Method for remediation of intervertebral disks
A method for the implantation of a device made of bioresorbable materials between interspinous processes is described. The implant has a spacer that can be placed between adjacent spinous processes to limit the movement of the vertebrae. Once inserted between interspinous processes, the implant acts to limit extension (backward bending) of the spine without inhibiting the flexion (forward bending) of the spinal column. The device is used as an adjunct to remediation of an intervertebral disk.
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This application is related to U.S. patent application Ser. No. 10/230,505, filed Aug. 29, 2002, entitled “DEFLECTABLE SPACER FOR USE AS AN INTERSPINOUS PROCESS IMPLANT AND METHOD,” U.S. Provisional Application Ser. No. 60/421,921, filed Oct. 29, 2002, entitled “INTERSPINOUS PROCESS APPARATUS AND METHOD WITH A SELECTABLY EXPANDABLE SPACER,” and U.S. patent application Ser. No. 10/684,847, filed Oct. 14, 2003, entitled “INTERSPINOUS PROCESS APPARATUS AND METHOD FOR SELECTABLY EXPANDABLE SPACER,” which are incorporated herein by reference. This application also is related to U.S. patent application Ser. No. ______ filed ______ entitled, “BIORESORBABLE INTERSPINOUS PROCESS IMPLANT FOR USE WITH INTERVERTEBRAL DISK REMEDIATION OR REPLACEMENT IMPLANTS AND PROCEDURES,” incorporated herein by reference. This application is also related to U.S. patent application Ser. No. 10/037,236, filed Nov. 9, 2001, entitled “INTER-SPINOUS PROCESS IMPLANT AND METHOD WITH DEFORMABLE SPACER,” which is related to U.S. patent application Ser. No. 09/799,215, filed Mar. 5, 2001, entitled “SPINE DISTRACTION IMPLANT,” which is related to U.S. patent application Ser. No. 09/473,173, filed Dec. 28, 1999, entitled “SPINE DISTRACTION IMPLANT,” now U.S. Pat. No. 6,235,030, which is related to U.S. patent application Ser. No. 09/179,570, filed Oct. 27, 1998, entitled “SPINE DISTRACTION IMPLANT,” now U.S. Pat. No. 6,048,342, which is related to U.S. patent application Ser. No. 09/474,037, filed Dec. 28, 1999, entitled “SPINE DISTRACTION IMPLANT,” now U.S. Pat. No. 6,190,387, which is related to U.S. patent application Ser. No. 09/175,645, filed Oct. 20, 1998, entitled “SPINE DISTRACTION IMPLANT,” now U.S. Pat. No. 6,068,630, and U.S. application Ser. No. 10/694,103, filed Oct. 27, 2003, entitled “INTERSPINOUS PROCESS IMPLANT WITH RADIOLUCENT SPACER AND LEAD-IN TISSUE EXPANDER.” All of the above are incorporated herein by reference. This application is also related to U.S. patent application Ser. No. 10/684,669, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH TRANSLATING PIVOT POINT AND METHOD,” U.S. Provisional Patent Application Ser. No. 60/526,724, filed Dec. 2, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH TRANSLATING PIVOT POINT AND LATERAL IMPLANT METHOD,” U.S. patent application Ser. No. 10/684,668, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH CROSSBAR SPACER AND METHOD,” U.S. Provisional Application Ser. No. 60/517,973, filed Nov. 6, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH CROSSBAR SPACER AND LATERAL IMPLANT METHOD,” U.S. patent application Ser. No. 10/685,011, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH A SPACER AND METHOD,” and U.S. Provisional Application Ser. No. 60/524,350 filed Nov. 21, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH A SPACER AND LATERAL IMPLANT METHOD,” all of which are also incorporated herein by reference.
