotic plaque of the lesion to remodel the lumen wall. The balloon is then deflated to a smaller profile to allow the catheter to be withdrawn from the patient's vasculature.
A problem associated with the above procedure includes formation of intimal flaps or torn arterial linings which can collapse and occlude the conduit after the balloon is deflated. Moreover, thrombosis and restenosis of the artery may develop over several months after the procedure, which may require another angioplasty procedure or a surgical by-pass operation. To reduce the partial or total occlusion of the artery by the collapse of arterial lining and to reduce the chance of the development of thrombosis and restenosis, a stent is implanted in the lumen to maintain the vascular patency.
Stents are used not only as a mechanical intervention but also as a vehicle for providing biological therapy. As a mechanical intervention, stents act as scaffoldings, functioning to physically hold open and, if desired, to expand the wall of the passageway. Typically, stents are capable of being compressed, so that they can be inserted through small vessels via catheters, and then expanded to a larger diameter once they are at the desired location. Examples in patent literature disclosing stents which have been applied in PTCA procedures include stents illustrated in U.S. Pat. No. 4,733,665 issued to Palmaz, U.S. Pat. No. 4,800,882 issued to Gianturco, and U.S. Pat. No. 4,886,062 issued to Wiktor.
Biological therapy can be achieved by medicating stents. Medicated stents provide for the local administration of a therapeutic substance at the diseased site. In order to provide an efficacious concentration to the treated site, systemic administration of such medication often produces adverse or toxic side effects for the patient. Local delivery is a preferred method of treatment in that smaller total levels of medication are administered in comparison to systemic dosages, but are concentrated at a specific site. Local delivery thus produces fewer side effects and achieves more favorable results.
One proposed method for medicating stents involves the use of a polymeric carrier coated onto the surface of a stent. A solution which includes a solvent, a polymer dissolved in the solvent, and a therapeutic substance dispersed in the blend is applied to the stent. The solvent is allowed to evaporate, leaving on the stent surface a coating of the polymer and the therapeutic substance impregnated in the polymer.
The current state of the art discloses a variety of polymeric material that can be used for the sustained delivery of therapeutic substances. What is lacking, however, is coating configurations and layering designs which provide for tailored drug delivery capabilities. The embodiments of the invention provide for improved coating patterns for stents or other implantable medical devices.
In accordance with one embodiment, a stent having a coating is provided. The coating comprises a first region including a thermoplastic polyacrylate material and a therapeutic substance and a second region free from any therapeutic substances disposed on the surface of the stent and beneath the first region. The thermoplastic polyacrylate material can comprise oligomers, pre-polymers, homopolymers, copolymers, or terpolymers of alkylacrylates or alkylmethacrylates. In one embodiment, the polyacrylate material is poly(n-butyl methacrylate). The second region can include a non-acrylate polymer, such as an ethylene vinyl alcohol copolymer. In one embodiment, the coating can include a third region disposed over the first region, the third region including a thermoplastic polyacrylate material and optionally a therapeutic substance. The first region can have a variable thickness along at least a segment of the length of the stent such that the concentration of the substance varies along the length of the stent.
In accordance with another embodiment of the invention, a stent is provided comprising a coating, wherein the coating includes a first, second, and third layers disposed over one another wherein at least two of the layers include a thermoplastic polyacrylate material and wherein at least one of the layers includes a therapeutic substance. In one embodiment, the first layer is disposed on the outer surface of the stent, the second and third layers include the thermoplastic polyacrylate material, and the therapeutic substance is contained in the second layer and optionally the third layer but not the first layer. In accordance with another embodiment, the first layer and the third layer include the therapeutic substance but not the second layer and the second layer and the third layer include the thermoplastic polyacrylate material. In accordance with yet another embodiment, the first, second and third layers include the thermoplastic polyacrylate material and at least one of the layers is free from any therapeutic substances.
A stent comprising a coating having a variable thickness along at least a portion of the length of the stent is also provided so as to provide a concentration gradient of an active agent or agents along from a thin region of the coating to a thicker region of the coating.
In accordance with yet another embodiment, a method of coating a stent is provided, the method comprises forming a coating on the stent, the coating including a first region having a thermoplastic polyacrylate material and a therapeutic substance and a second region free from any therapeutic substances disposed on the surface of the stent beneath the first region.
In accordance with yet another embodiment of the invention, a method of coating a stent is provided comprising forming at least three layers of coating on a stent, wherein at least two of the layers include a thermoplastic polyacrylate material and wherein at least one of the layers includes a therapeutic substance.
In accordance with yet another embodiment of the invention, a method of coating a stent is provided comprising depositing a coating on the stent wherein the coating has a variable thickness along at least a segment of the length of the stent.
In accordance with yet another embodiment of the invention, a method of coating a stent, is provided comprising, depositing a first layer on the stent, the first layer including a first therapeutic substance; masking a region of the first layer; depositing a second layer on the first layer not covered by the masking layer, the second layer including a second therapeutic substance.
A stent coating having an engineered drug release rate can be fabricated by depositing on the stent any combination of the following layers, but for a reservoir layer which must be present in the coating: a primer layer; a reservoir layer of or containing an active agent or a drug; a topcoat layer free from any agents or drugs for serving as a rate reducing membrane; and a finishing coat layer. The finishing coat layer, which if used would be the outermost layer in the coating configuration for contacting the vessel tissues, can include an active agent or can be modified to have therapeutic materials, such as heparin, attached or conjugated to the surface thereof. Alternatively, the finishing coat layer can be made from a very bio-friendly material such a poly ethylene glycol (PEG). The purpose of the finishing coat layer is to reduce or prevent any adverse effects, such as more than acceptable degrees of inflammation or thrombi accumulation, which may be caused by the presence of the coated stent. The finishing coat layer can also serve as a rate limiting membrane for reducing the rate of release of the agent from the reservoir layer.
