Coated endovascular stent

Description

BACKGROUND OF THE INVENTION

The present invention relates to endovascular stents and more particularly pertains to coatings that are applied to stents in order to reduce thrombogenicity.

Stents are implanted within blood vessels in an effort to maintain their patency by preventing collapse of the lumen and/or by impeding restenosis. Unfortunately, the presence of a foreign object within the blood flow may have a thrombogenic effect. It has therefore been found to be desirable to use various anti-coagulant drugs in an effort to reduce the likelihood of the development of restenosis and provide an antithrombogenic effect.

A drug that has been found to be particularly effective for such purpose is heparin. By maintaining an effective concentration of the drug in and about the implantation site until the stent is encapsulated by tissue, the risk of thrombogenesis is substantially mitigated. To that end, various approaches have been employed in the administration of heparin.

While the systemic administration of heparin can cause the implantation site to be subjected to an effective level of heparin, such level of heparin would necessarily also be present throughout the rest of the body which can lead to undesirable side effects such as bleeding. It has therefore been recognized that a regimen wherein the heparin is substantially constrained to the implantation site is far more desirable. An approach that has been devised to achieve such end requires the coating or impregnation of the stent itself with heparin. The heparin is thereby concentrated where it is most needed while its presence, and consequently its effect, throughout the rest of the body is minimized.

Disadvantages associated with heretofore known heparinized stents include, the limited shelf life of such devices, the fact the heparin is degraded when the stent is sterilized either by heat or by exposure to ethylene dioxide, the inability of the physician to alter the dosage that the patient is subjected to and the inability to replenish any heparin that may be lost while the device is deployed. Additionally, the cost of heretofore known heparinized stent devices has been very high as it necessarily includes the costs associated with the stringent regulatory requirements attendant a drug containing device.

The prior art has been unable to overcome these disadvantages and shortcomings and a new approach is needed to safely, effectively, and economically deliver heparin to an implantation site.

SUMMARY OF THE INVENTION

The present invention provides for the coating of an implantable endovascular device to facilitate the subsequent loading of heparin onto its surface. Such loading can be achieved in vitro just prior to implantation or preferably, in vivo after the device is in place. As a result, the device has a considerably longer shelf-life than heparin-containing devices, the need for special handling and sterilization procedures associated with heparin-containing devices is obviated, and the dosage of heparin can be readily tailored to an individual patient's needs including any adjustment that may be required after the device has been deployed. An additional advantage provided by such a device is that it is not subject to the stringent regulatory requirements associated with drug-containing devices.

More particularly, the present invention provides for the coating of stent surfaces with a material or combination of materials that are selected for their ability to adhere to the stent surface, to attract heparin and to form preferably an ionic bond therewith. The heparin is attracted by and attaches to functional groups incorporated in the coating which may include primary, secondary, and/or tertiary amines or other functionalities such as carboxyl groups.

The heparin-attracting coating may be applied so as to encapsulate the entire stent or alternatively, to cover only selected surfaces thereof. By limiting coverage to only the inner surface of the stent, i.e., the surface that is directly exposed to blood flow, a much higher level of heparin can be loaded onto the stent than would be safe if such level were in direct contact with the vessel wall. A toxic effect on the vessel wall is thereby avoided while the blood is exposed to a more effective concentration of heparin. Alternatively, it may be deemed sufficient to coat only the ends of the stent, i.e., where disturbance of flow is greatest and where thromboses are most likely to occur.

The coating may be applied by different processes such as by dipping, spraying or molding. The preferred method is by plasma deposition wherein a base layer, selected for its ability to adhere to the stent surface, is first deposited on the stent followed by the deposition of a top layer thereon that is selected for its ability to bond to the base layer and to avail the appropriate functional groups for bonding to the heparin.

These and other features and advantages of the present invention will become apparent from the following detailed description which, taken in conjunction with the accompanying drawings, illustrates by way of example the principles of the invention.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1

is a perspective view of an implantable stent.

FIG. 2

is a greatly enlarged, schematic, cross-sectional view of a portion of the stent of the present invention.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

A wide variety of different stent configurations have been devised to address various issues inherent in their use and function. Additionally, various materials have been employed in their construction including metals and polymers. Both the degree of turbulence caused by a particular stent configuration when subjected to blood flow as well as the material from which it is constructed affects the degree of thrombogenicity associated with a particular stent device. The present invention provides a coating for such stents to which heparin becomes attached and thus serves to reduce or eliminate thrombosis formation. Moreover, the stent's coating allows the heparin to be loaded thereon immediately before the implantation procedure or after the stent is in place.

