CA2538392A1 - Medical devices - Google Patents
Medical devices Download PDFInfo
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- CA2538392A1 CA2538392A1 CA002538392A CA2538392A CA2538392A1 CA 2538392 A1 CA2538392 A1 CA 2538392A1 CA 002538392 A CA002538392 A CA 002538392A CA 2538392 A CA2538392 A CA 2538392A CA 2538392 A1 CA2538392 A1 CA 2538392A1
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- Prior art keywords
- metal
- acid solution
- therapeutic agent
- tubular member
- color
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- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Classifications
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61F—FILTERS IMPLANTABLE INTO BLOOD VESSELS; PROSTHESES; DEVICES PROVIDING PATENCY TO, OR PREVENTING COLLAPSING OF, TUBULAR STRUCTURES OF THE BODY, e.g. STENTS; ORTHOPAEDIC, NURSING OR CONTRACEPTIVE DEVICES; FOMENTATION; TREATMENT OR PROTECTION OF EYES OR EARS; BANDAGES, DRESSINGS OR ABSORBENT PADS; FIRST-AID KITS
- A61F2/00—Filters implantable into blood vessels; Prostheses, i.e. artificial substitutes or replacements for parts of the body; Appliances for connecting them with the body; Devices providing patency to, or preventing collapsing of, tubular structures of the body, e.g. stents
- A61F2/82—Devices providing patency to, or preventing collapsing of, tubular structures of the body, e.g. stents
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
- A61L31/02—Inorganic materials
- A61L31/022—Metals or alloys
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
- A61L31/08—Materials for coatings
- A61L31/10—Macromolecular materials
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
- A61L31/14—Materials characterised by their function or physical properties, e.g. injectable or lubricating compositions, shape-memory materials, surface modified materials
- A61L31/146—Porous materials, e.g. foams or sponges
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
- A61L31/14—Materials characterised by their function or physical properties, e.g. injectable or lubricating compositions, shape-memory materials, surface modified materials
- A61L31/148—Materials at least partially resorbable by the body
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L31/00—Materials for other surgical articles, e.g. stents, stent-grafts, shunts, surgical drapes, guide wires, materials for adhesion prevention, occluding devices, surgical gloves, tissue fixation devices
- A61L31/14—Materials characterised by their function or physical properties, e.g. injectable or lubricating compositions, shape-memory materials, surface modified materials
- A61L31/16—Biologically active materials, e.g. therapeutic substances
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61F—FILTERS IMPLANTABLE INTO BLOOD VESSELS; PROSTHESES; DEVICES PROVIDING PATENCY TO, OR PREVENTING COLLAPSING OF, TUBULAR STRUCTURES OF THE BODY, e.g. STENTS; ORTHOPAEDIC, NURSING OR CONTRACEPTIVE DEVICES; FOMENTATION; TREATMENT OR PROTECTION OF EYES OR EARS; BANDAGES, DRESSINGS OR ABSORBENT PADS; FIRST-AID KITS
- A61F2250/00—Special features of prostheses classified in groups A61F2/00 - A61F2/26 or A61F2/82 or A61F9/00 or A61F11/00 or subgroups thereof
- A61F2250/0058—Additional features; Implant or prostheses properties not otherwise provided for
- A61F2250/0067—Means for introducing or releasing pharmaceutical products into the body
- A61F2250/0068—Means for introducing or releasing pharmaceutical products into the body the pharmaceutical product being in a reservoir
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61F—FILTERS IMPLANTABLE INTO BLOOD VESSELS; PROSTHESES; DEVICES PROVIDING PATENCY TO, OR PREVENTING COLLAPSING OF, TUBULAR STRUCTURES OF THE BODY, e.g. STENTS; ORTHOPAEDIC, NURSING OR CONTRACEPTIVE DEVICES; FOMENTATION; TREATMENT OR PROTECTION OF EYES OR EARS; BANDAGES, DRESSINGS OR ABSORBENT PADS; FIRST-AID KITS
- A61F2250/00—Special features of prostheses classified in groups A61F2/00 - A61F2/26 or A61F2/82 or A61F9/00 or A61F11/00 or subgroups thereof
- A61F2250/0058—Additional features; Implant or prostheses properties not otherwise provided for
- A61F2250/0085—Identification means; Administration of patients
- A61F2250/0087—Identification means; Administration of patients colour-coded
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
- A61L2300/00—Biologically active materials used in bandages, wound dressings, absorbent pads or medical devices
-
- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y10—TECHNICAL SUBJECTS COVERED BY FORMER USPC
- Y10T—TECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
- Y10T428/00—Stock material or miscellaneous articles
- Y10T428/24—Structurally defined web or sheet [e.g., overall dimension, etc.]
- Y10T428/24802—Discontinuous or differential coating, impregnation or bond [e.g., artwork, printing, retouched photograph, etc.]
Abstract
Medical devices, particularly stents, suitable for drug delivery and including a porous structure and/or colors are disclosed.
Description
Medical Devices TECHNICAL FIELD
This invention relates to medical devices, such as, for example, endoprostheses.
BACKGROUND
o The body includes various passageways such as arteries, other blood vessels, and other body lumens. For various treatments and diagnostic techniques, it is often desirable to deliver a medical device into these lumens. For example, these passageways sometimes become occluded or weakened. The passageways can be occluded by e.g. a tumor, restricted by plaque, or weakened by an aneurysm.
When ~ 5 this occurs, the passageway can be reopened or reinforced, or even replaced, with a medical endoprosthesis.
An endoprosthesis is typically a tubular member that is placed in a lumen in the body. Examples of endoprostheses include stems and covered stems, sometimes called "stmt-grafts". An endoprosthesis can be delivered inside the body by a 2o catheter that supports the endoprosthesis in a compacted or reduced-size form as the endoprosthesis is transported to a desired site. Upon reaching the site, the endoprosthesis is expanded, for example, so that it can contact the walls of the lumen.
The expansion mechanism may include forcing the endoprosthesis to expand radially.
For example, the expansion mechazusm can include the catheter carrying a balloon, 25 which carnes the endoprosthesis. The balloon can be inflated to deform and to fix the expanded endoprosthesis at a predetermined position in contact with the lumen wall.
The balloon can then be deflated, and the catheter removed.
In another delivery technique, the endoprosthesis is self expanding. For example, the endoprosthesis can be formed of an elastic material that can be 3o reversibly compacted and expanded. During introduction into the body, the endoprosthesis is restrained in a compacted condition. Upon reaching the desired implantation site, the restraint is removed, for example, by retracting a restraining device such as an outer sheath, enabling the endoprosthesis to self expand by its own internal elastic restoring force. Another self expansion technique uses shape memory metals which can "remember" a particular geometric configuration, e.g. an expanded condition, upon exposure to a trigger, such as an increase in temperature.
SUMMARY
In one aspect, the invention features a stmt device having a generally tubular member. The generally tubular member includes a porous structure including an oxide of titanium, niobium, or tantalum, or an alloy thereof. The porous structure includes hollow post-shaped elements.
In another aspect, the invention features a stmt device having a generally tubular member. The member includes a porous structure of hollow post-shaped elements.
In another aspect, the invention features a method of making a stmt. The method includes providing a metal, exposing the metal to an acid solution such that the acid solution forms a meniscus on the metal, connecting the metal as an anode in an electrical circuit in the acid solution, and applying a voltage to the circuit. The metal is incorporated in a stmt.
2o In another aspect, the invention features a method of making a stmt, the method including providing a metal, exposing the metal to an acid solution, and controlling the oxygen content of the acid solution. The method also includes connecting the metal as an anode in an electrical circuit in the acid solution, and applying a voltage to the circuit. The metal is incorporated in a stmt.
In another aspect, the invention features a family of medical devices.
Members of the medical devices include an oxide providing a different color or color pattern (e.g., indicative of usage).
In another aspect, the invention features a medical device including an oxide providing a color or color pattern indicative of manufacturing information (e.g., a lot, so date, or manufacturer identification).
Embodiments can include one or more of the following features. The porous structure can be of an oxide of titanium. In some embodiments, the porous structure is on an outer surface of the generally tubular member. The porous structure can include a polymer that can be, e.g., a coating over the porous structure. In some cases, the coating is a diffusion or protective layer. The coating can be biodegradable.
This invention relates to medical devices, such as, for example, endoprostheses.
BACKGROUND
o The body includes various passageways such as arteries, other blood vessels, and other body lumens. For various treatments and diagnostic techniques, it is often desirable to deliver a medical device into these lumens. For example, these passageways sometimes become occluded or weakened. The passageways can be occluded by e.g. a tumor, restricted by plaque, or weakened by an aneurysm.
When ~ 5 this occurs, the passageway can be reopened or reinforced, or even replaced, with a medical endoprosthesis.
An endoprosthesis is typically a tubular member that is placed in a lumen in the body. Examples of endoprostheses include stems and covered stems, sometimes called "stmt-grafts". An endoprosthesis can be delivered inside the body by a 2o catheter that supports the endoprosthesis in a compacted or reduced-size form as the endoprosthesis is transported to a desired site. Upon reaching the site, the endoprosthesis is expanded, for example, so that it can contact the walls of the lumen.
The expansion mechanism may include forcing the endoprosthesis to expand radially.
For example, the expansion mechazusm can include the catheter carrying a balloon, 25 which carnes the endoprosthesis. The balloon can be inflated to deform and to fix the expanded endoprosthesis at a predetermined position in contact with the lumen wall.
The balloon can then be deflated, and the catheter removed.
In another delivery technique, the endoprosthesis is self expanding. For example, the endoprosthesis can be formed of an elastic material that can be 3o reversibly compacted and expanded. During introduction into the body, the endoprosthesis is restrained in a compacted condition. Upon reaching the desired implantation site, the restraint is removed, for example, by retracting a restraining device such as an outer sheath, enabling the endoprosthesis to self expand by its own internal elastic restoring force. Another self expansion technique uses shape memory metals which can "remember" a particular geometric configuration, e.g. an expanded condition, upon exposure to a trigger, such as an increase in temperature.
SUMMARY
In one aspect, the invention features a stmt device having a generally tubular member. The generally tubular member includes a porous structure including an oxide of titanium, niobium, or tantalum, or an alloy thereof. The porous structure includes hollow post-shaped elements.
In another aspect, the invention features a stmt device having a generally tubular member. The member includes a porous structure of hollow post-shaped elements.
In another aspect, the invention features a method of making a stmt. The method includes providing a metal, exposing the metal to an acid solution such that the acid solution forms a meniscus on the metal, connecting the metal as an anode in an electrical circuit in the acid solution, and applying a voltage to the circuit. The metal is incorporated in a stmt.
2o In another aspect, the invention features a method of making a stmt, the method including providing a metal, exposing the metal to an acid solution, and controlling the oxygen content of the acid solution. The method also includes connecting the metal as an anode in an electrical circuit in the acid solution, and applying a voltage to the circuit. The metal is incorporated in a stmt.
In another aspect, the invention features a family of medical devices.
Members of the medical devices include an oxide providing a different color or color pattern (e.g., indicative of usage).
In another aspect, the invention features a medical device including an oxide providing a color or color pattern indicative of manufacturing information (e.g., a lot, so date, or manufacturer identification).
Embodiments can include one or more of the following features. The porous structure can be of an oxide of titanium. In some embodiments, the porous structure is on an outer surface of the generally tubular member. The porous structure can include a polymer that can be, e.g., a coating over the porous structure. In some cases, the coating is a diffusion or protective layer. The coating can be biodegradable.
The polymer can include a therapeutic agent. In certain embodiments, the porous structure includes a colorant.