To deposit any of the coating layers, techniques known to those having ordinary skill in the art can be used. For example, a polymer can be dissolved in a solvent, or a mixture of solvents, and the resulting composition can be sprayed on the stent or the stent can be immersed in the composition. In one embodiment, thermoplastic polyacrylate materials can be used for any of the aforementioned layers or combination of layers. “Thermoplastic polyacrylate materials” are broadly defined as materials which include thermoplastic polyacrylates. “Polyacrylates” are defined to include oligomers, pre-polymers, homopolymers, copolymers, terpolymers, etc. of alkylacrylates or alkylmethacrylates, and blends thereof. Thermoplastic polyacrylate materials can also include blends of thermoplastic polyacrylates with non-acrylic materials.
Representative alkyl groups in alkylacrylates or alkylmethacrylates include C1-C12 straight-chained or branched alkyls. Examples of alkylacrylates or alkylmethacrylates that can be used include poly(n-butyl methacrylate) (PBMA), poly(ethyl methacrylate) (PEMA), and poly(ethyl methacrylate-co-butyl methacrylate) [P(EMA-BMA)].
Examples of suitable non-acrylic materials that can be blended with thermoplastic polyacrylates include fluorinated polymers and/or copolymers, such as poly(vinylidene fluoride) (PVDF) and poly(vinylidene fluoride-co-hexafluoro propene) (PVDF-HFP). One example of a commercially available fluorinated polymer that can be used is a PVDF resin distributed by ATOFINA Chemicals, Inc. of Philadelphia, Pa. under the trade name KYNAR. A suitable blend of a thermoplastic polyacrylate and a fluorinated polymer can contain between about 10 and about 95% mass of the fluorinated polymer. In another embodiment, the non-acrylic polymer can be poly(ethylene-co-vinyl alcohol) (also known as EVAL or EVOH). Poly(ethylene-co-vinyl alcohol) is available from Adrich Co., Milwaukee Wis. or EVAL Company of America, Lisle, Ill. These non-acrylic polymers, however, need not be used with the thermoplastic polyacrylate and can be used alone or in combination with other polymers to form any of the coating layers.
Representative examples of other polymers that can be used for any of the coating layer included poly(hydroxyvalerate), poly(L-lactic acid), polycaprolactone, poly(lactide-co-glycolide), poly(hydroxybutyrate), poly(hydroxybutyrate-co-valerate), polydioxanone, polyorthoester, polyanhydride, poly(glycolic acid), poly(D,L-lactic acid), poly(glycolic acid-co-trimethylene carbonate), polyphosphoester, polyphosphoester urethane, poly(amino acids), cyanoacrylates, poly(trimethylene carbonate), poly(iminocarbonate), co-poly(ether-esters) (e.g. PEO/PLA), polyalkylene oxalates, polyphosphazenes, biomolecules (such as fibrin, fibrinogen, cellulose, starch, collagen and hyaluronic acid), polyurethanes, silicones, polyesters, polyolefins, polyisobutylene and ethylene-alphaolefin copolymers, vinyl halide polymers and copolymers (such as polyvinyl chloride), polyvinyl ethers (such as polyvinyl methyl ether), polyvinylidene chloride, polyacrylonitrile, polyvinyl ketones, polyvinyl aromatics (such as polystyrene), polyvinyl esters (such as polyvinyl acetate), copolymers of vinyl monomers with each other and olefins (such as ethylene-methyl methacrylate copolymers, acrylonitrile-styrene copolymers, ABS resins, and ethylene-vinyl acetate copolymers), polyamides (such as Nylon 66 and polycaprolactam), alkyd resins, polycarbonates, polyoxymethylenes, polyimides, polyethers, epoxy resins, polyurethanes, rayon, rayon-triacetate, cellulose, cellulose acetate, cellulose butyrate, cellulose acetate butyrate, cellophane, cellulose nitrate, cellulose propionate, cellulose ethers, and carboxymethyl cellulose.
Representative examples of some solvents suitable for making the composition include N,N-dimethylacetamide (DMAC), N,N-dimethylformamide (DMF), tethrahydrofurane (THF), cyclohexanone, xylene, toluene, and acetone. Solvent mixtures can also be used as well. One representative examples of a suitable mixture is FLUX REMOVER AMS, a trade name of a solvent mixture manufactured by Tech Spray, Inc. of Amarillo, Tex. comprising about 93.7% of a mixture of 3,3-dichloro-1,1,1,2,2-pentafluoropropane and 1,3-dichloro-1,1,2,2,3-pentafluoropropane, and the balance methanol, with trace amounts of nitromethane.