Critical requirements for the coating of the present invention include that it adheres to the stent surface and that it has functional groups that attract heparin and to which heparin bonds. Functional groups that are known to have the requisite affinity for heparin include primary, secondary, and tertiary amines wherein primary amines are preferred due to their enhanced affinity. Alternatively, carboxyl groups may be used. The functional groups must include positively charged entities that serve to attract the negatively charged entities associated with the heparin. Such attraction facilitates the formation of an ionic bond.

The coating can be applied by different processes such as by dipping, spraying, molding or by plasma deposition. Plasma deposition is preferred and first requires the deposition of a base layer or primer that prepares the surface of the stent to receive the functionality group containing substance. In the preferred embodiment, a metallic stent is first plasma deposited with methane gas leaving a film on the surface of the stent wherein the methane molecules are oriented with the carbon against the stent and the hydrogen exposed. A top layer that includes the desired functionalities is then deposited on the base layer. Such second layer may be formed by the plasma deposition of ammonia gas to leave the primary amine functional groups extending from the stent surface. Other chemicals such as alkylamine, nitrile compounds or amine containing monomers can also be used to plasma deposit amine functionalities on the surface. In the event a mixture of primary, secondary, and tertiary amines is deposited by such methods it is preferred that the primary amine constitutes a greater percentage of the mixture due to its greater affinity for heparin. Alternatively, the deposition of carboxyl functional groups can be achieved by the plasma deposition of monomers like methyl methacrylate or acrylic acid.

The resulting coating thickness should be 0.001 inch or less while a thickness less than 1 micron is preferred. Although it may be desirable to have a uniform concentration of functional groups extending from the surface, it is not critical to the function of the coating. On the other hand, a concentration of at least 54 picamoles/stent must be achieved in order to ensure that heparin becomes attached at an effective level.

The coating may be applied to the entire stent or just to selected surfaces thereon.

FIG. 1

generally illustrates a stent

12

in its deployed state and serves to identify the vessel wall-facing surface

14

, the blood flow-facing surface

16

, its upstream edge

18

, and its downstream edge

20

. By coating only the surfaces facing the blood flow, a concentration of heparin can be loaded thereon that would be toxic to the vessel wall tissue if it were to be present on the surfaces in direct contact with the vessel wall. Alternatively, it may be sufficient to exclusively coat the upstream and/or downstream edges of the stent for a particular stent configuration implanted in a particular patient as thrombosis is most likely to occur at such interfaces due to turbulence induced by their presence in the blood flow.

After the coating process is completed, the coated stent is cleaned and sterilized and appropriately packaged for long-term storage. Due to the absence of any degradable drugs or substances on the stent, a fairly extended shelf-life can be expected.

The stent of the present invention can be used in two different ways. A first use calls for the stent to be implanted in the form in which it had been stored, without having heparin loaded thereon. Once in place, it is contacted with heparinized blood, either by an injection of heparin via a catheter extended to a position just upstream of the implantation site or by IV. As the heparin macromolecules

22

pass by the functional groups

24

in the coating

26

, the heparin is attracted thereto and becomes attached (FIG.

2

). Heparin that does not attach, quickly becomes diluted downstream of the implantation site to levels that do not adversely affect the patient. Subsequent heparin flow past the implantation site can cause more and more heparin molecules to be pulled from the blood flow until the stent coating is saturated. Once attached, heparin can inhibit coagulation by binding with anti-thrombin III and/or other factors of the coagulation cascade. Should a heparin molecule become detached, it is replaced by other heparin molecules still present in the blood flow. Alternatively, an additional dosage of heparin can be administered.

Alternatively, the physician may pre-treat the stent prior to implantation by flushing it with, for example, a heparinized saline solution. In this way, the physician can easily and precisely adjust the heparin level by controlling the concentration of the heparin in the saline solution and/or controlling the exposure time thereto. Once implanted, the heparin level can be increased or replenished by introducing heparin into the blood flow upstream of the implantation site as was described above. The heparin level is maintained on the stent until the natural healing processes cause the stent surfaces to be completely covered by tissue at which point thrombogenicity ceases to be of concern.