CLAIM OF PRIORITYU.S. Provisional Patent Application Ser. No. 60/526,215 entitled: METHOD FOR REMEDIATION OF INTERVERTEBRAL DISKS, by Zucherman et al., filed Dec. 2, 2003 (Attorney Docket No. KLYCD-01082US0), and U.S. Provisional Patent Application Ser. No. 60/526,353 entitled BIORESORBABLE INTERSPINOUS PROCESS IMPLANT FOR USE WITH INTERVERTEBRAL DISK REMEDIATION OR REPLACEMENT IMPLANTS AND PROCEDURES, by James F. Zucherman et al., filed Dec. 2, 2003 (Attorney Docket No. KLYCD-01082US 1) both which are incorporated herein by reference.
BACKGROUNDThis field of art of this disclosure is an interspinous process implant.
The spinal column is a biomechanical structure composed primarily of ligaments, muscles, vertebrae and intervertebral disks. The biomechanical functions of the spine include: (1) support of the body, which involves the transfer of the weight and the bending movements of the head, trunk and arms to the pelvis and legs, (2) complex physiological motion between these parts, and (3) protection of the spinal cord and the nerve roots.
As the present society ages, it is anticipated that there will be an increase in adverse spinal conditions which are characteristic of older people. By way of example, with aging comes an increase in spinal stenosis (including, but not limited to, central canal and lateral stenosis), and facet anthropathy. Spinal stenosis typically results from the thickening of the bones that make up the spinal column and is characterized by a reduction in the available space for the passage of blood vessels and nerves. Pain associated with such stenosis can be relieved by medication and/or surgery.
In addition, to spinal stenosis, and facet anthropathy, the incidence of damage to the intervertebral disks due to injury or degeneration is also common. The primary purpose of the intervertebral disk is as a shock absorber. The disk is constructed of an inner gel-like structure, the nucleus pulposus (the nucleus), and an outer rigid structure comprised of collagen fibers, the annulus fibrosus (the annulus). At birth, the disk is 80% water, and then gradually diminishes, becoming stiff. With age, disks may degenerate, and bulge, thin, herniate, or ossify. Additionally, damage to disks may occur as a result spinal cord trauma or injury.
Given an increasing need, there is increasing attention currently focused on devices and methods for remediation of conditions of the spine. Remediation includes replacement or repair, or both of an affected part or parts of the spine, as will be discussed in more detail subsequently. Regarding the evolution of remediation of damage to intervertebral disks, rigid fixation procedures resulting in fusion are still the most commonly performed, though trends suggest a move away from such procedures. Currently, areas evolving to address the shortcomings of fusion for remediation of disk damage include technologies and procedures that preserve or repair the annulus, that replace or repair the nucleus, and that utilize technology advancement on devices for total disk replacement. The trend away from fusion is driven by both issues concerning the quality of life for those suffering from damaged intervertebral disks, as well as responsible health care management. These issues drive the desire for procedures that are minimally invasive, can be tolerated by patients of all ages, especially seniors, and can be performed preferably on an out patient basis.
Accordingly, there is a need in the art for innovation in technologies and methods that advance the art in the area of minimally invasive intervertebral disk remediation, thereby enhancing the quality of life for those suffering from the condition, as well as responding to the current needs of health care management.
BRIEF DESCRIPTION OF THE DRAWINGS
What is disclosed herein is a device that limits spinal extension without limiting spinal flexion. More specifically, the embodiments of the device disclosed herein act to limit extension (backward bending) of the spine without inhibiting the flexion (forward bending) of the spinal column.
The disclosed device is made in part or entirely from bioresorbable materials. The device is used to distract the spinous processes of adjacent vertebrae in order to increase the volume of the spinal canal, and concomitantly relieve intervertebral load. In this regard, the bioresorbable device may be used in procedures where temporary increase in spinal canal volume and relief of intervertebral load is indicated for remediation of an adverse spinal cord condition. Such distraction as a part of surgical remediation of spinal disorders may be performed either before or after the remediation procedure is performed. Remediation includes replacement or repair, or both of an affected part or parts of the spine. For example, remediation of the intervertebral disk may include either disk replacement or disk repair, as well as repair of one part of the disk; the annulus for example, and replacement of another; the nucleus for example. One feature of a bioresorbable device is that it does not require an additional surgery for removal after temporary use.