In on embodiment, the agent or drug can be dissolved in the composition or dispersed in the composition in fine particles for manufacturing the reservoir layer and the finishing coating layer. The agent can include any substance capable of exerting a therapeutic or prophylactic effect in the practice of the present invention. The drug may include small molecule drugs, peptides, proteins, and oligonucleotides. One example of an agent that can be used by being incorporated into the reservoir layer or the finishing coating layer is estradiol. By way of example, the mass ratio between estradiol and the polymer can be between about 5:1 and 0.2:1 for the finishing coat layer and between about 1:2 and 1:0.6 for the reservoir layer. Examples of other drugs include those that fall under the genus of antiproliferative, antineoplastic, anti-inflammatory, antiplatelet, anticoagulant, antifibrin, antithrombin, antimitotic, antibiotic, antiallergic and antioxidant substances. Specific examples include actinomycin D, paclitaxel, docetaxel, methotrexate, azathioprine, vincristine, vinblastine, fluorouracil, doxorubicin hydrochloride, mitomycin, sodium heparin, low molecular weight heparins, heparinoids, hirudin, argatroban, forskolin, vapiprost, prostacyclin and prostacyclin analogues, dextran, D-phe-pro-arg-chloromethylketone (synthetic antithrombin), dipyridamole, glycoprotein IIbilia platelet membrane receptor antagonist antibody, recombinant hirudin, angiopeptin, angiotensin converting enzyme inhibitors such as captopril, cilazapril or lisinopril, calcium channel blockers (such as nifedipine), colchicine, fibroblast growth factor (FGF) antagonists, fish oil (ω-3-fatty acid), histamine antagonists, lovastatin (an inhibitor of HMG-CoA reductase, a cholesterol lowering drug), monoclonal antibodies (such as those specific for Platelet-Derived Growth Factor (PDGF) receptors), nitroprusside, phosphodiesterase inhibitors, prostaglandin inhibitors, suramin, serotonin blockers, steroids, thioprotease inhibitors, triazolopyrimidine (a PDGF antagonist), and nitric oxide. An example of an antiallergic agent is permirolast potassium. Other therapeutic substances or agents which may be appropriate include alpha-interferon, genetically engineered epithelial cells, rapamycin and structural derivatives or functional analogs thereof, such as 40-O-(2-hydroxy)ethyl-rapamycin (known by the trade name of EVEROLIMUS available from Novartis), 40-O-(3-hydroxy)propyl-rapamycin and 40-O-[2-(2-hydroxy)ethoxy]ethyl-rapamycin; tacrolimus and dexamethasone.
The drug can be also included in micro-depot areas of a stent. Different drugs can be used with the same stent. For example, paclitaxel can be loaded in the micro-depot areas, everolimus in the drug-reservoir layer, and dexamethasone in the finishing coat layer.
In accordance with another embodiment, the drug, such as estradiol, can be incorporated into a polymeric reservoir layer or the optional finishing coat layer in the form of particles of micron to sub-micron size. For example, the particles can have a diameter between about 0.5 and 4.0 μm. The drug can be encapsulated into the particles, followed by suspending the particles in the polymer solution. The suspension can be then applied to the stent. By way of example, the mass ratio between micro- or nanoparticles and the polymer in the suspension can be within a range of between about 1:5 and 1:10.
The particles can be defined by spherical outer shells made of an encapsulating polymer which include an inside space filled with the drug. When the stent is in contact with body fluids, the polymer forming the outer shell of the particles can hydrolyze and degrade thus releasing the drug. The particles can be made by emulsion method according to techniques known to those having ordinary skill in the art. Examples of suitable encapsulating polymers include poly(glycolic acid) (PGA), poly(D-lactic acid)(PDLA), poly(L-lactic acid)(PLLA), poly(butylene terephtalate-co-ethylene glycol)(PBT-PEG), and mixtures thereof.
In accordance with one embodiment of the invention, the reservoir layer can have a variable thickness along at least a segment of the length of the stent. Referring to
When the last desired sub-layer of the reservoir layer 16 has been formed, the masking material is removed and discarded, and a topcoat layer 18 or a finishing coat layer 20 can be deposited on reservoir layer 16. If a topcoat layer is used, the finishing coat layer can be applied over the topcoat layer.
In accordance with one embodiment of the invention, a stent coating that develops cracks immediately upon expansion of the stent can be fabricated. This coating can be used if a high rate of release of the drug is desired. The cracks which typically develop across the entire coating may help to achieve such high rate of release by providing a channel through which the drug would easily and quickly diffuse from the drug-polymer layer through the topcoat membrane.
The coatings and methods of the present invention have been described in conjunction with a stent. The stent can be a balloon-expandable or self-expandable stent, or can include micro-depot areas to contain drugs. The use of the coating, however, is not limited to stents and the coating can also be used with a variety of other medical devices. Examples of the implantable medical device that can be used in conjunction with the embodiments of this invention include stent-grafts, grafts (e.g., aortic grafts), artificial heart valves, cerebrospinal fluid shunts, pacemaker electrodes, axius coronary shunts and endocardial leads (e.g., FINELINE and ENDOTAK, available from Guidant Corporation).
The underlying structure of the device can be of virtually any design. The device can be made of a metallic material or an alloy such as, but not limited to, cobalt-chromium alloys (e.g., ELGILOY), stainless steel (316L), “MP35N,” “MP20N,” ELASTINITE (Nitinol), tantalum, tantalum-based alloys, nickel-titanium alloy, platinum, platinum-based alloys such as, e.g., platinum-iridium alloy, iridium, gold, magnesium, titanium, titanium-based alloys, zirconium-based alloys, or combinations thereof. Devices made from bioabsorbable or biostable polymers can also be used with the embodiments of the present invention. “MP35N” and “MP20N” are trade names for alloys of cobalt, nickel, chromium and molybdenum available from Standard Press Steel Co. of Jenkintown, Pa. “MP35N” consists of 35% cobalt, 35% nickel, 20% chromium, and 10% molybdenum. “MP20N” consists of 50% cobalt, 20% nickel, 20% chromium, and 10% molybdenum.
Various embodiments of the present invention can be further illustrated by the following examples.
A first composition can be prepared by mixing the following components:
(a) between about 1.0 mass % and about 15 mass %, for example, about 2.0 mass % of EVAL; and
(b) the balance, DMAC solvent.