While a particular form of the invention has been illustrated and described, it will also be apparent to those skilled in the art that various modifications can be made without departing from the spirit and scope of the invention. Accordingly, it is not intended that the invention be limited except by the appended claims.

Claims

1. A device, comprising:a body that is implantable within a lumen of the vascular system, such lumen being defined by vessel walls and wherein said body has surfaces capable of contacting said vessel walls and surfaces incapable of contacting said vessel walls upon implantation; and a coating devoid of heparin exclusively deposited on surfaces of said body that are incapable of contacting said vessel walls wherein such coating is formed of material that adheres to said body and includes function groups to attract heparin and form a bond therewith when such material is exposed to a solution containing heparin whereby a toxic effect to the patient's vasculature is avoided.
2. The device of claim 1, wherein said functional groups of said coating deposited on surfaces of said body incapable of contacting said vessel walls attract heparin and form a bond when said material is exposed to a heparin-containing solution comprising heparinized blood.
3. The device of claim 1, wherein said functional groups of said coating deposited on surfaces of said body capable of contacting said vessel walls attract heparin and form a bond when said material is exposed to a heparin-containing solution comprising heparinized saline.
4. An endovascular stent, comprising:a support structure that is implantable within a patient's vasculature; a coating deposited on said support structure wherein such coating is formed of material that adheres to said stent structure and that includes functional groups to attract heparin and form an ionic bond therewith when such material is exposed to a solution containing heparin; and wherein said support structure is configured such that upon implantation in a blood vessel, such support structure has surfaces that face the vessel walls, surfaces that face the blood flow, and has an upstream edge and a downstream edge and wherein said coating is exclusively deposited on said surface facing said blood flow.
5. An endovascular stent, comprising:a support structure that is implantable within a patient's vasculature; a coating deposited on said support structure wherein such coating is formed of material that adheres to said stent structure and includes functional groups to attract heparin and form an ionic bond therewith when such material is exposed to a solution containing heparin; and wherein said support structure is configured such that upon implantation in a blood vessel, such support structure has surfaces that face the vessel walls, surfaces that face the blood flow, and has an upstream edge and a downstream edge and wherein said coating is exclusively deposited on said edges.
6. A device comprising:a body that is implantable within a lumen of the vascular system, such lumen being defined by vessel walls and wherein said body has surfaces capable of contacting said vessel walls and surfaces incapable of contacting said vessel walls upon implantation; and; a coating deposited exclusively on surfaces of said body that are incapable of contacting said vessel walls, wherein such coating is formed of material that adheres to said body and includes functional groups to attract heparin and form a bond therewith when such material is exposed to a solution containing heparin; and wherein said functional groups comprise a primary amine.
7. A device, comprising:a body that is implantable within a lumen of the vascular system, such lumen being defined by vessel walls and wherein said body has surfaces capable of contacting said vessel walls and surfaces incapable of contacting said vessel walls upon implantation; and; a coating deposited exclusively on surfaces of said body that are incapable of contacting said vessel walls, wherein such coating is formed of material that adheres to said body and includes functional groups to attract heparin and form a bond therewith when such material is exposed to a solution containing heparin; and wherein said functional groups comprise a secondary amine.
8. The device of claim 1, wherein said functional groups comprise a teriary amine.
9. The device of claim 1, wherein said functional groups comprise carboxyl groups.
10. The device of claim 1, wherein said coating comprises a base layer, wherein such base layer is selected for its ability to adhere to said body, and a top layer, wherein such top layer is selected for its ability to bond to said base layer and includes said functional groups for bonding with heparin.
11. The device of claim 10, wherein said base layer is hydrophobically attached to said body.
12. The device of claim 10, wherein said top layer is covalently bonded to said base layer.