In some embodiments, the member includes a therapeutic agent. The therapeutic agent can be an antithrombogenic, antioxidant, anti-inflammatory, antiproliferative, antibiotic, drug, cell, or genetic material.
In some embodiments, the generally tubular member includes (e.g., a layer ofJ
titanium, niobium, tantalum, or an alloy thereof. The layer can have a thickness between about 50 nm and about 500 nrn. In some cases, the porous structure is over the layer. The titanium, niobium, tantalum, or alloy thereof can be a layer on a different metal. The different metal can be about 90% or more of the thickness of the ~ 5 tubular member. In certain embodiments, the generally tubular member includes stainless steel, nitinol, or a cobalt-based alloy (e.g., Elgiloy).
The post-shaped elements can include a porous metal oxide, e.g., on the surface of the generally tubular member. In some embodiments, the porous metal oxide has a thickness between about SO nm and about 500 nm and/or pore diameters 2o between about 20 nm and about 200 nrn. The post-shaped elements can have a post height of about 100 nm to about 200 nrn. The post-shaped elements can have pore diameters of about 20 nm to about 200 nm (e.g., about 70 nm to about 100 nm).
In certain embodiments, the device has a color corresponding to light having a wavelength between about 370 nm and about 750 run (e.g., a wavelength of about 25 nm, about 470 nm, about 530 nm, about 580 nm, about 620 nm, or about 700 ritn).
In some cases, the meniscus is formed sequentially on different portions of the metal. The acid solution can be a hydrofluoric acid solution (e.g., a 1.5% (by weight) ,hydrofluoric acid solution). The voltage can be about 5 V to about 100 V In some embodiments, the metal has a thickness between about 200 nm and about 400 nm.
3o In certain embodiments, the method includes applying a therapeutic agent and/or diffusion layer to the stmt. The method can include controlling the oxygen content by bubbling gas (e.g., including oxygen) through the acid solution.
Embodiments may include one or more of the following advantages. A
morphology of hollow post-shaped elements can be formed on a medical device by, 35 e.g. anodization, to provide desired characteristics. For example, a porous structure on the surface of a medical device, such as a stmt, can be a reservoir for a therapeutic material. The geometry of the porous structure, i.e. size and spacing of post-shaped elements, can be selected to, e.g., affect the rate of drug release. In addition, anodization can result in a relatively thick oxidation of a metal. The strength of the metal oxide formed by anodization can be comparable to, or even greater than, the strength of the metal. As a result, a porous oxide structure can be formed on metal body generally without substantially sacrificing the strength of the metal body on which the porous oxide structure is formed, or without impeding the function of the medical device. The robust, durable nature of the porous metal oxide structure protects it from damage during handling (e.g., during crimping, sterilizing, packaging). Furthermore, the durability of the porous metal oxide structure makes it ~ 5 resistant to damage from abrasion during assembly onto a catheter and delivery into the body, such that the porous structure can be relatively thin and the overall profile of the medical device is kept small. An anodized porous metal oxide can be more corrosion-resistant than the metal in its non-anodized state. A robust, porous metal oxide reservoir layer can reduce the need for, or the thickness of, drug protecting, 2o carrying, or metering layers of polymers. To the extent a polymer coating is desirable, the surface morphology increases surface area and provides for improved bonding between the coating and the surface. The morphology can also be selected to affect the apparent color of the medical device by optical reflectance and interference phenomena. For example, a family of medical devices having, e.g., different sizes, 2s therapeutic agents, or other features can be color-coded by varying the surface morphology. Anodization is effective to vary surface morphologies of metals that have desirable characteristics such as biocompatibility, radiopacity, and MRI
visibility. Particularly advantageous porous structures can be formed in titanium, niobium, or tantalum, and alloys including these metals, which can be used to make a 3o medical device, or which can be coated on another material (metal, ceramic, polymer) from which the medical device, or a component of the medical device, is made.
A
desired morphology can also reduce thrombosis by surface roughness, surface charge, and/or metal ion release.
Still further aspects, features, and advantages follow.
DESCRIPTION OF DRAWINGS
The file of this patent contains at least one drawing executed in color.
Copies of this patent with color drawings will be provided by the U.S. Patent and Trademark Office upon request and payment of the necessary fee.
FIGS. lA and 1B are perspective views of a stmt in the compressed and expanded condition, respectively.
FIGS. 2A and 2B are greatly enlarged cross sections through the side wall of a stmt, while FIG 2C is a top view of a portion of the stmt side wall shown in FIGS.
2A and 2B.
FIG 3A is a schematic of an anodization apparatus.
~ 5 FIG 3B is a front view of a stmt in the anodization apparatus of FIG 3A.
FIGS. 4A-4E are schematics of a surface treatment process.
FIGS. SA-SC illustrate delivery of a self expanding stmt.
FIGS. 6A-6C illustrate delivery of a balloon expandable stmt.
FIG 7A is a color photograph of a surface morphology.
2o FIG 7A-1 is a labeled version of the color photograph of FIG 7A.
FIG 7B is a field emission SEM image of a surface morphology.
FIG 7C is a field emission SEM image of a surface morphology FIG. 7D is a color photograph of a stmt (at 2x magnification).
FIG. 7D-1 is a labeled version of the color photograph of FIG 7D.
Structure Referring to FIGS. 1A and 1B, a stmt 10 includes a metal body 12 in the shape of a tube. The metal body includes aperture regions 14 provided in a pattern to facilitate stmt functions, such as radial expansion, and lateral flexibility.
Refernng 3o particularly to FIG lA, for delivery into the body, the stmt 10 is provided or maintained in a relatively small diameter condition corresponding to a diameter D~.
Referring to FIG. 1B, upon placement at the treatment site, the stmt 10 is expanded to a larger diameter, DeXp, so that the stmt is in contact with the lumen wall.
The stmt may be expanded by a mechanical expander, such as an inflatable balloon, or it may 3s be self expanding. The metal body of the stmt may be formed by a generally continuous sheet or by filaments that are wrapped, braided, knitted or otherwise configured to generally define a stmt. A suitable stmt design is the Express stmt, available from Boston Scientific, Natick, Mass. Balloon expandable and self expanding stems are further discussed in Heath, U.S. 5,725,570, the entire contents of which are incorporated herein by reference.
1 o Referring to FIGS. 2A and 2B, greatly expanded cross-sections through the side wall of a stmt, the stmt side wall is composed of a base material 20, an intermediate layer 22, and a porous layer 24. The porous layer 24 has a morphology characterized by hollow post-shaped elements 26. The hollow post-shaped elements 26 define internal volumes 27. Between post-shaped elements 26 are void regions 28.
~ 5 Refernng particularly to FIG 2A, the internal volumes 27 and void regions 28 contain a therapeutic agent 30. A protective or diffusion layer 32 is provided over and within the surface openings of the porous structure. Suitable protective layers include bioerodible polymers which protect the therapeutic agent from exposure to body fluids for a time period based on the thickness and erosion rate of the polymer.
2o Suitable diffusion layers include porous polymers that control the rate of diffusion from the reservoir. In embodiments, a therapeutic agent in the reservoir can be combined in a matrix of erodible polymer.
Referring particularly to FIGS. 2B and 2C, the morphology of the porous layer 24 can be selected to enhance therapeutic agent delivery or other characteristics. For 25 example, the porous morphology can be characterized by the internal volume of the hollow post-shaped elements, the voids between hollow post-shaped elements, and/or the density of the post-shaped elements, which affect the amount of therapeutic agent that can be delivered. The inner diameter or aspect ratio of the post-shaped elements and/or the size of the voids can be varied, which affects the diffusion rate from the 3o reservoir. Pores of different sizes can exhibit different light interference and reflection patterns, thereby resulting in different natural colors.
A hollow post-shaped morphology can be characterized by a thickness Tn.,, height Hp, and a spacing Sp between post-shaped elements. In embodiments, height Hp is about 100 nm to about 200 nm, and spacing Sp is about 1 nm to about 200 nm 35 (e.g., a typical spacing is about 10 nm to about 180 nm). As shown in FIG
2C, post shaped elements 26 have an outer diameter OD and an inner diameter ID. Outer diameter OD is about 20 nm to about 250 run. Inner diameter m is about 5 nrn to about 200 nm (e.g., about 70 nm to about 100 nm). The wall thickness of the tube-shaped elements, measured at the top of the elements, is, for example, about 5 nm to about 50 nm.
In embodiments, the porous layer 24 has a post-shaped element density of about 10 to about 300 post-shaped elements per square micron. In embodiments, the post-shaped element density is different in different parts of the porous layer. The percentage of open area on the layer (i.e., the space on which there are no post-shaped elements) can be about 50% to about 99%. In embodiments, a porous layer has a certain color or colors. For example, an anodized titanium surface can appear to be a specific color because of the size of its pores, and their light reflection and interference patterns. In embodiments, a morphology defined by an array of post-shaped elements acts as a grating that preferentially reflects light of a particular color.
In other embodiments, an anodized surface can vary color by thin film effects, e.g., when the surface is a continuous oxidized layer, rather than discrete post-shaped 2o elements. The porous layer may produce a color corresponding to light having a wavelength between about 370 nm and about 750 nm. The color of the porous layer can, for example, correspond to light having a wavelength of about 420 nm, about 470 nm, about 530 nm, about 580 nm, about 620 nm, or about 700 nm. In other embodiments, the color can be in the infrared or ultraviolet range. Coloring agents such as dyes can be added into the porous layer. A sealing layer (e.g., a polymer) can be formed over the porous layer to protect the coloring agent. Alternatively, the pores can be sealed by treating the porous layer with boiling water. The color of the porous layer can be used to indicate the type of therapeutic agent in a stmt, for example. The color can indicate the specific dose of therapeutic agent or its release rate.
In 3o embodiments, the color can be an indication of the specific purpose for the stmt (e.g., a coronary stmt). Different portions of a stmt can have different colors. The colors can be provided in a pattern to indicate, e.g., manufacturing information (e.g., manufacturing lot or date, and/or manufacturer's logo), or usage indication.
The porous layer, intermediate layer and stmt body can be made of metal or metal oxide. The metals or metal oxides of the layers can be the same or different.
Suitable metals include, e.g., titanium, tantalum, niobium, and aluminum, in substantially pure elemental form or in alloys. In particular embodiments, the stmt body can be stainless steel or nitinol. Titanium, niobium, and tantalum are particularly desirable because of their high biocompatibility Tantalum and niobium are particularly desirable for their radiopacity and MRI visibility In a particular embodiment, the stmt body is made of stainless steel, nitinol, or another metal with desirable strength and flexibility characteristics, the intermediate layer is non-porous titanium, tantalum, or niobium, and the porous layer is oxidized titanium, tantalum or niobium. The base metal provides most of the thickness of the stmt wall, e.g., about 90% or more. In some embodiments, the stmt body is porous but a surface layer is nonporous. In some cases, the stmt body itself is made of an anodizable metal (e.g., titanium, tantalum, niobium, or alloys thereof), and is treated as described with reference to FIGS. 3A and 3B, infra.
Manufacture Referring to FIGS. 3A and 3B, the hollow post-shaped porous morphology can 2o be formed by anodization. In anodization, a work piece such as a stmt 40 is placed in a chemical bath 42 and connected as the anode of an electrical circuit 44 to induce surface oxidation. The stmt can, for example, be oriented horizontally or vertically, and then dipped into the chemical bath. The cathode 46 of the circuit can be, e.g., titanium or graphite. In embodiments, several (e.g., three, four, five) cathodes 46 can surround stmt 40 to enhance current distribution across the surface of stmt 40.