The first composition can be sprayed on the surface of a bare 13 mm TETRA stent (available from Guidant Corporation). The spray can have a 0.014 fan nozzle maintained at about 60° C. with a feed pressure of about 0.2 atm (about 3 psi) and an atomization pressure of about 1.3 atm (about 20 psi). Between about 40 μg and 100 μg, for example, about 70 μg of the wet coating can be applied. The composition can be baked at about 140° C. for about 2 hours, yielding a dry primer layer.
A second composition can be prepared by mixing the following components:
(c) between about 1.0 mass % and about 15 mass %, for example, about 2.0 mass % of EVAL;
(d) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(e) the balance, DMAC solvent.
The second composition can be applied onto the dried primer layer to form a drug-polymer or reservoir layer, using the same spraying technique and equipment used for applying the primer layer. Between about 300 μg and 500 μg of the wet coating can be applied, followed by drying by baking the stent. The dry drug-polymer layer can contain between about 30 and 70 mass % of the drug, for example, between about 34 and 63 mass %, corresponding to the drug/polymer ration in the dry reservoir layer between about 1:2.3 and about 1:0.4, for example, between about 1:1.9 and 1:0.6.
A third composition can be prepared by mixing the following components:
(f) between about 1.0 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(g) the balance, a mixture of solvents including xylene, FLUX REMOVER AMS (“FLUX REMOVER”) and acetone in a ratio of about 25:19:5 by mass.
The third composition can be applied onto the dried drug-polymer layer, to form a topcoat layer. Between about 150 μg and 300 μg, for example, about 200 μg of the wet coating can be applied, followed by drying.
A fourth composition can be prepared by mixing the following components:
(h) between about 1.0 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(i) between about 0.5 mass % and about 2.0 mass %, for example, about 1 mass % of estradiol; and
(j) the balance, a mixture of solvents including xylene, FLUX REMOVER, and acetone in a ratio of about 25:19:5 by mass.
The fourth composition can be applied onto the dried topcoat layer, to form a finishing coat layer. Between about 100 μg and 175 μg, for example, about 100 μg of the wet coating can be applied, followed by drying. The dry finishing coat layer can contain between about 33 and 70 mass % of the drug, corresponding to the drug/polymer ration in the finishing coat layer between about 1:2 and about 1:0.4.
The rate of release of estradiol from various stents coated according to the procedure of Example 1 was measured by using a standard technique known to those having ordinary skill in the art.
A primer layer can be formed as described in Example 1. A first composition can be prepared by mixing the following components:
(a) between about 0.1 mass % and about 15 mass %, for example, about 1.0 mass % of EVAL;
(b) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(c) the balance, DMAC solvent.
About 250 μg of the wet composition can be applied onto the dried primer layer, followed by drying, to form a drug-polymer layer.
A second composition can be prepared by mixing the following components:
(d) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(e) the balance, a solvent mixture including cyclohexanone and FLUX REMOVER in a ratio of about 30:19 by mass.
About 300 μg of the wet composition can be applied onto the drug-polymer layer, followed by drying, to form the topcoat layer.
A third composition can be prepared by mixing the following components:
(f) between about 1.0 mass % and about 15 mass %, for example, about 1.5 mass % of PBMA;
(g) between about 0.5 mass % and about 2.0 mass %, for example, about 1 mass % of estradiol; and
(h) the balance, a mixture of solvents including acetone, cyclohexanone and FLUX REMOVER, in a ratio of about 16:12:11 by mass.
About 75 μg of the wet composition can be applied onto the dried topcoat layer, followed by drying, to form a finishing coat layer.
A drug-polymer layer disposed on top of an optional primer layer can be formed as described in Example 2. A first composition can be prepared by mixing the following components:
(a) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of KYNAR; and
(b) the balance, a solvent mixture including acetone, cyclohexanone and FLUX REMOVER in a ratio of about 50:25:23 by mass.
About 300 μg of the wet composition can be applied onto the drug-polymer layer, followed by drying.
A second composition can be prepared by mixing the following components:
(c) between about 0.5 mass % and about 15 mass %, for example, about 1.0 mass % of KYNAR;
(d) between about 0.05 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(e) the balance, a mixture of solvents including acetone, cyclohexanone and FLUX REMOVER, in a ratio of about 50:250:23 by mass.
Between about 100 μg and 175 μg of the wet coating can be applied, followed by drying. The dry finishing coat layer can contain between about 33 and 56 mass % of the drug, corresponding to the drug/polymer ration in the finishing coat layer between about 1:2 and about 1:0.8.
A primer layer can be formed as described in Example 1. A first composition can be prepared by mixing the following components:
(a) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of EVAL;
(b) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(c) the balance, a solvent mixture, the mixture including DMAC and ethanol (EtOH) in a ratio of about 57:40 by mass.
About 300 μg of the wet composition can be applied onto the dried primer layer, followed by drying to form a first sub-layer of a drug-polymer layer.
A second composition, a suspension, can be prepared by mixing the following components:
(d) between about 0.5 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(e) between about 0.5 mass % and about 2.0 mass %, for example, about 2.0 mass % of drug-loaded particles (DLP), the DLP comprising estradiol incorporated in a shell made of PLLA; and
(f) the balance, a mixture of solvents including ethanol, FLUX REMOVER, and acetone, in a ratio of about 40:37:20 by mass.
About 300 μg of the suspension can be applied onto the first sub-layer of the drug-polymer layer to form a second sub-layer of the drug-polymer layer and to complete the formation of the drug-polymer layer.