A bioresorbable material is a material that is broken down by natural processes, and removed thereby. Classes of materials that are useful as bioresorbable materials include polymers, ceramics, and glasses. Polymers of interest include polyesters, polyether esters, polycarbonates, polysaccharides, polyanhydrides, polyurethanes, and polyamide, including copolymers, composites, and blends thereof, as well as composites and blends with ceramics, glasses, and graphite, and the like. A copolymer is a polymer derived from more than one species of monomer. A polymer composite is a heterogeneous combination of two or more materials, wherein the constituents are not miscible, and therefore exhibit an interface between one another. A polymer blend is a macroscopically homogeneous mixture of two or more different species of polymer, the constituents of which are in principle separable by physical means. Fillers, which are solid extenders, may be added to a polymer, copolymer, polymer blend, or polymer composite. Fillers are added to modify properties, such as mechanical, optical, and thermal properties. For bioresorbable materials, it may be desirable to add a filler that would reinforce the material mechanically to enhance strength for certain uses, such as load bearing devices. Bioresorbable ceramics, glasses, and graphite are examples of classes of materials that are desirable for use as fillers to enhance polymer material strength. It may be desirable to add reinforcement elements to a bioresorbable polymer matrix that have the same chemical composition as the polymer matrix. In this instance, the material is referred to as self-reinforced (“SR”).
Polyesters are a diverse class of polymers with a number of bioresorbable materials of interest. Poly ether esters are a closely related group, and due to the ester functionality, share many of the same properties of members of the polyester class. Since esters are a condensation polymer, they are easily degraded by hydrolytic processes. Moreover, the materials of interest are also biocompatible materials, meaning that they cause no untoward effect to the host; e.g., excessive inflammation, thrombosis, and the like. Additionally, these bioresorbable polyesters are readily broken down in vivo and eventually excreted in a biocompatible fashion.
Polyesters meeting the criteria of biocompatible, bioresorbable materials include polymers made from monomers of hydroxy acids such as the α-hydroxylactic acid, α-hydroxyglycolidic acid, β-hydroxybutyric acid, γ-hydroxycaprolic acid, and δ-hydroxvaleric acid. Fumaric acid and hydroxyalkanes, such as propylene glycol, butylene glycol, etc., form copolymers that are also candidate bioresorbable polyesters. An example of a biodegradable poly ether ester is poly(dioxanone).
Frequently, the starting materials are condensation products of the free acids, producing cyclized structures used as the monomer starting materials. Poly(dioxanone) is formed from the cyclized monomer, p-dioxanone. For the lower molecular weight hydroxy acids, two molecules of hydroxy acid may be condensed to form a cyclized monomer. In the case of lactic acid, the corresponding cyclized condensation product of two lactic acid molecules is referred to commonly as a lactide. In the case of glycolic acid, the resultant molecule is referred to commonly as a glycolide. In this regard, whether one starts with lactic acid, or forms thereof, or with lactide, the resultant polymer is a homopolymer of lactic acid. Similarly, in the case of glycolic acid, or forms thereof, and glycolide, regardless of the starting monomer, the resultant polymer is a homopolymer of glycolidic acid. The higher molecular weight hydroxy acids can undergo an internal cyclization to form lactones that may be used as starting monomers, as can the uncyclized monomer forms. Examples of these include caproic acid, which forms εcaprolactone, and valeric acid, which forms δ-valerolactone. Again, whether the cyclized monomer, or the free acid monomer, or forms thereof are used as starting materials, homopolymers of the corresponding acids will result. In terms of the common nomenclature for designating these polymers, either form of the starting material may be used to refer to the polymer formed thereby. Hence, reference to polylactide is equivalent to polylactate, since both are homopolymers of lactic acid.
Stereoisomers of the lactic acid, and lactide exist. The properties of the copolymers formed from the stereoisomers of lactide may vary considerably. Interestingly, there is no linear relationship between properties of homopolymers, and their corresponding copolymers. In that regard, a 70:30 copolymer of poly-L-lactide with poly-D,L-lactide produces a material that has a degradation time of thirty-six months, while the degradation time of poly-D,L-lactide is about twelve months and that of poly-L-lactide is greater than twenty-four months. As another example, a 50:50 copolymer blend of glycolide with D,L lactide produces a material that degrades in about two months, while the degradation of poly-D,L-lactide and polyglycolide is about twelve months.