US Referenced Citations (66)

Number	Name	Date	Kind
3288728	Gorham	Nov 1966	A
3839743	Schwarcz	Oct 1974	A
4164524	Ward et al.	Aug 1979	A
4346028	Griffith	Aug 1982	A
4633873	Dumican et al.	Jan 1987	A
4656083	Hoffman et al.	Apr 1987	A
4699611	Bowden	Oct 1987	A
4718907	Karwoski et al.	Jan 1988	A
4722335	Vilasi	Feb 1988	A
4723549	Wholey et al.	Feb 1988	A
4816339	Tu et al.	Mar 1989	A
4828561	Woodroof	May 1989	A
4865870	Hu et al.	Sep 1989	A
4877030	Beck et al.	Oct 1989	A
4879135	Greco et al.	Nov 1989	A
4943346	Mattelin	Jul 1990	A
4994298	Yasuda	Feb 1991	A
5047050	Arpesani	Sep 1991	A
5053048	Pinchuk	Oct 1991	A
5085629	Goldberg et al.	Feb 1992	A
5108755	Daniels et al.	Apr 1992	A
5116365	Hillstead	May 1992	A
5134192	Feijen et al.	Jul 1992	A
5156623	Hakamatsuka et al.	Oct 1992	A
5192311	King et al.	Mar 1993	A
5197977	Hoffman, Jr. et al.	Mar 1993	A
5222971	Willard et al.	Jun 1993	A
5226913	Pinchuk	Jul 1993	A
5234456	Silvestrini	Aug 1993	A
5234457	Andersen	Aug 1993	A
5236447	Kubo et al.	Aug 1993	A
5269802	Garber	Dec 1993	A
5279594	Jackson	Jan 1994	A
5282823	Schwartz et al.	Feb 1994	A
5282860	Matsuno et al.	Feb 1994	A
5289831	Bosley	Mar 1994	A
5290271	Jernberg	Mar 1994	A
5304200	Spaulding	Apr 1994	A
5306286	Stack et al.	Apr 1994	A
5314472	Fontaine	May 1994	A
5330500	Song	Jul 1994	A
5342348	Kaplan	Aug 1994	A
5342621	Eury	Aug 1994	A
5356433	Rowland et al.	Oct 1994	A
5360443	Barone et al.	Nov 1994	A
5364354	Walker et al.	Nov 1994	A
5370684	Vallana et al.	Dec 1994	A
5383927	DeGoicoechea et al.	Jan 1995	A
5389106	Tower	Feb 1995	A
5423849	Engelson et al.	Jun 1995	A
5455040	Marchant	Oct 1995	A
5464650	Berg et al.	Nov 1995	A
5562728	Lazarus et al.	Oct 1996	A
5571166	Dinh et al.	Nov 1996	A
5588962	Nicholas et al.	Dec 1996	A
5609629	Fearnot et al.	Mar 1997	A
5618298	Simon	Apr 1997	A
5624411	Tuch	Apr 1997	A
5628755	Heller et al.	May 1997	A
5628781	Williams et al.	May 1997	A
5637113	Tartaglia et al.	Jun 1997	A
5718726	Amon et al.	Feb 1998	A
5804318	Pinchuk et al.	Sep 1998	A
5824048	Tuch	Oct 1998	A
5997517	Whitbourne	Dec 1999	A
6120535	McDonald et al.	Sep 2000	A

Foreign Referenced Citations (29)

Number	Date	Country
2008312	Jul 1990	CA
2007648	Apr 1991	CA
1322628	Oct 1993	CA
1336319	Jul 1995	CA
1338303	May 1996	CA
0380 668	Apr 1989	EP
0 351 314	Jan 1990	EP
0517 075	Dec 1992	EP
0 540 290	May 1993	EP
0 565 251	Oct 1993	EP
A-0 604 022	Jan 1994	EP
A-0 578 998	Jun 1994	EP
A-0 621 017	Oct 1994	EP
0 649 637	Apr 1995	EP
0 701 802	Mar 1996	EP
0 716 836	Jun 1996	EP
0 832 618	Sep 1996	EP
0 756 853	Feb 1997	EP
SHO49-48336	Dec 1974	JP
SHO54-18317	Jul 1979	JP
SHO60-28504	Jul 1985	JP
HEI6-38851	May 1994	JP
HEI8-33718	Feb 1996	JP
HEI10-151190	Jun 1998	JP
WO 9117789	Nov 1991	WO
WO 9306792	Apr 1993	WO
WO 9511817	May 1995	WO
WO 9628115	Sep 1996	WO
WO 9710011	Mar 1997	WO

Non-Patent Literature Citations (65)