A third composition can be prepared by mixing the following components:
(g) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(h) the balance, a solvent mixture including DMAC and FLUX REMOVER in a ratio of about 30:19 by mass.
About 200 μg of the wet composition can be applied onto the drug-polymer layer, followed by drying, to form the topcoat layer.
A fourth composition can be prepared by mixing the following components:
(i) between about 0.5 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(j) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(k) the balance, a mixture of solvents including acetone, cyclohexanone and FLUX REMOVER, in a ratio of about 20:15:14 by mass.
About 100 μg of the wet composition can be applied onto the dried topcoat layer followed by drying, to form a finishing coat layer.
An optional primer layer can be formed as described in Example 1. A first composition can be prepared by mixing the following components:
(a) between about 0.1 mass % and about 15 mass %, for example, about 1.0 mass % of EVAL;
(b) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(c) the balance, DMAC solvent.
About 250 μg of the wet first composition can be applied onto the dried primer layer, followed by drying, to form a first sub-layer of a drug-polymer layer.
A second composition including a suspension can be prepared and applied onto the first sub-layer as described in Example 4, to form a second sub-layer of the drug-polymer layer and to complete the formation of the drug-polymer layer. Following the formation of the drug-polymer layer, a topcoat layer and a finishing coat layer formulations can be prepared and applied to form the topcoat and finishing coat layers, as described in Example 4.
A first composition can be prepared by mixing the following components:
(a) between about 1.0 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(b) the balance, cyclohexanone solvent.
About 70 μg of the wet composition can be applied onto the surface of a bare stent to form an optional primer layer.
A second composition can be prepared by mixing the following components:
(c) between about 0.1 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(d) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(e) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 75 μg of the wet second composition can be applied onto the dried primer layer, followed by drying, to form a first sub-layer of a drug-polymer layer. Following formation of the first sub-layer of the drug-polymer layer, a portion of the first sub-layer can be masked (about 50% of the length of the first sub-layer can be masked).
A third composition can be prepared by mixing the following components:
(f) between about 0.1 mass % and about 15 mass %, for example, about 1.5 mass % of PBMA;
(g) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(h) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 16:15:8 by mass.
About 75 μg of the wet third composition can be applied onto the dried first sub-layer, followed by drying, to form a second sub-layer of the drug-polymer layer. Following formation of the second sub-layer of the drug-polymer layer, a portion of the second sub-layer can be masked and the steps repeated until the drug-polymer coating has a total of about 300 μg of PBMA and about 200 μg of estradiol.
A final composition can be prepared, containing:
(i) between about 1.0 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(j) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 200 μg of the wet final composition can be applied onto the drug-polymer layer, followed by drying, to form the topcoat layer.
An optional primer layer can be formed as described in Example 1. A first composition can be prepared by mixing the following components:
(a) between about 0.1 mass % and about 15 mass %, for example, about 1.5 mass % of PBMA;
(b) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(c) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 16:15:8 by mass.
About 75 μg of the wet first composition can be applied onto the dried primer layer, followed by drying, to form a first layer of a drug-polymer layer. Following formation of the first layer, a portion of the first layer, for example, about 50% of the length of the first layer, can be masked.
A second composition can be prepared by mixing the following components:
(d) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(e) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 200 μg of the wet second composition can be applied onto the first layer, followed by drying, to form a second layer.
A third composition can be prepared by mixing the following components:
(f) between about 0.1 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(g) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(h) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 75 μg of the wet third composition can be applied to the stent, followed by drying, to form a third layer. Following formation of the third layer, a portion of the third layer, for example, about 50% of the length of the third layer can be masked.
A fourth composition can be prepared by mixing the following components:
(i) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(j) the balance, a mixture of solvents, the mixture including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 100 μg of the wet fourth composition can be applied to the stent, followed by drying to form a fourth layer.
A fifth composition can be prepared by mixing the following components:
(k) between about 0.1 mass % and about 15 mass %, for example, about 1.0 mass % of PBMA;
(l) between about 0.5 mass % and about 2.0 mass %, for example, about 1.0 mass % of estradiol; and
(m) the balance, a mixture of solvents including xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 75 μg of the wet fifth composition can be applied onto the stent, followed by drying, to form a fifth layer.
A sixth composition can be prepared by mixing the following components:
(n) between about 0.1 mass % and about 15 mass %, for example, about 2.0 mass % of PBMA; and
(o) the balance, a mixture of solvents, xylene, FLUX REMOVER, and acetone in a ratio of about 20:19:10 by mass.
About 200 μg of the wet sixth composition can be applied, followed by drying, to form a topcoat layer.
A first composition was prepared by mixing the following components:
(a) about 3.0 mass % of EVAL;
(b) about 25 mass % of ethanol; and
(c) the balance, DMAC solvent.
The first composition was applied onto the stent to form a primer layer as described in Example 1. The primer layer had solids of about 40 μg.
A second composition was prepared by mixing the following components:
(d) about 2.0 mass % of EVAL;
(e) about 1.0 mass % of EVEROLIMUS;
(f) about 25 mass % of pentane; and
(g) the balance, DMAC solvent.
The second composition was applied onto the dried primer layer to form a drug-polymer layer as described in Example 1. The drug-polymer layer was dried for about 1 hour at a temperature of about 80° C., to form the dry reservoir layer having solids of about 834 μg.
A third composition was prepared by mixing the following components:
(h) about 4.0 mass % of EVAL;
(i) about 20 mass % of pentane; and
(j) the balance, DMAC solvent.
The third composition was onto the dried drug-polymer layer, to form a topcoat layer, as described in Example 1. The drug-polymer layer was dried for about 1 hour at a temperature of about 80° C., to form the dry reservoir layer having solids of about 100 μg.