Referring particularly to FIG 3B, the process parameters, such as exposure time to the chemical bath and oxygen consumptionaeration, can be controlled to effect a desirable hollow post-shaped morphology by anodizing at a meniscus.
The stmt 40 is partially immersed in the chemical bath 42. At the interface of the bath and the atmosphere, a meniscus 50 forms on the surface of the stmt. The exposure time of a portion of the stmt to the meniscus can be varied by moving the stmt relative to the bath, e.g., by rotating the stmt about its axis, while anodization is conducted. As illustrated in the examples below, anodization at the meniscus can be used to form well-defined morphologies of hollow post-shaped elements on metals such as titanium.
The depth, diameter, and spacing of the post-shaped elements can be controlled by controlling process parameters such as the process time, exposure depth, and oxygen consumption/aeration in the chemical bath, the composition of the chemical bath, circuit voltage, process temperature, and the metal undergoing treatment. If low acid concentrations and temperatures are used, then the resulting anodized surface may be less porous and harder than it is if higher temperatures and acid concentrations are used. Higher temperatures, higher acid concentrations, and longer anodization time periods can produce more porous and, in some cases, softer, coatings. The chemical bath includes an acid solution. Particular acids include strong acids such as hydrogen halides, e.g., HF or HCl, and phosphoric and sulfuric acids ~ 5 and mixtures thereof.
The circuit voltage can influence the size of the openings of the hollow post-shaped elements. For example, higher voltages yield larger openings. The circuit voltage is typically in the range of about 5 V to about 100 V, e.g., about 20 V to about 80 V The temperature for the anodization process can be equal to or greater than 2o about 10°C (e.g., between about 10°C and about 70°C, between about 20°C and about 60°C). In a particular example, the chemical bath can be an acid solution, such as a hydrofluoric acid solution (e.g., a 1.5% by weight hydrofluoric acid solution), a phosphoric acid solution (e.g., a 20% by volume phosphoric acid solution), or a sulfuric acid and phosphoric acid solution (e.g., a 10% by volume sulfuric acid and 2s 80% by volume phosphoric acid solution). The circuit voltage can be, e.g., between about 5 V and about 100 V (e.g., about 20 V or about 80 V). For example, the temperature for the anodization process can be about 25°C. Exposure time to the chemical bath can be less than about one minute (e.g., between about five seconds and about ten seconds).
3o In the embodiments described above, anodization is carried out at the meniscus to form an anodized surface of post-like structures. The oxygen level available to the anodized region can also be varied using other techniques (e.g., oxygen or air can be bubbled through the chemical bath). In embodiments, an entire surface to be anodized (e.g., a stmt) can be immersed in the chemical bath, rather than 35 being anodized at the meniscus.
Refernng to FIGS. 4A-4E, a stent-forming process is illustrated. In FIG 4A, a base material 60 is provided. The base material may be a metal, such as stainless steel, that forms the body of the stmt. The thickness of the body is typically about 0.005 mm or more, e.g., about 0.05 mm to about 0.3 mm. An anodizable metal is provided as a surface layer 62 on the stmt. The surface layer can be provided by techniques including physical vapor deposition, chemical vapor deposition, spraying, electroplating, dipping, or combinations of these processes. The surface layer preferably is provided by physical vapor deposition. The deposited layer is typically near the full density of the metal, e.g., between about 90% and about 100%
(e.g., about 99%) the density of the full metal. The deposited layer does not exhibit ~5 significant or regular porosity. In embodiments, the thickness of the deposited layer is typically in the range of about 10% or less of the thickness of the stmt body.
In embodiments, the thickness of the layer is about 0.1 micron to about 1.0 micron. The layer can be provided on just the exterior wall surface of the stmt, just the interior surface, or both the interior and exterior surfaces. The layer can completely cover the 2o stmt surface or just portions of the surface.
Referring to FIG 4B, the surface layer 62 is anodized. Anodization oxidizes the surface layer, thereby creating porous layer 64 having a morphology of hollow post-shaped elements. For example, if the surface layer is titanium, then anodization creates a titanium oxide layer.
25 Refernng to FIG 4C, a greatly enlarged cross-sectional view of FIG 4B, the anodization process creates a porous layer 64 that exhibits a desired porosity. Porous layer 64 has post-shaped elements 68 defining internal volumes 70. Post-shaped elements 68 are separated by void regions 72. Porous layer 64 can exhibit enhanced surface toughness relative to the material from which it is formed. The porous layer 3o can be provided over the entire stmt or over portions of the stmt, e.g., the exterior surface.
Referring to FIG 4D, a material such as a therapeutic agent can be provided into the porous structure by, for example, dipping, spray coating or the like.
The therapeutic agent can be provided into the volumes and void regions defined by the s5 post-shaped elements. In FIG 4D, a therapeutic agent 74 has been delivered into both the internal volumes of the post-shaped elements 70 and the void regions 72.
to Referring to FIG 4E, the porous layer 64 can be coated with a protective or diffusion layer 80. In some cases, the protective layer also is a diffusion layer. The protective and/or diffusion layer can be within each pore or can cover the entire stmt.
The protective layer can be a biodegradable material that protects and retains the therapeutic agent in the porous structure prior to delivery into the body.
For 1o example, the protective layer can be a polymer, e.g.
polytetrafluoroethylene (available from DuPont under the tradename Teflon'). The thickness of the protective layer can be between about 0.1 ,um and about 10 ,um. The protective layer can be an erodible polymer. Suitable erodible polymers include water soluble polymers such as polyvinyl alcohol (e.g., that has not been cross-linked), hydrogels (e.g., polyacrylic ~5 acid, haluronic acid, gelatin, carboxymethyl cellulose), polyethylene glycols (PEG), chitosan, and polyesters (e.g., polycaprolactones).
The diffusion layer controls the release of the therapeutic agent out of the pores. The diffusion layer can be biodegradable. Alternatively or additionally, the diffusion layer can be a polymer. Polymers may be, for example, homopolymers or 2o copolymers, crosslinked or uncrosslinked, linear or branched, natural or synthetic, thermoplastic or thermosetting. Polymers include the following: polycarboxylic acid polymers and copolymers including polyacrylic acids; acetal polymers and copolymers; acrylate and methacrylate polymers and copolymers (e.g., n-butyl methacrylate); cellulosic polymers and copolymers, including cellulose acetates, 25 cellulose nitrates, cellulose propionates, cellulose acetate butyrates, cellophanes, rayons, rayon triacetates, and cellulose ethers such as caxboxymethyl celluloses and hydoxyalkyl celluloses; polyoxymethylene polymers and copolymers; polyimide polymers and copolymers such as polyether block imides, polyamidimides, polyesterimides, and polyetherimides; polysulfone polymers and copolymers 3o including polyarylsulfones and polyethersulfones; polyamide polymers and copolymers including nylon 6,6, polycaprolactams and polyacrylamides; resins including alkyd resins, phenolic resins, urea resins, melamine resins, epoxy resins, allyl resins and epoxide resins; polycarbonates; polyacrylonitriles;
polyvinylpyrrolidones (cross-linked and otherwise); polymers and copolymers of 35 vinyl monomers including polyvinyl alcohols, polyvinyl halides such as polyvinyl chlorides, ethylene-vinylacetate copolymers (EVA), polyvinylidene chlorides, polyvinyl ethers such as polyvinyl methyl ethers, styrene polymers and copolymers such as polystyrenes, styrene-malefic anhydride copolymers, styrene-butadiene copolymers, styrene-ethylene-butylene copolymers (e.g., a polystyrene-polyethylene/butylene-polystyrene (SEES) copolymer, available as Kraton~ G
series polymers), acrylonitrile-styrene copolymers, acrylonitrile-butadiene-styrene copolymers, styrene-butadiene copolymers and styrene-isobutylene copolymers (e.g., polyisobutylene-polystyrene block copolymers such as SIBS, see, e.g., U.S.
Patent No. 6,545,097), polyvinyl ketones, polyvinylcarbazoles, and polyvinyl esters such as polyvinyl acetates; polybenzimidazoles; ionomers; polyalkyl oxide polymers and copolymers including polyethylene oxides (PEO); glycosaminoglycans; polyesters ~ 5 including polyethylene terephthalates and aliphatic polyesters such as polymers and copolymers of lactide (which includes lactic acid as well as d-,1- and meso lactide), epsilon-caprolactone, glycolide (including glycolic acid), hydroxybutyrate, hydroxyvalerate, para-dioxanone, trimethylene carbonate (and its alkyl derivatives), 1,4-dioxepan-2-one, 1,5-dioxepan-~-one, and 6,6-dimethyl-1,4-dioxan-2-one (a 2o copolymer of polylactic acid and polycaprolactone is one specific example);
polyether polymers and copolymers including polyarylethers such as polyphenylene ethers, polyether ketones, polyether ether ketones; polyphenylene sulfides;
polyisocyanates;
polyolefin polymers and copolymers, including polyalkylenes such as polypropylenes, polyethylenes (low and high density, low and high molecular weight), polybutylenes 25 (such as polybut-1-ene and polyisobutylene), poly-4-methyl-pen-1-enes, ethylene-alpha-olefin copolymers, ethylene-methyl methacrylate copolymers and ethylene-vinyl acetate copolymers; fluorinated polymers and copolymers, including polytetrafluoroethylenes (PTFE), poly(tetrafluoroethylene-co-hexafluoropropene) (FEP), modified ethylene-tetrafluoroethylene copolymers (ETFE), and polyvinylidene 3o fluorides (PVDF); silicone polymers and copolymers; polyurethanes; p-xylylene polymers; polyiminocarbonates; copoly(ether-esters)such as polyethylene oxide-polylactic acid copolymers; polyphosphazines; polyalkylene oxalates;
polyoxaamides and polyoxaesters (including those containing amines and/or amido groups);
polyorthoesters; biopolymers, such as polypeptides, proteins, polysaccharides and 35 fatty acids (and esters thereof), including fibrin, fibrinogen, collagen, elastin, chitosan, s gelatin, starch, glycosaminoglycans such as hyaluronic acid; as well as blends and additional copolymers of the above.
Examples of polymers include block copolymers comprising at least one A
block and at least one B block. The A blocks are preferably soft elastomeric blocks, which are based upon one or more polyolefins, or other polymer with a glass transition temperature at or below room temperature. For example, the A blocks can be polyolefinic blocks having alternating quaternary and secondary carbons of the general formulation: -(CRR'-CH2)n-, where R and R' are, independently, linear or branched aliphatic groups such as methyl, ethyl, propyl, isopropyl, butyl, isobutyl and so forth, or represent cyclic aliphatic groups such as cyclohexane, cyclopentane, and ~ 5 the like, either with or without pendant groups. Preferred polyolefinic blocks include HOC
polymeric blocks of isobutylene, cH3, (i.e., polymers where R and R' are methyl groups). Other examples of A blocks include silicone rubber blocks and acrylate rubber blocks.
The B blocks are preferably hard thermoplastic blocks with glass transition 2o temperatures significantly higher than the elastomeric A blocks which, when combined with the soft A blocks, are capable of, inter alia, altering or adjusting the hardness of the resulting copolymer to achieve a desired combination of qualities.
Examples of B blocks include polymers of methacrylates or polymers of vinyl aromatics. More specific examples of B blocks include blocks that are (a) formed ~CHZ
25 from monomers of styrene , styrene denvatives (e.g., a methylstyrene, ring-alkylated styrenes or ring-halogenated styrenes or other substituted styrenes where one or more substituents are present on the aromatic ring) or mixtures of the same, collectively referred to herein as "styrenic blocks"
or "polystyrenic blocks" or are (b) formed from monomers of methylmethacrylate, 3o ethylmethacrylate, hydroxyethyl methacrylate or mixtures of the same.