Major suppliers of bulk biodegradable polyester materials include Boehringer Ingelheim, Purac, and Dow. Boehringer Ingelheim's extensive RESOMER® line includes a variety of medical grade poly(L-lactide), poly(D,L-lactide), poly(L-lactide-co-D,L-lactide), poly(L-lactide-co-glycolide), poly(L-lactide-co-ε-caprolactone), poly(L-lactide-co-trimethylene carbonate), and poly(dioxanone) resins for fabrication of the disclosed device. Similarly, Purac's PURASORB® line includes lactide and glycolide monomers, as well as polylactide, polyglycolide, and polylactide/glycolide copolymer resins. Dow's Tone™ products include high molecular weight polycaprolactone resins of high crystallinity. Metabolix Inc. is a supplier of a family of poly(hydroxybutryate-co-valerate) copolymer resins under the trade name Biopol.
Polycarbonates have strength properties desirable for biocompatible, bioresorbable load bearing implants. The copolymerization of lactide or glycolide with trimethylene carbonate produces poly(lactide-co-trimethylene carbonate) and poly(glycolide-co-trimethylene carbonate), respectively. These copolymers have been used to make a range of products from sutures to tacks and screws. Tyrosine derived polycarbonates such as poly(desaminotyrosyl-tyrosine ethyl carbonate) and poly(desaminotyrosyl-tyrosine hexyl carbonate) have also been used in orthopedic applications, such as bone pins and screws. As mentioned above, Boehringer Ingelheim is a bulk supplier of a poly(L-lactide-co-trimethylene carbonate) resin, RESOMER® LT 706. Additionally, Integra Life Sciences is a supplier of tyrosine polycarbonates.
Other examples of biocompatible, bioresorbable classes of polymers are polysaccharides and polyanhydrides. Polysaccharides are a diverse class and include glucans and glycosaminoglycans. Glucans are any homopolymer of glucose, and include celluloses, starches, and dextroses. Starch blends have properties desirable for load-bearing biocompatible, bioresorbable implants. Blends exhibiting good strength characteristics include starch/cellulose acetate blends, starch/polycaprolactone blends, as well as starch blended with copolymers of ethylene and vinyl alcohol. Glucosaminoglycans includes hyaluronates, dermatan sulfates, chondroitin sulfates, heparins, keratans, chitins, and chitosans. The glucosaminoglycans are a ubiquitous class polysaccharides occurring naturally as structural materials, and show potential for as polymers and copolymers for biocompatible, bioresorbable implants. Polyanhydrides are formed by the condensation of diacid molecules. One example of a bioresorbable polyanhydride copolymer is the condensation of sebacic acid (“SA”) with hexanedecandioic acid (“HAD”) to form poly (“SA-co-HAD”) anhydride.
It should be noted that there are two important phases of the process of bioresorption: time to complete loss of strength of the material, and time to complete resorption. There are several factors that affect the rate of degradation of bioresorbable materials, and hence both the time to complete loss of strength, and time to complete resorption. In general, reduction in strength follows the reduction in molecular weight of a polymeric material as it degrades. Factors that affect degradation of bioresorbable polymers include the crystalline nature of the starting material, the hydrophilic nature of the polymer backbone, whether or not the polymer has a reinforcing filler, the initial molecular weight of the polymer, the degree of porosity of the polymer material, the surface area to mass ratio of the device, and the degree of stress on the implanted device.
An example of how the crystalline vs. amorphous nature of the starting material impact degradation is illustrated in the comparing the properties of poly-L-lactide vs. poly-D,L-lactide. The time to complete loss of strength of poly-D,L-lactide is about 6 months, while that of poly-L-lactide is more than 12 months. Recalling from the above, poly-D,L-lactide degrades more rapidly (12 months) than poly-L-lactide (24 months). The racemic mixture of the stereoisomer produces significantly amorphous powders, which yield lower strength materials degrading more rapidly than polymers made from their highly crystalline counter part. Still another example of how the crystalline versus amorphous nature of a material affects degradation time comes from the previously given example of a 50:50 copolymer blend of glycolide with D,L lactide. This copolymer exhibits a highly amorphous state, and produces a material that degrades significantly faster (two months) than the degradation of poly-D,L-lactide and polyglycolide (twelve months).