The stent coated as described in Example 8 was expanded. Immediately upon the expansion, the cracks developed across the entire coating, as shown by the microphotograph presented in
While particular embodiments of the present invention have been shown and described, it will be obvious to those skilled in the art that changes and modifications can be made without departing from this invention in its broader aspects. Therefore, the appended claims are to encompass within their scope all such changes and modifications as fall within the true spirit and scope of this invention.
| Number | Name | Date | Kind |
|---|---|---|---|
| 2968649 | Pailthorp et al. | Jan 1961 | A |
| 3051677 | Rexford | Aug 1962 | A |
| 3178399 | Lo | Apr 1965 | A |
| 3324069 | Koblitz et al. | Jun 1967 | A |
| 3779805 | Alsberg | Dec 1973 | A |
| 3856827 | Cavitt | Dec 1974 | A |
| 4076929 | Dohany | Feb 1978 | A |
| 4197380 | Chao et al. | Apr 1980 | A |
| 4304010 | Mano | Dec 1981 | A |
| 4346710 | Thanawalla et al. | Aug 1982 | A |
| 4353960 | Endo et al. | Oct 1982 | A |
| 4399264 | Squire | Aug 1983 | A |
| 4413359 | Akiyama et al. | Nov 1983 | A |
| 4423183 | Close | Dec 1983 | A |
| 4485250 | Squire | Nov 1984 | A |
| 4530569 | Squire | Jul 1985 | A |
| 4564013 | Lilenfeld et al. | Jan 1986 | A |
| 4569978 | Barber | Feb 1986 | A |
| 4632842 | Karwoski et al. | Dec 1986 | A |
| 4636346 | Gold et al. | Jan 1987 | A |
| 4718907 | Karwoski et al. | Jan 1988 | A |
| 4733665 | Palmaz | Mar 1988 | A |
| 4749585 | Greco et al. | Jun 1988 | A |
| 4754009 | Squire | Jun 1988 | A |
| 4770939 | Sietsess et al. | Sep 1988 | A |
| 4800882 | Gianturco | Jan 1989 | A |
| 4871357 | Hsu et al. | Oct 1989 | A |
| 4876109 | Mayer et al. | Oct 1989 | A |
| 4886062 | Wiktor | Dec 1989 | A |
| 4897457 | Nakamura et al. | Jan 1990 | A |
| 4908404 | Benedict et al. | Mar 1990 | A |
| 4910276 | Nakamura et al. | Mar 1990 | A |
| 4931287 | Bae et al. | Jun 1990 | A |
| 4935477 | Squire | Jun 1990 | A |
| 4948851 | Squire | Aug 1990 | A |
| 4973142 | Squire | Nov 1990 | A |
| 4975505 | Squire | Dec 1990 | A |
| 4977008 | Squire | Dec 1990 | A |
| 4977025 | Squire | Dec 1990 | A |
| 4977026 | Squire | Dec 1990 | A |
| 4977297 | Squire | Dec 1990 | A |
| 4977901 | Ofstead | Dec 1990 | A |
| 4982056 | Squire | Jan 1991 | A |
| 4985308 | Squire | Jan 1991 | A |
| 4999248 | Squire | Mar 1991 | A |
| 5000547 | Squire | Mar 1991 | A |
| 5006382 | Squire | Apr 1991 | A |
| 5030394 | Sietses et al. | Jul 1991 | A |
| 5047020 | Hsu | Sep 1991 | A |
| 5051114 | Nemser et al. | Sep 1991 | A |
| 5051978 | Mayer et al. | Sep 1991 | A |
| 5053048 | Pinchuk | Oct 1991 | A |
| 5076659 | Bekiarian et al. | Dec 1991 | A |
| 5093427 | Barber | Mar 1992 | A |
| 5107852 | Davidson et al. | Apr 1992 | A |
| 5110645 | Matsumoto et al. | May 1992 | A |
| 5112457 | Marchant | May 1992 | A |
| 5176972 | Bloom et al. | Jan 1993 | A |
| 5185408 | Tang et al. | Feb 1993 | A |
| 5246451 | Trescony et al. | Sep 1993 | A |
| 5276121 | Resnick | Jan 1994 | A |
| 5296283 | Froggatt | Mar 1994 | A |
| 5302385 | Khan et al. | Apr 1994 | A |
| 5308685 | Froggatt | May 1994 | A |
| 5310838 | Hung et al. | May 1994 | A |
| 5324889 | Resnick | Jun 1994 | A |
| 5326839 | Resnick | Jul 1994 | A |
| 5328471 | Slepian | Jul 1994 | A |
| 5336518 | Narayanan et al. | Aug 1994 | A |
| 5338608 | Resnick | Aug 1994 | A |
| 5342348 | Kaplan | Aug 1994 | A |
| 5353368 | Resnick | Oct 1994 | A |
| 5354910 | Hung et al. | Oct 1994 | A |
| 5368566 | Crocker | Nov 1994 | A |
| 5380299 | Fearnot et al. | Jan 1995 | A |
| 5383853 | Jung et al. | Jan 1995 | A |
| 5383928 | Scott et al. | Jan 1995 | A |
| 5395311 | Andrews | Mar 1995 | A |