Entry
J. R. Hollahan et al., Attachment of Amino Groups to Polymer Surfaces by Radiofrequency Plasmas, Journal of Applied Polymer Science, vol. 13, pp. 807-816 (1969).
N. Inagaki et al., Hydrophilic Surface Modification of Polyethylene by No-Plasma Treatment, Adhesion Sci.Technol., vol. 4, No. 2, pp. 99-107 (1990).
Carl-Gustaf Gölander et al., RF-Plasma-Modified Polystyrene Surfaces for Studying Complement Activation, J. Biomater. Sci. Plymer Edn, vol. 4, No. 1, pp. 25-30 (1992).
Fabienne Poncin-Epaillard et al., Reactivity of a Polypropylene Surface Modified in a Nitrogen Plasma, Plasma Surface Modification of Polymers, pp. 167-180 (1994).
Thomas R. Gengenbach et al., Evolution of the Surface Composition and Topography of Perfluorinated Polymers Following Ammonia-Plasma Treatment, Plasma Surface Modification of Polymers, pp. 123-146 (1994).
U.S. patent application Ser. No. 08/233,046 filed Aug. 25, 1994.
Lambert, Thomas L. M.D., et al., Localized Arterial Wall Drug Delivery From a Polymer-Coated Removable Metallic Stent, Circulation, Eol. 90, No. 2 (Aug. 1994) pp. 1003-1011.
De Scheerder, Ivan K, et al., Biocompatibility of Polymer-Coated Oversized Stents Implanted in Normal Porcine Coronary Arteries, Atherosclerosis, vol. 114 (1995) pp. 105-114.
U.S. patent application Ser. No. 08/564,936 (FWC of 08/233,046) filed Apr. 28, 1995.
U.S. patent application Ser. No. 08/234,547 filed Aug. 1994.
U.S. patent application Ser. No. 08/559,931 (FWC of 08/234,547) filed Nov. 17, 1995.
U.S. patent application Ser. No. 08/156,268 filed Nov. 22, 1993.
Union Carbide Technology Letter, New Business Department—Parylene, Oct. 1973, No. 7 (8 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1973, No. 9 (23 pages).
Union Carbide, Technology Letter, May 1974, No. 11 (12 pages).
Union Carbide Technology Letter, Oct. 1975, No. 15 (13 pages).
Union Carbide, Electronic Materials, Parylene Products, Mar. 1976, No. 16 (4 pages).
Eskin, et al., Growth of Cultured Calf Aortic Smooth Muscle Cells on Cardiovascular Prosthetic Materials, J. Biomed. Mater. Res. vol. 10, pp 113-122 (1976).
Loeb, et al., Parylene as a Chronically Stable, Reproducible Microelectrode Insulator, IEEE Transactions on Biomedical Engineering, Mar. 1977, (pp. 121-128).
Union Carbide, Electronic Materials, Parylene Products, Aug. 1977, No. 18 (7 pages).
Union Carbide, Electronic Materials, Parylene Prodcuts, Oct. 1977, No. 1 Revision 2 (7 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 2 Revision 1 (9 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 3 (21 pages).
Union Carbide, Electronics Materials, Parylene Products, Oct. 1977, No. 4 (13 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 6 (12 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 7 Revision 1 (8 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 8, Edited (19 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 10 (50 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 11 (12 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 12, Revision 1 (6 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 13, Revision 1 (7 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 14, Revision 1 (11 pages).
Union Carbide, Electronic Materials, Parylene Products, Oct. 1977, No. 15, Revision 1 (8 pages).
Union Carbide, Electronics Materials, Parylene Products, Oct. 1977, No. 17, Revision 1 (11 pages).
ISEEE Transactions on Biomedical Engineering, vol. BME-27, No. 11, Nov. 1980 (5 pages).
Sadhir, et al., The Adhesion of Glow-Discharge Polymers, Silastic and Parylene to Implantable Platinum Electrodes: Results of Tensile Pull Tests After Exposure to Isotonic Sodium Chloride, Oct. 1981, vol. 2, Biomaterials (pp. 239-243).
Hahn, et al., Glow Discharge Polymers as Coatings for Implanted Devices, John M. Dlaton Research Center, University of Missouri-Columbia and the Graduate Center for Materials REsearch, 1981 (pp. 109-113).