The block copolymers are provided in a variety of architectures, including cyclic, linear, and branched architectures. Branched architectures include star-shaped architectures (e.g., architectures in which three or more chains emanate from a single region), comb architectures (e.g., copolymers having a main chain and a plurality of side chains), and dendritic architectures (including arborescent or hyperbranched copolymers).
Some specific examples of such block copolymers include the following: (a) BA (linear diblock), (b) BAB or ABA (linear triblock), (c) B(AB)" or A(BA)"
(linear 1o alternating block), or (d) X-(AB)" or X-(BA)" (includes diblock, triblock and other radial block copolymers), where n is a positive whole number and X is a starting seed, or initiator, molecule. One specific group of polymers have X-(AB) n structures, which are frequently referred to as diblock copolymers and triblock copolymers where n=1 and n=2, respectively (this terminology disregards the presence of the ~5 starting seed molecule, for example, treating A-X-A as a single A block, with the triblock therefore denoted as BAB). A particularly beneficial polymer from this group is polystyrene-polyisobutylene-polystyrene triblock copolymer (SIBS).
Where n=3 or more, these structures are commonly referred to as star-shaped block copolymers. Other examples of block polymers include branched block copolymers 2o such as dendritic block copolymers, wherein at least one of the A and B
blocks is branched, for instance, where the A blocks are branched and are capped by the B
blocks.
The thickness of the diffusion layer can be, e.g., between about 0.1 ~.m and about 10 ,um.
25 ~ The porous layer can be partially sealed to control drug diffusion. A
partial sealant layer can be added to the porous layer, or the porous layer can be partially sealed by treating the porous layer with boiling water. During such treatment, the oxide is hydrated, causing it to swell and thereby start to close in the pores. The parameters of the sealing process can be adjusted to achieve a desired amount of 3o sealing.
The protective layer, diffusion layer, or sealant layer can include a therapeutic agent instead of or in addition to a therapeutic agent in the porous layer.
The therapeutic agent in these layers can be the same as or different from the therapeutic agent in the porous layer. For example, the protective, diffusion, or sealant layer can 35 include an antithrombogenic agent, which is released quickly during delivery and deployment, while the porous layer contains an anti-inflammatory, which is released more slowly at the site. The therapeutic agent provided in the volumes and voids of the porous layer can be dissolved in a Garner, such as an erodible polymer or a diffusion-controlling polymer.
The term "therapeutic agent" includes one or more "therapeutic agents" or "drugs". The terms "therapeutic agents" and "drugs" are used interchangeably and include pharmaceutically active compounds, nucleic acids with and without carrier vectors such as lipids, compacting agents (such as histones), virus (such as adenovirus, adeno-associated virus, retrovirus, lentivirus and a-virus), polymers, antibiotics, hyaluronic acid, gene therapies, proteins, cells, stem cells and the like, or combinations thereof, with or without targeting sequences. Specific examples of ~5 therapeutic agents include, for example, pharmaceutically active compounds, proteins, cells, stem cells, oligonucleotides, ribozymes, antisense oligonucleotides, DNA
compacting agents, genelvector systems (i.e., any vehicle that allows for the uptake and expression of nucleic acids), nucleic acids (including, for example, recombinant nucleic acids; naked DNA, cDNA, RNA; genomic DNA, cDNA or RNA in a 2o noninfectious vector or in a viral vector and which further may have attached peptide targeting sequences; antisense nucleic acid (RNA or DNA); and DNA chimeras which include gene sequences and eneoding for ferry proteins such as membrane translocating sequences ("MTS") and herpes simplex virus-1 ("VP22")), and viral, liposomes and cationic and anionic polymers and neutral polymers that are selected 25 from a number of types depending on the desired application. Non-limiting examples of virus vectors or vectors derived from viral sources include adenoviral vectors, herpes simplex vectors, papilloma vectors, adeno-associated vectors, retroviral vectors, and the like. Non-limiting examples of biologically active solutes include anti-thrombogenic agents such as heparin, heparin derivatives, urokinase, and PPACK
so (dextrophenylalanine proline arginine chloromethylketone); antioxidants such as probucol and retinoic acid; angiogenic and anti-angiogenic agents and factors;
agents blocking smooth muscle cell proliferation such as rapamycin, angiopeptin, and monoclonal antibodies capable of bloclcing smooth muscle cell proliferation;
anti-inflammatory agents such as dexamethasone, prednisolone, corticosterone, 35 budesonide, estrogen, sulfasalazine, acetyl salicylic acid, and mesalamine;
calcium entry blockers such as verapamil, diltiazem and nifedipine;
antineoplastic/antiproliferative/anti-mitotic agents such as paclitaxel, 5-fluorouracil, methotrexate, doxorubicin, daunorubicin, cyclosporine, cisplatin, vinblastine, vincristine, epothilones, endostatin, angiostatin and thymidine kinase inhibitors;
antimicrobials such as triclosan, dephalosporins, aminoglycosides, and nitorfurantoin;
anesthetic agents such as lidocaine, buplvacaine, and ropivacaine; nitrix oxide (NO) o donors such as lisidomine, molsidomine, L-argine, NO-protein adducts, NO-carbohydrate adducts, polymeric or oligomeric NO adducts; anti-coagulants such as D-Phe-Pro-Arg chloromethyl ketone, an RGD peptide-containing compound, heparine, antithrombin compounds, platelet receptor antagonists, anti-thrombin antibodies, anti-platelet receptor antibodies, enoxaparin, hirudin, Warafin sodium, ~5 Dicumarol, aspirin, prostaglandin inhibitors, platelet inhibitors and tick antiplatelet factors; vascular cell growth promoters such as growth factors, growth factor receptor antagonists, transcriptional activators, and translational promoters; vascular cell growth inhibitors such as growth factor inhibitors, growth factor receptor antagonists, transcriptional repressors, translational repressors, replication inhibitors, inhibitory 2o antibodies, antibodies directed against growth factors, bifunctional molecules consisting of a growth factor and a cytotoxin, bifunctional molecules consisting of an antibody and a cytotoxin; cholesterol-lowering agents; vasodilating agents;
agents which interfere with endogenous vascoactive mechanisms; survival genes which protect against cell death, such as anti-apoptotic Bcl-2 family factors and Akt kinase;
25 and combinations thereof. Cells can be of human origin (autologous or allogenic) or from an animal source (xenogeneic), genetically engineered if desired to deliver proteins of interest at the injection site. The delivery mediated is formulated as needed to maintain cell function and viability.
so Stent Delivery Referring to FIGS. SA-SC, the delivery of a self expanding stmt is illustrated.
The stmt 200 is deployed on a catheter 202 and covered by a sheath 204. When the target site is reached, the sheath is retracted and the stmt self expands into contact with the body lumen.
35 Referring now to FIGS. 6A-6C, the delivery of a balloon-expandable stmt is illustrated. The stmt 300 is carried on a catheter 302 over a balloon 304.
When the treatment site is reached, the balloon is expanded to expand the stmt into contact with the lumen wall.
The stmt body may be made of, for example, Nitinol, a nickel-titanium alloy that can provide the stmt with superelasticity and shape memory properties. In some cases, the stmt body may be made of stainless steel (e.g., 300 series stainless steel), or o aluminum. In some embodiments, the stmt body may be made of tantalum, niobium, titanium, or alloys thereof. The stmt body may be made of composite materials as described in Heath, U.S. 5,725,570, and Mayer, U.S. 5,800,511. In some cases, the stmt body may be made of a cobalt-based alloy, such as the cobalt-based alloys sold under the tradenames Elgiloy (available from Carpenter Technology Corporation, Reading, PA), Phynox (available from Metal Imphy, Imphy, France), and MP35N
(available from Carpenter Technology Corporation, Reading, PA). A stmt as described above has applications, including, for example, in the vascular system (e.g., in the coronary arteries), or in the gastrointestinal tract. The stmt may be an esophageal stmt. The stmt may be used in the biliary duct, or in other body lumens.
Examines Experimental The anodizing process for titanium is first illustrated using flat sheet coupons of 99.6+% pure titanium (25 x 25 x 0.5 mm). A DC power source is used, with the coupon connected up as the anode. The coupon is suspended into the solution, not fully immersed as the electrical connection is through a crocodile clip. The cathode used is also a piece of titanium, though a graphite electrode is used for some experiments. Anodizing is performed using the following different solutions:
~ 20% Phosphoric Acid ~ 80% Phosphoric Acid, 10% Sulfuric Acid ~ 1.5% (wt) Hydrofluoric Acid Voltages range from 5 V up to 100 V. Typically color/oxide develops within the first few seconds of the process i.e. usually in much less than one minute - as the oxide develops and thickens the current flow drops rapidly due to the increase in resistance. Coupons are removed, rinsed in deionized water and then alcohol, and dried. The color obtained is documented and a selection of samples are examined optically and on field emission SEM.
A number of titanium coated stents are also anodized, at ~0 V in the phosphoric acid solution. The stems initially have an outer layer of titanium (200-400 nm) deposited by ion beam assisted deposition.
Results The anodizing process provides a wide variety of colors depending on the, voltage applied. The color is typically uniform throughout the surface for most experiments. However, the hydrofluoric acid solutions produce colors only at the meniscus of the solution (when coupons are not fully immersed). Also, several colors develop at the meniscus in these samples. This phenomenon is not observed on samples anodized in the phosphoric and sulfuric acid solutions. The following is a summary of the voltages used and colors obtained.
20% Phosphoric Acid Solution Voltage Color (V) 5 Silver 10 Dark Gold 20 Purple Light Blue 80 Pink/light gold 90 Pink/purple 100 Purple/green 80% Phosphoric Acid/10% Sulfuric Acid Solution Voltage Color (V]
10 Dark Gold 15 Brown/gold 20 Purple 25 Blue/purple 30 Dark Blue 40 Blue 50 Blue/green 60 Yellow/green 70 Yellow/gold 80 Dull gold 1.5 % Hydrofluoric Acid Solution Voltage Color (V) 5 Multi-color band 20 Multi-color band 30 Multi-color band A selection of samples are examined on a field-emission SEM, with emphasis on the thicker oxide samples, based on voltages and colors.
1o Referring to FIGS. 7A and 7A-1, in the HF solution, uniform color over the completely immersed surface is obtained in the first several seconds but this rapidly redissolves, leaving the mufti-colored band 398 at the meniscus. The band is approximately 1.5 mm wide and is located between the scribed parallel lines "L1" and "L2" in FIGS. 7A and 7A-1. FIG. 7A-1 shows the approximate locations of ~ 5 differently colored regions in mufti-colored band 398. Regions 400 and 402 are gray, region 404 is yellow and pink, region 406 is blue, region 408 is yellow, region 410 is pink, region 412 is blue, region 414 is green and yellow, region 416 is purple/pink, region 418 is pink, region 420 is dark green, and regions 422 and 424 are gray.
Referring to FIG. 7B, the sample anodized in the phosphoric acid solution at 20 90 V reveals a porous structure in the oxide.
Referring to FIG. 7C, samples which develop the multicolor bands in the hydrofluoric acid solutions axe examined. Each of the different colors within this band is examined separately in order to identify whether they have different structures. Pronounced structure is obtained within the dark green layer at the lower 25 end of the band. This dark green layer reveals a uniform porous structure of hollow post-shaped elements.
Moving upward through the bands of color, the porous structure becomes less pronounced and is at earlier stages of growth or re-dissolution. The structure is observed up to the purple/pink band but beyond that is not detected.