| 5403341 | Solar | Apr 1995 | A |
| 5408020 | Hung et al. | Apr 1995 | A |
| 5417969 | Hsu et al. | May 1995 | A |
| 5443458 | Eury | Aug 1995 | A |
| 5447724 | Helmus et al. | Sep 1995 | A |
| 5455040 | Marchant | Oct 1995 | A |
| 5464650 | Berg et al. | Nov 1995 | A |
| 5545208 | Wolff et al. | Aug 1996 | A |
| 5560463 | Link et al. | Oct 1996 | A |
| 5562734 | King | Oct 1996 | A |
| 5569463 | Helmus et al. | Oct 1996 | A |
| 5575818 | Pinchuk | Nov 1996 | A |
| 5578073 | Haimovich et al. | Nov 1996 | A |
| 5584877 | Miyake et al. | Dec 1996 | A |
| 5591224 | Schwartz et al. | Jan 1997 | A |
| 5604283 | Wada et al. | Feb 1997 | A |
| 5605696 | Eury et al. | Feb 1997 | A |
| 5616608 | Kinsella et al. | Apr 1997 | A |
| 5628728 | Tachibana et al. | May 1997 | A |
| 5632771 | Boatman et al. | May 1997 | A |
| 5632776 | Kurumatani et al. | May 1997 | A |
| 5632840 | Campbell | May 1997 | A |
| 5635201 | Fabo | Jun 1997 | A |
| 5667767 | Greff et al. | Sep 1997 | A |
| 5670558 | Onishi et al. | Sep 1997 | A |
| 5679400 | Tuch | Oct 1997 | A |
| 5684061 | Ohnishi et al. | Nov 1997 | A |
| 5691311 | Maraganore et al. | Nov 1997 | A |
| 5697967 | Dinh et al. | Dec 1997 | A |
| 5700286 | Tartaglia et al. | Dec 1997 | A |
| 5713949 | Jayaraman | Feb 1998 | A |
| 5716981 | Hunter et al. | Feb 1998 | A |
| 5750234 | Johnson et al. | May 1998 | A |
| 5758205 | Hara et al. | May 1998 | A |
| 5759205 | Valentini | Jun 1998 | A |
| 5760118 | Sinclair et al. | Jun 1998 | A |
| 5776184 | Tuch | Jul 1998 | A |
| 5804318 | Pinchuk et al. | Sep 1998 | A |
| 5820917 | Tuch | Oct 1998 | A |
| 5824048 | Tuch | Oct 1998 | A |
| 5824049 | Ragheb et al. | Oct 1998 | A |
| 5827587 | Fukushi | Oct 1998 | A |
| 5830178 | Jones et al. | Nov 1998 | A |
| 5837313 | Ding et al. | Nov 1998 | A |
| 5851508 | Greff et al. | Dec 1998 | A |
| 5858746 | Hubbell et al. | Jan 1999 | A |
| 5858990 | Walsh | Jan 1999 | A |
| 5860963 | Azam et al. | Jan 1999 | A |
| 5861168 | Cooke et al. | Jan 1999 | A |
| 5865814 | Tuch | Feb 1999 | A |
| 5869127 | Zhong | Feb 1999 | A |
| 5873904 | Ragheb et al. | Feb 1999 | A |
| 5874165 | Drumheller | Feb 1999 | A |
| 5879697 | Ding et al. | Mar 1999 | A |
| 5897911 | Loeffer | Apr 1999 | A |
| 5900425 | Kanikanti et al. | May 1999 | A |
| 5911704 | Humes | Jun 1999 | A |
| 5921933 | Sarkis et al. | Jul 1999 | A |
| 5922393 | Jayaraman | Jul 1999 | A |
| 5928279 | Shannon et al. | Jul 1999 | A |
| 5932299 | Katoot | Aug 1999 | A |
| 5945115 | Dunn et al. | Aug 1999 | A |
| 5971954 | Conway et al. | Oct 1999 | A |
| 5980928 | Terry | Nov 1999 | A |
| 5980972 | Ding | Nov 1999 | A |
| 5997517 | Whitbourne | Dec 1999 | A |
| 6015541 | Greff et al. | Jan 2000 | A |
| 6033724 | Molitor | Mar 2000 | A |
| 6042875 | Ding et al. | Mar 2000 | A |
| 6051648 | Rhee et al. | Apr 2000 | A |
| 6056993 | Leidner et al. | May 2000 | A |
| 6060451 | DiMaio et al. | May 2000 | A |
| 6060534 | Ronan et al. | May 2000 | A |
| 6080488 | Hostettler et al. | Jun 2000 | A |
| 6090134 | Tu et al. | Jul 2000 | A |
| 6096070 | Ragheb et al. | Aug 2000 | A |
| 6096396 | Patton et al. | Aug 2000 | A |
| 6096798 | Luthra et al. | Aug 2000 | A |
| 6096809 | Lorcks et al. | Aug 2000 | A |
| 6099562 | Ding et al. | Aug 2000 | A |
| 6099563 | Zhong | Aug 2000 | A |
| 6110188 | Narciso, Jr. | Aug 2000 | A |
| 6110483 | Whitbourne et al. | Aug 2000 | A |
| 6113629 | Ken | Sep 2000 | A |
| 6120536 | Ding et al. | Sep 2000 | A |
| 6120904 | Hostettler et al. | Sep 2000 | A |
| 6121027 | Clapper et al. | Sep 2000 | A |
| 6124045 | Soda et al. | Sep 2000 | A |
| 6129761 | Hubbell | Oct 2000 | A |
| 6153252 | Hossainy et al. | Nov 2000 | A |