Concerning the hydrophilic nature of the polymer backbone, an example of how this property impacts degradation is demonstrated through the comparison of the stability of poly-L-lactide against polyglycolide. Poly-L-lactide has an increased hydrophobic nature (decreased hydrophilic nature) compared with polyglycolide, due to the methyl group in the backbone structure, and is therefore less susceptible to hydrolysis. The time to complete loss of strength of poly-L-lactide is greater than twelve months, while that of polyglycolide is about two months. The comparative degradation times for poly-L-lactide and polyglycolide are twenty-four months versus about six to twelve months, respectively.
The impact of reinforcing filler on increasing material strength can be understood by comparing poly-L-lactide to SR poly-L-lactide properties. Time to complete loss of strength for poly-L-lactide is greater than twelve months, while for SR poly-L-lactide is about eighteen months, while the degradation times are about twenty-four months and seventy-two months, respectively. Other types of reinforcing fillers include ceramics, glasses, and graphite fibers. Ceramics including hydroxyapaptite and tricalcium phosphate, and blends thereof are commonly used reinforcing bioresorbable materials. Bioglasses are silicate glasses containing sodium, calcium, and phosphate as the main components. Ceramics, bioglasses, and bioglass/ceramic compositions have been used in numerous polymer and copolymer bioresorbable material blends to add strength to these materials. The bioresorption of the inorganic ceramic and glass materials follows as the dissolution of the ions, and bioresorption thereof.
In addition to the molecular properties influencing material properties that impact degradation, bulk properties of the material, such as the porosity of material, as well as properties of the device, such as the surface area to mass ratio, affect degradation time, as well. As previously mentioned, there are two phases to the degradation process: time to complete loss of strength and time to complete resorption. These two phases of degradation correlate to two distinct processes: (1) water penetration into the material, with initial degradation of polymer chains, referred to as the hydrolysis phase; and (2) degradation of material strength and fragmentation, and procession of enzymatic attack, phagocytosis, and metabolism. This phase is referred to as metabolism or bulk erosion. Increased porosity of a device and increased relative surface area to mass of a device will enhance the hydrolysis phase, and hence tend to hasten the overall degradation process.
Regarding the impact of degradative processes on the site of the implant, as loss of strength proceeds, the implant will begin to fragment. Increased stress on the implant, and increased vascularization may increase the degradation time. Stress may have a role in decreasing structural integrity, and the increase in the rate of water absorption thereby, and hence affect the rate of bulk erosion. Once the polymer has fragmented into small pieces, in vivo processes, such as phagocytosis, and enzymatic activity speeding up the hydrolysis process may proceed to hasten in the bioresorption process. Such in vivo processes are enhanced by increased vascularization. The presence of the small particles, as well as a local drop in tissue pH in the case of ester hydrolysis due to increased levels of free acid, induces an inflammatory response in the tissue. When bioresorption is complete, the inflammatory response subsides. In that regard, it may be desirable, depending on the use of the device, to fabricate devices from polymers that take longer to complete loss of strength, and have slower rates of degradation.
By what is disclosed of molecular properties, bulk material properties, device design, and factors at the site of implantation, it is therefore possible to design devices from selected materials accordingly.
The following description is presented to enable any person skilled in the art to make and use the disclosed device. Various modifications to the embodiments described will be readily apparent to those skilled in the art, and the principles defined herein can be applied to other embodiments and applications without departing from the spirit and scope of the present disclosure as defined by the appended claims. Thus, the present disclosure is not intended to be limited to the embodiments shown, but is to be accorded the widest scope consistent with the principles and features disclosed herein.