The diameter of the post-shaped elements is approximately in the range of about 70 nm to about 100 nm. Their depth is in the range of about 100 nm to about 0 200 nm. This measurement can be performed by atomic force microscopy.
Referring to FIGS. 7D and 7D-1, a comparison between an anodized titanium-coated surface 500 (blue in color) and a non-anodized titanium-coated surface (silver in color) is provided. The titanium-coated stems which are anodized at and in a 20% phosphoric acid solution show a dark blue color after the treatment.
~ 5 Stents and coupons given this treatment do not reveal a hollow post-shaped porous oxide structure.
Discussion In phosphoric solutions at high voltages, the titanium oxide has a somewhat 2o non-uniform porosity. When anodized in dilute hydrofluoric acid solutions, a very pronounced, controlled hollow post-shaped porous structure develops. This structure develops at the meniscus where the sample is suspended into the solution. The oxide forms rapidly but rapidly re-dissolves, except at the meniscus, where it develops into a morphology of post-shaped elements. The porous morphology can thus be 25 controlled.
Other Embodiments While a stmt has been described above, a hollow post-shaped morphology and/or color differentiation may be used in other implantable medical devices.
For 3o example, it may be used in guidewires, catheters (including balloon angioplasty catheters), or filters (including vena cave filters). In some embodiments, one portion of a medical device includes an anodized metal (e.g., titanium), while another portion of the medical device includes a different anodized metal (e.g., tantalum).
The characteristics of a porous layer on one section of a medical device can differ from the 35 characteristics of a porous layer on a different section of the medical device. For example, one section can have larger pores and can contain one type of therapeutic agent (e.g., an antithrombogenic agent), while another section has smaller pores and contains a different type of therapeutic agent (e.g., an anti-inflammatory).
Thus, the two different therapeutic agents can be delivered into the body at different rates. In some cases, the porous layer can include a coating that is a therapeutic agent.
All publications, applications, references, and patents referred to above are incorporated by reference in their entirety.
Other embodiments are within the scope of the following claims.
In some embodiments, the member includes a therapeutic agent. The therapeutic agent can be an antithrombogenic, antioxidant, anti-inflammatory, antiproliferative, antibiotic, drug, cell, or genetic material.
In some embodiments, the generally tubular member includes (e.g., a layer ofJ
titanium, niobium, tantalum, or an alloy thereof. The layer can have a thickness between about 50 nm and about 500 nrn. In some cases, the porous structure is over the layer. The titanium, niobium, tantalum, or alloy thereof can be a layer on a different metal. The different metal can be about 90% or more of the thickness of the ~ 5 tubular member. In certain embodiments, the generally tubular member includes stainless steel, nitinol, or a cobalt-based alloy (e.g., Elgiloy).
The post-shaped elements can include a porous metal oxide, e.g., on the surface of the generally tubular member. In some embodiments, the porous metal oxide has a thickness between about SO nm and about 500 nm and/or pore diameters 2o between about 20 nm and about 200 nrn. The post-shaped elements can have a post height of about 100 nm to about 200 nrn. The post-shaped elements can have pore diameters of about 20 nm to about 200 nm (e.g., about 70 nm to about 100 nm).
In certain embodiments, the device has a color corresponding to light having a wavelength between about 370 nm and about 750 run (e.g., a wavelength of about 25 nm, about 470 nm, about 530 nm, about 580 nm, about 620 nm, or about 700 ritn).
In some cases, the meniscus is formed sequentially on different portions of the metal. The acid solution can be a hydrofluoric acid solution (e.g., a 1.5% (by weight) ,hydrofluoric acid solution). The voltage can be about 5 V to about 100 V In some embodiments, the metal has a thickness between about 200 nm and about 400 nm.
3o In certain embodiments, the method includes applying a therapeutic agent and/or diffusion layer to the stmt. The method can include controlling the oxygen content by bubbling gas (e.g., including oxygen) through the acid solution.
Embodiments may include one or more of the following advantages. A
morphology of hollow post-shaped elements can be formed on a medical device by, 35 e.g. anodization, to provide desired characteristics. For example, a porous structure on the surface of a medical device, such as a stmt, can be a reservoir for a therapeutic material. The geometry of the porous structure, i.e. size and spacing of post-shaped elements, can be selected to, e.g., affect the rate of drug release. In addition, anodization can result in a relatively thick oxidation of a metal. The strength of the metal oxide formed by anodization can be comparable to, or even greater than, the strength of the metal. As a result, a porous oxide structure can be formed on metal body generally without substantially sacrificing the strength of the metal body on which the porous oxide structure is formed, or without impeding the function of the medical device. The robust, durable nature of the porous metal oxide structure protects it from damage during handling (e.g., during crimping, sterilizing, packaging). Furthermore, the durability of the porous metal oxide structure makes it ~ 5 resistant to damage from abrasion during assembly onto a catheter and delivery into the body, such that the porous structure can be relatively thin and the overall profile of the medical device is kept small. An anodized porous metal oxide can be more corrosion-resistant than the metal in its non-anodized state. A robust, porous metal oxide reservoir layer can reduce the need for, or the thickness of, drug protecting, 2o carrying, or metering layers of polymers. To the extent a polymer coating is desirable, the surface morphology increases surface area and provides for improved bonding between the coating and the surface. The morphology can also be selected to affect the apparent color of the medical device by optical reflectance and interference phenomena. For example, a family of medical devices having, e.g., different sizes, 2s therapeutic agents, or other features can be color-coded by varying the surface morphology. Anodization is effective to vary surface morphologies of metals that have desirable characteristics such as biocompatibility, radiopacity, and MRI
visibility. Particularly advantageous porous structures can be formed in titanium, niobium, or tantalum, and alloys including these metals, which can be used to make a 3o medical device, or which can be coated on another material (metal, ceramic, polymer) from which the medical device, or a component of the medical device, is made.
A
desired morphology can also reduce thrombosis by surface roughness, surface charge, and/or metal ion release.
Still further aspects, features, and advantages follow.
DESCRIPTION OF DRAWINGS
The file of this patent contains at least one drawing executed in color.
Copies of this patent with color drawings will be provided by the U.S. Patent and Trademark Office upon request and payment of the necessary fee.
FIGS. lA and 1B are perspective views of a stmt in the compressed and expanded condition, respectively.
FIGS. 2A and 2B are greatly enlarged cross sections through the side wall of a stmt, while FIG 2C is a top view of a portion of the stmt side wall shown in FIGS.
2A and 2B.
FIG 3A is a schematic of an anodization apparatus.
~ 5 FIG 3B is a front view of a stmt in the anodization apparatus of FIG 3A.
FIGS. 4A-4E are schematics of a surface treatment process.
FIGS. SA-SC illustrate delivery of a self expanding stmt.
FIGS. 6A-6C illustrate delivery of a balloon expandable stmt.
FIG 7A is a color photograph of a surface morphology.
2o FIG 7A-1 is a labeled version of the color photograph of FIG 7A.
FIG 7B is a field emission SEM image of a surface morphology.
FIG 7C is a field emission SEM image of a surface morphology FIG. 7D is a color photograph of a stmt (at 2x magnification).
FIG. 7D-1 is a labeled version of the color photograph of FIG 7D.
Structure Referring to FIGS. 1A and 1B, a stmt 10 includes a metal body 12 in the shape of a tube. The metal body includes aperture regions 14 provided in a pattern to facilitate stmt functions, such as radial expansion, and lateral flexibility.
Refernng 3o particularly to FIG lA, for delivery into the body, the stmt 10 is provided or maintained in a relatively small diameter condition corresponding to a diameter D~.
Referring to FIG. 1B, upon placement at the treatment site, the stmt 10 is expanded to a larger diameter, DeXp, so that the stmt is in contact with the lumen wall.
The stmt may be expanded by a mechanical expander, such as an inflatable balloon, or it may 3s be self expanding. The metal body of the stmt may be formed by a generally continuous sheet or by filaments that are wrapped, braided, knitted or otherwise configured to generally define a stmt. A suitable stmt design is the Express stmt, available from Boston Scientific, Natick, Mass. Balloon expandable and self expanding stems are further discussed in Heath, U.S. 5,725,570, the entire contents of which are incorporated herein by reference.
1 o Referring to FIGS. 2A and 2B, greatly expanded cross-sections through the side wall of a stmt, the stmt side wall is composed of a base material 20, an intermediate layer 22, and a porous layer 24. The porous layer 24 has a morphology characterized by hollow post-shaped elements 26. The hollow post-shaped elements 26 define internal volumes 27. Between post-shaped elements 26 are void regions 28.
~ 5 Refernng particularly to FIG 2A, the internal volumes 27 and void regions 28 contain a therapeutic agent 30. A protective or diffusion layer 32 is provided over and within the surface openings of the porous structure. Suitable protective layers include bioerodible polymers which protect the therapeutic agent from exposure to body fluids for a time period based on the thickness and erosion rate of the polymer.
2o Suitable diffusion layers include porous polymers that control the rate of diffusion from the reservoir. In embodiments, a therapeutic agent in the reservoir can be combined in a matrix of erodible polymer.
Referring particularly to FIGS. 2B and 2C, the morphology of the porous layer 24 can be selected to enhance therapeutic agent delivery or other characteristics. For 25 example, the porous morphology can be characterized by the internal volume of the hollow post-shaped elements, the voids between hollow post-shaped elements, and/or the density of the post-shaped elements, which affect the amount of therapeutic agent that can be delivered. The inner diameter or aspect ratio of the post-shaped elements and/or the size of the voids can be varied, which affects the diffusion rate from the 3o reservoir. Pores of different sizes can exhibit different light interference and reflection patterns, thereby resulting in different natural colors.
A hollow post-shaped morphology can be characterized by a thickness Tn.,, height Hp, and a spacing Sp between post-shaped elements. In embodiments, height Hp is about 100 nm to about 200 nm, and spacing Sp is about 1 nm to about 200 nm 35 (e.g., a typical spacing is about 10 nm to about 180 nm). As shown in FIG
2C, post shaped elements 26 have an outer diameter OD and an inner diameter ID. Outer diameter OD is about 20 nm to about 250 run. Inner diameter m is about 5 nrn to about 200 nm (e.g., about 70 nm to about 100 nm). The wall thickness of the tube-shaped elements, measured at the top of the elements, is, for example, about 5 nm to about 50 nm.
In embodiments, the porous layer 24 has a post-shaped element density of about 10 to about 300 post-shaped elements per square micron. In embodiments, the post-shaped element density is different in different parts of the porous layer. The percentage of open area on the layer (i.e., the space on which there are no post-shaped elements) can be about 50% to about 99%. In embodiments, a porous layer has a certain color or colors. For example, an anodized titanium surface can appear to be a specific color because of the size of its pores, and their light reflection and interference patterns. In embodiments, a morphology defined by an array of post-shaped elements acts as a grating that preferentially reflects light of a particular color.
In other embodiments, an anodized surface can vary color by thin film effects, e.g., when the surface is a continuous oxidized layer, rather than discrete post-shaped 2o elements. The porous layer may produce a color corresponding to light having a wavelength between about 370 nm and about 750 nm. The color of the porous layer can, for example, correspond to light having a wavelength of about 420 nm, about 470 nm, about 530 nm, about 580 nm, about 620 nm, or about 700 nm. In other embodiments, the color can be in the infrared or ultraviolet range. Coloring agents such as dyes can be added into the porous layer. A sealing layer (e.g., a polymer) can be formed over the porous layer to protect the coloring agent. Alternatively, the pores can be sealed by treating the porous layer with boiling water. The color of the porous layer can be used to indicate the type of therapeutic agent in a stmt, for example. The color can indicate the specific dose of therapeutic agent or its release rate.