| 6165212 | Dereume et al. | Dec 2000 | A |
| 6179817 | Zhong | Jan 2001 | B1 |
| 6197051 | Zhong | Mar 2001 | B1 |
| 6203551 | Wu | Mar 2001 | B1 |
| 6214901 | Chudzik et al. | Apr 2001 | B1 |
| 6224894 | Jamiolkowski et al. | May 2001 | B1 |
| 6231590 | Slaikeu et al. | May 2001 | B1 |
| 6242041 | Katoot et al. | Jun 2001 | B1 |
| 6254632 | Wu et al. | Jul 2001 | B1 |
| 6258121 | Yang et al. | Jul 2001 | B1 |
| 6262034 | Mathiowitz et al. | Jul 2001 | B1 |
| 6273913 | Wright et al. | Aug 2001 | B1 |
| 6299604 | Ragheb et al. | Oct 2001 | B1 |
| 6319520 | Wuthrich et al. | Nov 2001 | B1 |
| 6344035 | Chudzik et al. | Feb 2002 | B1 |
| 6362271 | Lin et al. | Mar 2002 | B1 |
| 6408878 | Unger et al. | Jun 2002 | B2 |
| 6410612 | Hatanaka | Jun 2002 | B1 |
| 6464683 | Samuelson et al. | Oct 2002 | B1 |
| 6503556 | Harish et al. | Jan 2003 | B2 |
| 6545097 | Pinchuk et al. | Apr 2003 | B2 |
| 6551708 | Tsuda et al. | Apr 2003 | B2 |
| 6716444 | Castro et al. | Apr 2004 | B1 |
| 6746773 | Llanos et al. | Jun 2004 | B2 |
| 6824559 | Michal | Nov 2004 | B2 |
| 20010014717 | Hossainy et al. | Aug 2001 | A1 |
| 20010029351 | Falotico et al. | Oct 2001 | A1 |
| 20020051730 | Bodnar et al. | May 2002 | A1 |
| 20020090389 | Humes et al. | Jul 2002 | A1 |
| 20020094440 | Lianos et al. | Jul 2002 | A1 |
| 20020099438 | Furst | Jul 2002 | A1 |
| 20020111590 | Davila et al. | Aug 2002 | A1 |
| 20020122877 | Harish et al. | Sep 2002 | A1 |
| 20020123801 | Pacetti et al. | Sep 2002 | A1 |
| 20020133183 | Lentz et al. | Sep 2002 | A1 |
| 20020143386 | Davila et al. | Oct 2002 | A1 |
| 20020165608 | Llanos et al. | Nov 2002 | A1 |
| 20020188037 | Chudzik et al. | Dec 2002 | A1 |
| 20030004563 | Jackson et al. | Jan 2003 | A1 |
| 20030031780 | Chudzik et al. | Feb 2003 | A1 |
| 20030039689 | Chen et al. | Feb 2003 | A1 |
| 20030060877 | Falotico et al. | Mar 2003 | A1 |
| 20030065346 | Evens et al. | Apr 2003 | A1 |
| 20030065377 | Davila et al. | Apr 2003 | A1 |
| 20030073961 | Happ | Apr 2003 | A1 |
| 20030077312 | Schmulewicz et al. | Apr 2003 | A1 |
| 20040063805 | Pacetti et al. | Apr 2004 | A1 |
| 20040102758 | Davila et al. | May 2004 | A1 |
| Number | Date | Country |
|---|---|---|
| 19723723 | Dec 1998 | DE |
| 0568310 | Nov 1993 | EP |
| 0623354 | Nov 1994 | EP |
| 0633032 | Jan 1995 | EP |
| 0 665 023 | Aug 1995 | EP |
| 0747069 | Dec 1996 | EP |
| 0815803 | Jan 1998 | EP |
| 0893108 | Jan 1999 | EP |
| 0950385 | Oct 1999 | EP |
| 0950386 | Oct 1999 | EP |
| 0 970 711 | Jan 2000 | EP |
| 0968688 | Jan 2000 | EP |
| 0997115 | May 2000 | EP |
| 1 023 879 | Aug 2000 | EP |
| 1 192 957 | Apr 2002 | EP |
| WO 9205695 | Apr 1992 | WO |
| WO 9218320 | Oct 1992 | WO |
| WO 9402185 | Feb 1994 | WO |
| WO 9621404 | Jul 1996 | WO |
| WO 9741164 | Nov 1997 | WO |
| WO 9808463 | Mar 1998 | WO |
| WO 9813405 | Apr 1998 | WO |
| WO 9836784 | Aug 1998 | WO |
| WO 9858680 | Dec 1998 | WO |
| WO 9932051 | Jul 1999 | WO |
| WO 9955396 | Nov 1999 | WO |
| WO 0002599 | Jan 2000 | WO |
| WO 0012147 | Mar 2000 | WO |
| WO 0027455 | May 2000 | WO |
| WO 0029043 | May 2000 | WO |
| WO 0032255 | Jun 2000 | WO |
| WO 0038754 | Jul 2000 | WO |
| WO 0041738 | Jul 2000 | WO |
| WO 0064506 | Nov 2000 | WO |
| WO 0101890 | Jan 2001 | WO |
| WO 0130403 | May 2001 | WO |
| WO 0149340 | Jul 2001 | WO |
| WO 0187342 | Nov 2001 | WO |
| WO 0187368 | Nov 2001 | WO |
| WO 0187372 | Nov 2001 | WO |
| WO 0187376 | Nov 2001 | WO |
| WO 0224249 | Mar 2002 | WO |
| WO 0226139 | Apr 2002 | WO |
| WO 0226271 | Apr 2002 | WO |
| WO 0226281 | Apr 2002 | WO |
| WO 0234311 | May 2002 | WO |
| WO 0247731 | Jun 2002 | WO |
| WO 0247732 | Jun 2002 | WO |
| WO 03022324 | Mar 2003 | WO |