An embodiment of an implant 100 of the disclosed device is depicted in
Additionally, as can be seen in
The advantage of the use of the spacer 150 as depicted in the embodiment of
As may be required for positioning the implant 100 between the spinous processes, implant 100 can also include a second wing 132 (
In another embodiment, the spacer 150 has a cross-section with a major dimension and a minor dimension, wherein the major dimension is greater than the minor dimension and, for example, less than about two times the minor dimension.
Implant 200 is depicted in
For the implants 200 of
Additionally, for the embodiments shown in
In
The implants described also can be used with other elements that further stabilize the spine and the implant's 100 location in the spine as it functions to increase temporarily the volume of the spinal canal and to relieve the intervertebral load. For example, the implants 100, 200, and 300 can be used with a tether or suture which is fitted and secured around adjacent spinous processes. The tether or suture (these terms to be used interchangeably herein) can be made of biocompatible, bioresorbable material(s) described above and as such, the tether need not be explanted, sparing the patient from additional surgery.
A first use of a tether is depicted in
A further use of the tether is depicted in
As depicted in
One use contemplated for such devices is implantation in conjunction with intervertebral disk remediation, either implanting a disk replacement device or performing surgical repair on an intervertebral disk. Devices and methods suitable for disk replacement have been described in U.S. patent application Ser. No. 10/685,134, filed Oct. 14, 2003, entitled “TOOLS FOR IMPLANTING AN ARTIFICIAL VERTEBRAL DISK AND METHOD,” U.S. patent application Ser. No. 10/684,669, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH TRANSLATING PIVOT POINT AND METHOD,” U.S. Provisional Patent Application Ser. No. 60/526,724, filed Dec. 2, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH TRANSLATING PIVOT POINT AND LATERAL IMPLANT METHOD,” U.S. patent application Ser. No. 10/684,668, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH CROSSBAR SPACER AND METHOD,” U.S. Provisional Application No. 60/517,973, filed Nov. 6, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH CROSSBAR SPACER AND LATERAL IMPLANT METHOD,” U.S. patent application Ser. No. 10/685,011, filed Oct. 14, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH A SPACER AND METHOD,” and U.S. Provisional Application Ser. No. 60/524,50, filed Nov. 21, 2003, entitled “ARTIFICIAL VERTEBRAL DISK REPLACEMENT IMPLANT WITH A SPACER AND LATERAL IMPLANT METHOD,” and are incorporated herein by reference. In addition to the total disk replacement devices described in the aforementioned applications, polymer-filled implants based on a biomimetic approach to disk repair and replacement may be used for remediation. Devices and methods describing the use of such implants are found in U.S. Pat. No. 6,416,766, issued Jul. 9, 2002, entitled “BIOLOGICAL DISK REPLACEMENT BONE MORPHOGENIC PROTEIN (BMP) CARRIERS AND ANTI-ADHESION MATERIALS,” and U.S. patent application Ser. No. 09/815,387, filed Mar. 22, 2001, entitled “IMPLANTABLE PROSTHETIC OR TISSUE EXPANDING DEVICE,” both incorporated herein by reference.
The bioresorbable load relief/spinal distraction devices disclosed above can be inserted laterally. The implanting physician after accessing the intervertebral space 810 optionally can distract the spinous process before inserting the device 830, 840. Alternatively, the tissue expander can be used to distract the spinous processes while inserting the device 830, 840.
The spinous processes can be further stabilized by the use of a bioresorbable tether together with the resorbable distracting device adapted to accept the tether 855, or with a bioresorbable device which does not have wings and need not be adapted to accept the tether 850. If the device does not have a first or second wing, the tether is looped around the spinous processes and fastened, after the implant is positioned between the spinous processes 850.
Certain of the bioresorbable devices are adapted to accept the tether so that the tether binds not only the spinous processes but also the implant, to maintain temporarily a minimum spacing between the spinous processes 855. The adaptations include an upper bore and a lower bore on the first wing, and a bore through the distraction guide. During the implantation, the device is inserted between the spinous processes with one first of the tether attached to the upper bore of the first wing. A curved needle or other tool can then be used to lead the second end of the tether over an upper spinous process, through the bore in the tissue expander, under a lower spinous process, and through the lower bore of the first wing, to fasten the second end to the lower bore of the first wing. The tether is tightened to the desired degree to maintain a minimal distraction of the spinous processes and the ends of the tether are fastened 860.