In 3o embodiments, the color can be an indication of the specific purpose for the stmt (e.g., a coronary stmt). Different portions of a stmt can have different colors. The colors can be provided in a pattern to indicate, e.g., manufacturing information (e.g., manufacturing lot or date, and/or manufacturer's logo), or usage indication.
The porous layer, intermediate layer and stmt body can be made of metal or metal oxide. The metals or metal oxides of the layers can be the same or different.
Suitable metals include, e.g., titanium, tantalum, niobium, and aluminum, in substantially pure elemental form or in alloys. In particular embodiments, the stmt body can be stainless steel or nitinol. Titanium, niobium, and tantalum are particularly desirable because of their high biocompatibility Tantalum and niobium are particularly desirable for their radiopacity and MRI visibility In a particular embodiment, the stmt body is made of stainless steel, nitinol, or another metal with desirable strength and flexibility characteristics, the intermediate layer is non-porous titanium, tantalum, or niobium, and the porous layer is oxidized titanium, tantalum or niobium. The base metal provides most of the thickness of the stmt wall, e.g., about 90% or more. In some embodiments, the stmt body is porous but a surface layer is nonporous. In some cases, the stmt body itself is made of an anodizable metal (e.g., titanium, tantalum, niobium, or alloys thereof), and is treated as described with reference to FIGS. 3A and 3B, infra.
Manufacture Referring to FIGS. 3A and 3B, the hollow post-shaped porous morphology can 2o be formed by anodization. In anodization, a work piece such as a stmt 40 is placed in a chemical bath 42 and connected as the anode of an electrical circuit 44 to induce surface oxidation. The stmt can, for example, be oriented horizontally or vertically, and then dipped into the chemical bath. The cathode 46 of the circuit can be, e.g., titanium or graphite. In embodiments, several (e.g., three, four, five) cathodes 46 can surround stmt 40 to enhance current distribution across the surface of stmt 40.
Referring particularly to FIG 3B, the process parameters, such as exposure time to the chemical bath and oxygen consumptionaeration, can be controlled to effect a desirable hollow post-shaped morphology by anodizing at a meniscus.
The stmt 40 is partially immersed in the chemical bath 42. At the interface of the bath and the atmosphere, a meniscus 50 forms on the surface of the stmt. The exposure time of a portion of the stmt to the meniscus can be varied by moving the stmt relative to the bath, e.g., by rotating the stmt about its axis, while anodization is conducted. As illustrated in the examples below, anodization at the meniscus can be used to form well-defined morphologies of hollow post-shaped elements on metals such as titanium.
The depth, diameter, and spacing of the post-shaped elements can be controlled by controlling process parameters such as the process time, exposure depth, and oxygen consumption/aeration in the chemical bath, the composition of the chemical bath, circuit voltage, process temperature, and the metal undergoing treatment. If low acid concentrations and temperatures are used, then the resulting anodized surface may be less porous and harder than it is if higher temperatures and acid concentrations are used. Higher temperatures, higher acid concentrations, and longer anodization time periods can produce more porous and, in some cases, softer, coatings. The chemical bath includes an acid solution. Particular acids include strong acids such as hydrogen halides, e.g., HF or HCl, and phosphoric and sulfuric acids ~ 5 and mixtures thereof.
The circuit voltage can influence the size of the openings of the hollow post-shaped elements. For example, higher voltages yield larger openings. The circuit voltage is typically in the range of about 5 V to about 100 V, e.g., about 20 V to about 80 V The temperature for the anodization process can be equal to or greater than 2o about 10°C (e.g., between about 10°C and about 70°C, between about 20°C and about 60°C). In a particular example, the chemical bath can be an acid solution, such as a hydrofluoric acid solution (e.g., a 1.5% by weight hydrofluoric acid solution), a phosphoric acid solution (e.g., a 20% by volume phosphoric acid solution), or a sulfuric acid and phosphoric acid solution (e.g., a 10% by volume sulfuric acid and 2s 80% by volume phosphoric acid solution). The circuit voltage can be, e.g., between about 5 V and about 100 V (e.g., about 20 V or about 80 V). For example, the temperature for the anodization process can be about 25°C. Exposure time to the chemical bath can be less than about one minute (e.g., between about five seconds and about ten seconds).
3o In the embodiments described above, anodization is carried out at the meniscus to form an anodized surface of post-like structures. The oxygen level available to the anodized region can also be varied using other techniques (e.g., oxygen or air can be bubbled through the chemical bath). In embodiments, an entire surface to be anodized (e.g., a stmt) can be immersed in the chemical bath, rather than 35 being anodized at the meniscus.
Refernng to FIGS. 4A-4E, a stent-forming process is illustrated. In FIG 4A, a base material 60 is provided. The base material may be a metal, such as stainless steel, that forms the body of the stmt. The thickness of the body is typically about 0.005 mm or more, e.g., about 0.05 mm to about 0.3 mm. An anodizable metal is provided as a surface layer 62 on the stmt. The surface layer can be provided by techniques including physical vapor deposition, chemical vapor deposition, spraying, electroplating, dipping, or combinations of these processes. The surface layer preferably is provided by physical vapor deposition. The deposited layer is typically near the full density of the metal, e.g., between about 90% and about 100%
(e.g., about 99%) the density of the full metal. The deposited layer does not exhibit ~5 significant or regular porosity. In embodiments, the thickness of the deposited layer is typically in the range of about 10% or less of the thickness of the stmt body.
In embodiments, the thickness of the layer is about 0.1 micron to about 1.0 micron. The layer can be provided on just the exterior wall surface of the stmt, just the interior surface, or both the interior and exterior surfaces. The layer can completely cover the 2o stmt surface or just portions of the surface.
Referring to FIG 4B, the surface layer 62 is anodized. Anodization oxidizes the surface layer, thereby creating porous layer 64 having a morphology of hollow post-shaped elements. For example, if the surface layer is titanium, then anodization creates a titanium oxide layer.
25 Refernng to FIG 4C, a greatly enlarged cross-sectional view of FIG 4B, the anodization process creates a porous layer 64 that exhibits a desired porosity. Porous layer 64 has post-shaped elements 68 defining internal volumes 70. Post-shaped elements 68 are separated by void regions 72. Porous layer 64 can exhibit enhanced surface toughness relative to the material from which it is formed. The porous layer 3o can be provided over the entire stmt or over portions of the stmt, e.g., the exterior surface.
Referring to FIG 4D, a material such as a therapeutic agent can be provided into the porous structure by, for example, dipping, spray coating or the like.
The therapeutic agent can be provided into the volumes and void regions defined by the s5 post-shaped elements. In FIG 4D, a therapeutic agent 74 has been delivered into both the internal volumes of the post-shaped elements 70 and the void regions 72.
to Referring to FIG 4E, the porous layer 64 can be coated with a protective or diffusion layer 80. In some cases, the protective layer also is a diffusion layer. The protective and/or diffusion layer can be within each pore or can cover the entire stmt.
The protective layer can be a biodegradable material that protects and retains the therapeutic agent in the porous structure prior to delivery into the body.
For 1o example, the protective layer can be a polymer, e.g.
polytetrafluoroethylene (available from DuPont under the tradename Teflon'). The thickness of the protective layer can be between about 0.1 ,um and about 10 ,um. The protective layer can be an erodible polymer. Suitable erodible polymers include water soluble polymers such as polyvinyl alcohol (e.g., that has not been cross-linked), hydrogels (e.g., polyacrylic ~5 acid, haluronic acid, gelatin, carboxymethyl cellulose), polyethylene glycols (PEG), chitosan, and polyesters (e.g., polycaprolactones).
The diffusion layer controls the release of the therapeutic agent out of the pores. The diffusion layer can be biodegradable. Alternatively or additionally, the diffusion layer can be a polymer. Polymers may be, for example, homopolymers or 2o copolymers, crosslinked or uncrosslinked, linear or branched, natural or synthetic, thermoplastic or thermosetting. Polymers include the following: polycarboxylic acid polymers and copolymers including polyacrylic acids; acetal polymers and copolymers; acrylate and methacrylate polymers and copolymers (e.g., n-butyl methacrylate); cellulosic polymers and copolymers, including cellulose acetates, 25 cellulose nitrates, cellulose propionates, cellulose acetate butyrates, cellophanes, rayons, rayon triacetates, and cellulose ethers such as caxboxymethyl celluloses and hydoxyalkyl celluloses; polyoxymethylene polymers and copolymers; polyimide polymers and copolymers such as polyether block imides, polyamidimides, polyesterimides, and polyetherimides; polysulfone polymers and copolymers 3o including polyarylsulfones and polyethersulfones; polyamide polymers and copolymers including nylon 6,6, polycaprolactams and polyacrylamides; resins including alkyd resins, phenolic resins, urea resins, melamine resins, epoxy resins, allyl resins and epoxide resins; polycarbonates; polyacrylonitriles;
polyvinylpyrrolidones (cross-linked and otherwise); polymers and copolymers of 35 vinyl monomers including polyvinyl alcohols, polyvinyl halides such as polyvinyl chlorides, ethylene-vinylacetate copolymers (EVA), polyvinylidene chlorides, polyvinyl ethers such as polyvinyl methyl ethers, styrene polymers and copolymers such as polystyrenes, styrene-malefic anhydride copolymers, styrene-butadiene copolymers, styrene-ethylene-butylene copolymers (e.g., a polystyrene-polyethylene/butylene-polystyrene (SEES) copolymer, available as Kraton~ G
series polymers), acrylonitrile-styrene copolymers, acrylonitrile-butadiene-styrene copolymers, styrene-butadiene copolymers and styrene-isobutylene copolymers (e.g., polyisobutylene-polystyrene block copolymers such as SIBS, see, e.g., U.S.
Patent No. 6,545,097), polyvinyl ketones, polyvinylcarbazoles, and polyvinyl esters such as polyvinyl acetates; polybenzimidazoles; ionomers; polyalkyl oxide polymers and copolymers including polyethylene oxides (PEO); glycosaminoglycans; polyesters ~ 5 including polyethylene terephthalates and aliphatic polyesters such as polymers and copolymers of lactide (which includes lactic acid as well as d-,1- and meso lactide), epsilon-caprolactone, glycolide (including glycolic acid), hydroxybutyrate, hydroxyvalerate, para-dioxanone, trimethylene carbonate (and its alkyl derivatives), 1,4-dioxepan-2-one, 1,5-dioxepan-~-one, and 6,6-dimethyl-1,4-dioxan-2-one (a 2o copolymer of polylactic acid and polycaprolactone is one specific example);
polyether polymers and copolymers including polyarylethers such as polyphenylene ethers, polyether ketones, polyether ether ketones; polyphenylene sulfides;
polyisocyanates;
polyolefin polymers and copolymers, including polyalkylenes such as polypropylenes, polyethylenes (low and high density, low and high molecular weight), polybutylenes 25 (such as polybut-1-ene and polyisobutylene), poly-4-methyl-pen-1-enes, ethylene-alpha-olefin copolymers, ethylene-methyl methacrylate copolymers and ethylene-vinyl acetate copolymers; fluorinated polymers and copolymers, including polytetrafluoroethylenes (PTFE), poly(tetrafluoroethylene-co-hexafluoropropene) (FEP), modified ethylene-tetrafluoroethylene copolymers (ETFE), and polyvinylidene 3o fluorides (PVDF); silicone polymers and copolymers; polyurethanes; p-xylylene polymers; polyiminocarbonates; copoly(ether-esters)such as polyethylene oxide-polylactic acid copolymers; polyphosphazines; polyalkylene oxalates;
polyoxaamides and polyoxaesters (including those containing amines and/or amido groups);
polyorthoesters; biopolymers, such as polypeptides, proteins, polysaccharides and 35 fatty acids (and esters thereof), including fibrin, fibrinogen, collagen, elastin, chitosan, s gelatin, starch, glycosaminoglycans such as hyaluronic acid; as well as blends and additional copolymers of the above.