Union Arbide, Electrode Materials, Parylene Products, Jan. 18, 1982, No. 5, Revision 4 (17 pages).
Hahn, et al., Biocompatibility of Glow-Discharge-Polymerized Films and Vacuum-Deposited Parylene, Journal of Applied Polymer Science: Applied Polymer Symposium 38, 55-64 (1984).
Casper, et al., Fiber-Reinforced Absorbable Compsite for Orthopedic Surgery, Polymeric Materials Science and Engineering, Proceedings of the ACS Division of Polymeric Materials: Science and Engineering, vol. 53, Fall Meeting 1985.
Kelly et al., Totally Resorbable High-Strength Composite Mateiral, Advances in Biomedical Polymers, Edited by Charles G. Gebelein (1987).
Yuen, et al., Tissue Response to Potential Neuroprosthetic Materials Implanted Subdurally, Biomaterials, Mar. 1987, vol. 8, (pp. 57-62).
Nichols, et al., Electrical Insulation of Implantable Devices by Composite Polymer Coatings, Dalton Research Center, University of Missouri, 1987.
Schmidt, et al., Long-Term Implants of Parylene-C Coated Microelectrodes, Medical & Biological Engineering & Computing, Jan. 1988 (pp. 96-101).
Olson, Parylene, a Biostable Coating for Medical Applications, for NOVA TRAN Parylene Coating Services (Jul. 25, 1988; Nov. 14, 1988).
Beach, et al., Xylylene Polymers, Encyclopedia of Polymer Science and Engineering, vol. 17, Second Edition, pp. 990-1025, 1989.
Muller, et al., Advances in Coronary Angioplasty: Endovascular stents, Coronary Artery Disease, Jul./Aug. 1990, vol. 1, No. 4.
Loh, et al., Plasma Enhanced Parylene Deposition, Antec, pp. 1099-1103, 1991.
Gebelein, et al., Biomedical and Dental Applications of Polymers, Polymer Science and Technology, vol. 14 (No. date)(pp. 143-161).
Wong, M.D., et al., An Update on Coronary Stents, Cardio, Feb. 1992.
The Parylene Press (A Publication of Specialty Coating Systems, Inc.), Winter 1992 (7 pages).
Charlson, et al., Temperature Selective Deposition of Parylene-C, IEEE Transactions on Biomedical Engineering, vol. 39, No. 2, Feb. 1992 (pp. 202-206).
Bull: Parylene Coating for Medical Applications, Medical Product Manufacturing News, Mar. 1993 (2 pages).
The Parylene Press (A Publication of Specialty Coating Systems, Inc.), Spring 1993 (6 pages).
The Parylene Press (A Publication of Specialty Coating Systems, Inc.), Summer 1993 (4 pages).
Information Regarding Parylene-C Coating for ACS Metal Stent, In-Home Memorandum from Ed Newton to Joe Callol, Mike Clayman, Dennis Houlsby and Joe Tartaglia, Oct. 15, 1993 attaching Parylene, a Biostable Coating for Medical Application by Roger Olson.
Moody: Vacuum Coating Ultrasonic Transducers, Sensors, Dec. 1993 (1 page).
Union Carbide A-174 Silane, Sales Brochure, Union Carbide Adhesion Promoters, Jan. 1968 (5 pages).
Parylene Conformal Coatings Speficiations and Properties, Sales Brochure, Union Carbide Specialty Coating Systems (12 pages).
Parylene Environmentally Compatible Conformal Coatings for Electronic Components Assemblies and Precision Parts, Brochure, Union Carbide Electronics Division (14 pages).
Parylene and Nova Tran™ Parylene Coating Services, for Unmatched Conformal Coating Performance, Brochure, Union Carbide Specialty Coating Systems (21 pages).
Repair and Recoating of Parylene Coated Printed Circuit Boards, Brochure, Union Carbide Specialty Coating Systems (15 pages).
Nova Tan™ Custom Coating Services, Parylene Conformal Coating, Brochure, Union Carbide (8 pages).
Parylene, a Biostable Coating for Medical Applications, Brochure, Union Carbide Specialty Coating Systems (6 pages).
Typical Parylene Properties, Printout, Para Tech Coating Company; Lab Top® Parylene Deposition System Model 3000, Sales Brochure, Para Tech Coating Company (7 pages).

Coated endovascular stent

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US Referenced Citations (66)

Foreign Referenced Citations (29)

Non-Patent Literature Citations (65)