Examples of polymers include block copolymers comprising at least one A
block and at least one B block. The A blocks are preferably soft elastomeric blocks, which are based upon one or more polyolefins, or other polymer with a glass transition temperature at or below room temperature. For example, the A blocks can be polyolefinic blocks having alternating quaternary and secondary carbons of the general formulation: -(CRR'-CH2)n-, where R and R' are, independently, linear or branched aliphatic groups such as methyl, ethyl, propyl, isopropyl, butyl, isobutyl and so forth, or represent cyclic aliphatic groups such as cyclohexane, cyclopentane, and ~ 5 the like, either with or without pendant groups. Preferred polyolefinic blocks include HOC
polymeric blocks of isobutylene, cH3, (i.e., polymers where R and R' are methyl groups). Other examples of A blocks include silicone rubber blocks and acrylate rubber blocks.
The B blocks are preferably hard thermoplastic blocks with glass transition 2o temperatures significantly higher than the elastomeric A blocks which, when combined with the soft A blocks, are capable of, inter alia, altering or adjusting the hardness of the resulting copolymer to achieve a desired combination of qualities.
Examples of B blocks include polymers of methacrylates or polymers of vinyl aromatics. More specific examples of B blocks include blocks that are (a) formed ~CHZ
25 from monomers of styrene , styrene denvatives (e.g., a methylstyrene, ring-alkylated styrenes or ring-halogenated styrenes or other substituted styrenes where one or more substituents are present on the aromatic ring) or mixtures of the same, collectively referred to herein as "styrenic blocks"
or "polystyrenic blocks" or are (b) formed from monomers of methylmethacrylate, 3o ethylmethacrylate, hydroxyethyl methacrylate or mixtures of the same.
The block copolymers are provided in a variety of architectures, including cyclic, linear, and branched architectures. Branched architectures include star-shaped architectures (e.g., architectures in which three or more chains emanate from a single region), comb architectures (e.g., copolymers having a main chain and a plurality of side chains), and dendritic architectures (including arborescent or hyperbranched copolymers).
Some specific examples of such block copolymers include the following: (a) BA (linear diblock), (b) BAB or ABA (linear triblock), (c) B(AB)" or A(BA)"
(linear 1o alternating block), or (d) X-(AB)" or X-(BA)" (includes diblock, triblock and other radial block copolymers), where n is a positive whole number and X is a starting seed, or initiator, molecule. One specific group of polymers have X-(AB) n structures, which are frequently referred to as diblock copolymers and triblock copolymers where n=1 and n=2, respectively (this terminology disregards the presence of the ~5 starting seed molecule, for example, treating A-X-A as a single A block, with the triblock therefore denoted as BAB). A particularly beneficial polymer from this group is polystyrene-polyisobutylene-polystyrene triblock copolymer (SIBS).
Where n=3 or more, these structures are commonly referred to as star-shaped block copolymers. Other examples of block polymers include branched block copolymers 2o such as dendritic block copolymers, wherein at least one of the A and B
blocks is branched, for instance, where the A blocks are branched and are capped by the B
blocks.
The thickness of the diffusion layer can be, e.g., between about 0.1 ~.m and about 10 ,um.
25 ~ The porous layer can be partially sealed to control drug diffusion. A
partial sealant layer can be added to the porous layer, or the porous layer can be partially sealed by treating the porous layer with boiling water. During such treatment, the oxide is hydrated, causing it to swell and thereby start to close in the pores. The parameters of the sealing process can be adjusted to achieve a desired amount of 3o sealing.
The protective layer, diffusion layer, or sealant layer can include a therapeutic agent instead of or in addition to a therapeutic agent in the porous layer.
The therapeutic agent in these layers can be the same as or different from the therapeutic agent in the porous layer. For example, the protective, diffusion, or sealant layer can 35 include an antithrombogenic agent, which is released quickly during delivery and deployment, while the porous layer contains an anti-inflammatory, which is released more slowly at the site. The therapeutic agent provided in the volumes and voids of the porous layer can be dissolved in a Garner, such as an erodible polymer or a diffusion-controlling polymer.
The term "therapeutic agent" includes one or more "therapeutic agents" or "drugs". The terms "therapeutic agents" and "drugs" are used interchangeably and include pharmaceutically active compounds, nucleic acids with and without carrier vectors such as lipids, compacting agents (such as histones), virus (such as adenovirus, adeno-associated virus, retrovirus, lentivirus and a-virus), polymers, antibiotics, hyaluronic acid, gene therapies, proteins, cells, stem cells and the like, or combinations thereof, with or without targeting sequences. Specific examples of ~5 therapeutic agents include, for example, pharmaceutically active compounds, proteins, cells, stem cells, oligonucleotides, ribozymes, antisense oligonucleotides, DNA
compacting agents, genelvector systems (i.e., any vehicle that allows for the uptake and expression of nucleic acids), nucleic acids (including, for example, recombinant nucleic acids; naked DNA, cDNA, RNA; genomic DNA, cDNA or RNA in a 2o noninfectious vector or in a viral vector and which further may have attached peptide targeting sequences; antisense nucleic acid (RNA or DNA); and DNA chimeras which include gene sequences and eneoding for ferry proteins such as membrane translocating sequences ("MTS") and herpes simplex virus-1 ("VP22")), and viral, liposomes and cationic and anionic polymers and neutral polymers that are selected 25 from a number of types depending on the desired application. Non-limiting examples of virus vectors or vectors derived from viral sources include adenoviral vectors, herpes simplex vectors, papilloma vectors, adeno-associated vectors, retroviral vectors, and the like. Non-limiting examples of biologically active solutes include anti-thrombogenic agents such as heparin, heparin derivatives, urokinase, and PPACK
so (dextrophenylalanine proline arginine chloromethylketone); antioxidants such as probucol and retinoic acid; angiogenic and anti-angiogenic agents and factors;
agents blocking smooth muscle cell proliferation such as rapamycin, angiopeptin, and monoclonal antibodies capable of bloclcing smooth muscle cell proliferation;
anti-inflammatory agents such as dexamethasone, prednisolone, corticosterone, 35 budesonide, estrogen, sulfasalazine, acetyl salicylic acid, and mesalamine;
calcium entry blockers such as verapamil, diltiazem and nifedipine;
antineoplastic/antiproliferative/anti-mitotic agents such as paclitaxel, 5-fluorouracil, methotrexate, doxorubicin, daunorubicin, cyclosporine, cisplatin, vinblastine, vincristine, epothilones, endostatin, angiostatin and thymidine kinase inhibitors;
antimicrobials such as triclosan, dephalosporins, aminoglycosides, and nitorfurantoin;
anesthetic agents such as lidocaine, buplvacaine, and ropivacaine; nitrix oxide (NO) o donors such as lisidomine, molsidomine, L-argine, NO-protein adducts, NO-carbohydrate adducts, polymeric or oligomeric NO adducts; anti-coagulants such as D-Phe-Pro-Arg chloromethyl ketone, an RGD peptide-containing compound, heparine, antithrombin compounds, platelet receptor antagonists, anti-thrombin antibodies, anti-platelet receptor antibodies, enoxaparin, hirudin, Warafin sodium, ~5 Dicumarol, aspirin, prostaglandin inhibitors, platelet inhibitors and tick antiplatelet factors; vascular cell growth promoters such as growth factors, growth factor receptor antagonists, transcriptional activators, and translational promoters; vascular cell growth inhibitors such as growth factor inhibitors, growth factor receptor antagonists, transcriptional repressors, translational repressors, replication inhibitors, inhibitory 2o antibodies, antibodies directed against growth factors, bifunctional molecules consisting of a growth factor and a cytotoxin, bifunctional molecules consisting of an antibody and a cytotoxin; cholesterol-lowering agents; vasodilating agents;
agents which interfere with endogenous vascoactive mechanisms; survival genes which protect against cell death, such as anti-apoptotic Bcl-2 family factors and Akt kinase;
25 and combinations thereof. Cells can be of human origin (autologous or allogenic) or from an animal source (xenogeneic), genetically engineered if desired to deliver proteins of interest at the injection site. The delivery mediated is formulated as needed to maintain cell function and viability.
so Stent Delivery Referring to FIGS. SA-SC, the delivery of a self expanding stmt is illustrated.
The stmt 200 is deployed on a catheter 202 and covered by a sheath 204. When the target site is reached, the sheath is retracted and the stmt self expands into contact with the body lumen.
35 Referring now to FIGS. 6A-6C, the delivery of a balloon-expandable stmt is illustrated. The stmt 300 is carried on a catheter 302 over a balloon 304.
When the treatment site is reached, the balloon is expanded to expand the stmt into contact with the lumen wall.
The stmt body may be made of, for example, Nitinol, a nickel-titanium alloy that can provide the stmt with superelasticity and shape memory properties. In some cases, the stmt body may be made of stainless steel (e.g., 300 series stainless steel), or o aluminum. In some embodiments, the stmt body may be made of tantalum, niobium, titanium, or alloys thereof. The stmt body may be made of composite materials as described in Heath, U.S. 5,725,570, and Mayer, U.S. 5,800,511. In some cases, the stmt body may be made of a cobalt-based alloy, such as the cobalt-based alloys sold under the tradenames Elgiloy (available from Carpenter Technology Corporation, Reading, PA), Phynox (available from Metal Imphy, Imphy, France), and MP35N
(available from Carpenter Technology Corporation, Reading, PA). A stmt as described above has applications, including, for example, in the vascular system (e.g., in the coronary arteries), or in the gastrointestinal tract. The stmt may be an esophageal stmt. The stmt may be used in the biliary duct, or in other body lumens.
Examines Experimental The anodizing process for titanium is first illustrated using flat sheet coupons of 99.6+% pure titanium (25 x 25 x 0.5 mm). A DC power source is used, with the coupon connected up as the anode. The coupon is suspended into the solution, not fully immersed as the electrical connection is through a crocodile clip. The cathode used is also a piece of titanium, though a graphite electrode is used for some experiments. Anodizing is performed using the following different solutions:
~ 20% Phosphoric Acid ~ 80% Phosphoric Acid, 10% Sulfuric Acid ~ 1.5% (wt) Hydrofluoric Acid Voltages range from 5 V up to 100 V. Typically color/oxide develops within the first few seconds of the process i.e. usually in much less than one minute - as the oxide develops and thickens the current flow drops rapidly due to the increase in resistance. Coupons are removed, rinsed in deionized water and then alcohol, and dried. The color obtained is documented and a selection of samples are examined optically and on field emission SEM.
A number of titanium coated stents are also anodized, at ~0 V in the phosphoric acid solution. The stems initially have an outer layer of titanium (200-400 nm) deposited by ion beam assisted deposition.
Results The anodizing process provides a wide variety of colors depending on the, voltage applied. The color is typically uniform throughout the surface for most experiments. However, the hydrofluoric acid solutions produce colors only at the meniscus of the solution (when coupons are not fully immersed). Also, several colors develop at the meniscus in these samples. This phenomenon is not observed on samples anodized in the phosphoric and sulfuric acid solutions. The following is a summary of the voltages used and colors obtained.
20% Phosphoric Acid Solution Voltage Color (V) 5 Silver 10 Dark Gold 20 Purple Light Blue 80 Pink/light gold 90 Pink/purple 100 Purple/green 80% Phosphoric Acid/10% Sulfuric Acid Solution Voltage Color (V]
10 Dark Gold 15 Brown/gold 20 Purple 25 Blue/purple 30 Dark Blue 40 Blue 50 Blue/green 60 Yellow/green 70 Yellow/gold 80 Dull gold 1.5 % Hydrofluoric Acid Solution Voltage Color (V) 5 Multi-color band 20 Multi-color band 30 Multi-color band A selection of samples are examined on a field-emission SEM, with emphasis on the thicker oxide samples, based on voltages and colors.
1o Referring to FIGS. 7A and 7A-1, in the HF solution, uniform color over the completely immersed surface is obtained in the first several seconds but this rapidly redissolves, leaving the mufti-colored band 398 at the meniscus. The band is approximately 1.5 mm wide and is located between the scribed parallel lines "L1" and "L2" in FIGS. 7A and 7A-1. FIG. 7A-1 shows the approximate locations of ~ 5 differently colored regions in mufti-colored band 398. Regions 400 and 402 are gray, region 404 is yellow and pink, region 406 is blue, region 408 is yellow, region 410 is pink, region 412 is blue, region 414 is green and yellow, region 416 is purple/pink, region 418 is pink, region 420 is dark green, and regions 422 and 424 are gray.
Referring to FIG. 7B, the sample anodized in the phosphoric acid solution at 20 90 V reveals a porous structure in the oxide.
Referring to FIG. 7C, samples which develop the multicolor bands in the hydrofluoric acid solutions axe examined. Each of the different colors within this band is examined separately in order to identify whether they have different structures. Pronounced structure is obtained within the dark green layer at the lower 25 end of the band. This dark green layer reveals a uniform porous structure of hollow post-shaped elements.
Moving upward through the bands of color, the porous structure becomes less pronounced and is at earlier stages of growth or re-dissolution. The structure is observed up to the purple/pink band but beyond that is not detected.
The diameter of the post-shaped elements is approximately in the range of about 70 nm to about 100 nm. Their depth is in the range of about 100 nm to about 0 200 nm. This measurement can be performed by atomic force microscopy.
Referring to FIGS. 7D and 7D-1, a comparison between an anodized titanium-coated surface 500 (blue in color) and a non-anodized titanium-coated surface (silver in color) is provided. The titanium-coated stems which are anodized at and in a 20% phosphoric acid solution show a dark blue color after the treatment.
~ 5 Stents and coupons given this treatment do not reveal a hollow post-shaped porous oxide structure.
Discussion In phosphoric solutions at high voltages, the titanium oxide has a somewhat 2o non-uniform porosity. When anodized in dilute hydrofluoric acid solutions, a very pronounced, controlled hollow post-shaped porous structure develops. This structure develops at the meniscus where the sample is suspended into the solution. The oxide forms rapidly but rapidly re-dissolves, except at the meniscus, where it develops into a morphology of post-shaped elements. The porous morphology can thus be 25 controlled.
Other Embodiments While a stmt has been described above, a hollow post-shaped morphology and/or color differentiation may be used in other implantable medical devices.
For 3o example, it may be used in guidewires, catheters (including balloon angioplasty catheters), or filters (including vena cave filters). In some embodiments, one portion of a medical device includes an anodized metal (e.g., titanium), while another portion of the medical device includes a different anodized metal (e.g., tantalum).
The characteristics of a porous layer on one section of a medical device can differ from the 35 characteristics of a porous layer on a different section of the medical device. For example, one section can have larger pores and can contain one type of therapeutic agent (e.g., an antithrombogenic agent), while another section has smaller pores and contains a different type of therapeutic agent (e.g., an anti-inflammatory).
Thus, the two different therapeutic agents can be delivered into the body at different rates. In some cases, the porous layer can include a coating that is a therapeutic agent.
All publications, applications, references, and patents referred to above are incorporated by reference in their entirety.
Other embodiments are within the scope of the following claims.
Claims (46)
1. A stent device comprising:
a generally tubular member, the member including a porous structure comprising an oxide of titanium, niobium, tantalum, or an alloy thereof, the porous structure including hollow post-shaped elements.
a generally tubular member, the member including a porous structure comprising an oxide of titanium, niobium, tantalum, or an alloy thereof, the porous structure including hollow post-shaped elements.
2. The device of claim 1, wherein the porous structure is of an oxide of titanium.
3. The device of claim 1, wherein the generally tubular member comprises a therapeutic agent.
4. The device of claim 3, wherein the therapeutic agent is selected from an antithrombogenic, antioxidant, anti-inflammatory, antiproliferative, or antibiotic.
5. The device of claim 3, wherein the therapeutic agent is selected from a drug, cell, or genetic material.
6. The device of claim 1, wherein the generally tubular member includes a layer of titanium, niobium, tantalum, or an alloy thereof, that has a thickness between about 50 nm and about 500 nm.
7. The device of claim 6, wherein the porous structure is over said layer.
8. The device of claim 1, wherein the post-shaped elements have pore diameters of about 20 nm to about 200 nm.
9. The device of claim 8, wherein the post-shaped elements have pore diameters of about 70 nm to about 100 nm.
10. The device of claim 9, wherein the post-shaped elements have a post height of about 100 nm to about 200 nm.
11. The device of claim 1, wherein the porous structure is on an outer surface of the generally tubular member.
12. The device of claim 1, wherein the generally tubular member comprises titanium, niobium, tantalum, or an alloy thereof.
13. The device of claim 1, wherein said titanium, niobium, tantalum, or alloy thereof is a layer on a different metal.
14. The device of claim 13, wherein the different metal is about 90% or more of the thickness of the tubular member.
15. The device of claim 1, wherein the generally tubular member comprises stainless steel, nitinol, or a cobalt-based alloy.
16. The device of claim 1, wherein the porous structure includes a polymer.
17. The device of claim 16, wherein the polymer is a coating over the porous structure.
18. The device of claim 17, wherein the coating is a diffusion or protective layer.
19. The device of claim 17, wherein the coating is biodegradable.
20. The device of claim 16, wherein the polymer includes a therapeutic agent.
21. The device of claim 1, wherein the porous structure includes a colorant.
22. The device of claim 1, wherein the device has a color corresponding to light having a wavelength between about 370 nm and about 750 nm.
23. The device of claim 22, wherein the color corresponds to light having a wavelength of about 420 nm, about 470 nm, about 530 nm, about 580 nm, about nm, or about 700 nm.
24. A stent device comprising:
a generally tubular member, the member including a porous structure of hollow post-shaped elements.
a generally tubular member, the member including a porous structure of hollow post-shaped elements.
25. The device of claim 24, wherein the generally tubular member includes a therapeutic agent.
26. The device of claim 25, wherein the therapeutic agent is selected from an antithrombogenic, antioxidant, anti-inflammatory, antiproliferative, or antibiotic.
27. The device of claim 25, wherein the therapeutic agent is selected from a drug, cell, or genetic material.
28. The device of claim 24, wherein the post-shaped elements comprise a porous metal oxide.
29. The device of claim 28, wherein the porous metal oxide has a thickness between about 50 nm and about 500 nm.
30. The device of claim 28, wherein the porous metal oxide has pore diameters between about 20 nm and about 200 nm.
31. The device of claim 28, wherein the porous metal oxide is on a surface of the generally tubular member.
32. A method of making a stent, comprising:
(a) providing a metal;
(b) exposing the metal to an acid solution such that the acid solution forms a meniscus on the metal;
(c) connecting the metal as an anode in an electrical circuit in the acid solution; and (d) applying a voltage to the circuit, the metal being incorporated in a stent.
(a) providing a metal;
(b) exposing the metal to an acid solution such that the acid solution forms a meniscus on the metal;
(c) connecting the metal as an anode in an electrical circuit in the acid solution; and (d) applying a voltage to the circuit, the metal being incorporated in a stent.
33. The method of claim 32, wherein the meniscus is formed sequentially on different portions of the metal.
34. The method of claim 32, wherein the acid solution comprises a hydrofluoric acid solution.
35. The method of claim 34, wherein the voltage is about 5 V to about 100 V.
36. The method of claim 34, wherein the acid solution comprises a 1.5%
(by weight) hydrofluoric acid solution.
(by weight) hydrofluoric acid solution.
37. The method of claim 32, wherein the metal has a thickness between about 200 nm and about 400 nm.
38. The method of claim 32, further comprising applying a therapeutic agent to the stent.
39. The method of claim 32, further comprising applying a diffusion layer to the stent.
40. A method of making a stent, comprising:
(a) providing a metal;
(b) exposing the metal to an acid solution;
(c) controlling the oxygen content of the acid solution;
(d) connecting the metal as an anode in an electrical circuit in the acid solution; and (e) applying a voltage to the circuit, the metal being incorporated in a stent.
(a) providing a metal;
(b) exposing the metal to an acid solution;
(c) controlling the oxygen content of the acid solution;
(d) connecting the metal as an anode in an electrical circuit in the acid solution; and (e) applying a voltage to the circuit, the metal being incorporated in a stent.
41. The method of claim 40, further comprising controlling the oxygen content by bubbling gas through the acid solution.
42. The method of claim 41, wherein the gas includes oxygen.
43. A family of medical devices, wherein members of said medical devices include an oxide providing a different color or color pattern.
44. The family of claim 43, wherein the color or color pattern is indicative of usage.
45. A medical device includes an oxide providing a color or color pattern indicative of manufacturing information.
46. The medical device of claim 45, wherein the manufacturing information is a lot, date, or manufacturer identification.
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| PCT/US2004/030319 WO2005027794A2 (en) | 2003-09-16 | 2004-09-16 | Medical devices |
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| CA2538392A1 true CA2538392A1 (en) | 2005-03-31 |
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| CA002538392A Abandoned CA2538392A1 (en) | 2003-09-16 | 2004-09-16 | Medical devices |
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| EP (1) | EP1670391B1 (en) |
| JP (1) | JP4755096B2 (en) |
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| CA (1) | CA2538392A1 (en) |
| DE (1) | DE602004017490D1 (en) |
| WO (1) | WO2005027794A2 (en) |
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-
2003
- 2003-09-16 US US10/664,679 patent/US7488343B2/en active Active
-
2004
- 2004-09-16 EP EP04784250A patent/EP1670391B1/en not_active Not-in-force
- 2004-09-16 CA CA002538392A patent/CA2538392A1/en not_active Abandoned
- 2004-09-16 JP JP2006527019A patent/JP4755096B2/en not_active Expired - Fee Related
- 2004-09-16 DE DE602004017490T patent/DE602004017490D1/en active Active
- 2004-09-16 AT AT04784250T patent/ATE412387T1/en not_active IP Right Cessation
- 2004-09-16 WO PCT/US2004/030319 patent/WO2005027794A2/en active Application Filing
-
2009
- 2009-01-02 US US12/348,211 patent/US8377111B2/en active Active
Also Published As
| Publication number | Publication date |
|---|---|
| ATE412387T1 (en) | 2008-11-15 |
| US7488343B2 (en) | 2009-02-10 |
| WO2005027794A2 (en) | 2005-03-31 |
| EP1670391B1 (en) | 2008-10-29 |
| DE602004017490D1 (en) | 2008-12-11 |
| US20090117351A1 (en) | 2009-05-07 |
| US8377111B2 (en) | 2013-02-19 |
| WO2005027794A3 (en) | 2005-06-09 |
| JP4755096B2 (en) | 2011-08-24 |
| JP2007505703A (en) | 2007-03-15 |
| EP1670391A2 (en) | 2006-06-21 |
| US20050060021A1 (en) | 2005-03-17 |
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