It is within the scope of the present invention to fasten the first end of the tether to the lower bore of the first wing, and to use a curved needle or other implement to lead the second end of the tether below the lower spinous process, through the bore in the tissue expander, over the upper spinous process, and through the upper bore on the first wing, to fasten the second end of the upper bore of the first wing.
Where the implant has a second wing, the same method is followed as for an implant with one wing, as the second wing need not engage the tether.
The foregoing description of embodiments of the present disclosure has been provided for the purposes of illustration and description. It is not intended to be exhaustive or to limit the disclosure to the precise forms disclosed. Many modifications and variations will be apparent to the practitioner skilled in the art. The embodiments were chosen and described in order to best explain the principles of this disclosure and its practical application, thereby enabling others skilled in the art to understand various embodiments and with various modifications that are suited to the particular use contemplated. It is intended that the scope of this disclosure be defined by the following claims and its equivalence.
Claims
1. A method for remediation of a damaged intervertebral disk, comprising the steps of:
- accessing an intervertebral space;
- restoring the damaged disk;
- inserting a bioresorbable device between spinous processes of the spinal column; and
- wherein the steps of restoring and inserting are done in any order.
2. The method of claim 1 further comprising the step of tethering the spinous processes with a bioresorbable tether.
3. The method of claim 2 wherein the tethering step further comprises threading the tether around the spinous processes and fastening the ends together.
4. The method of claim 1, where the step of inserting the device further comprises:
- accessing adjacent first and second spinal processes of the vertebrae;
- distracting the first and second spinous processes;
- implanting the device between said spinous processes, said device comprising a spacer; and
- where the distracting and implanting steps are done in any order or simultaneously.
5. The method of claim 4, wherein the step of implanting the spacer between the spinous processes further comprises;
- assembling the spacer on an insertion tool with a distal end and proximal end, the tool comprising; a distraction guide at the distal end of the insertion tool, a handle at the proximal end of the insertion tool, a central body proximal to the distraction guide, and a stop between the central body and the handle; and wherein the spacer fits over the distraction guide and is disposed between the stop and the distraction guide;
- separating tissues and ligaments with the distraction guide of the insertion tool;
- urging the spacer into the space between the spinous processes;
- removing the insertion tool, while leaving the spacer in place; and
- where the distracting and implanting steps are done in any order or simultaneously.
6. The method of claim 1, where the step of inserting the device further comprises:
- accessing adjacent first and second spinal processes of the vertebrae;
- distracting the first and second spinous processes;
- inserting a device between the spinous processes of the spinal column using the steps of: a central body with a distal end and a proximal end, said central body having a longitudinal axis; a spacer associated with the central body, wherein said spacer is adapted to be placed between spinous processes; a tissue expander extending from the distal end of the body; and where the distracting and inserting steps are done in any order or simultaneously.
7. The method of claim 1, where the step of inserting the device further comprises:
- accessing adjacent first and second spinal processes of the vertebrae;
- distracting the first and second spinous processes;
- inserting a device between the spinous processes of the spinal column, the device comprising: a central body with a distal end and a proximal end, said central body having a longitudinal axis; a stop located at the proximal end of the central body; a spacer associated with the central body, wherein said spacer is adapted to be placed between spinous processes; a tissue expander extending from the distal end of the body; and where the distracting and inserting steps are done in any order or simultaneously.
8. The method of claim 7, wherein the stop is a first wing.
9. The method of claim 8 further comprising tethering the spinous processes and the device wherein the device already is inserted between the spinous processes, and wherein the device has a bioresorbable tether anchored at a first end to the device.
10. The method of claim 9 wherein the tethering step further comprises using a tool to guide a second end of the tether over an upper spinous process, through a bore through the tissue expander, under a lower spinous process, and through a lower bore in the first wing; and anchoring the second end of the tether to the lower bore in the first wing, the first end of the tether anchored to an upper bore in the first wing.
11. The method of claim 9 wherein the tethering step further comprises using a tool to guide a second end of the tether under a lower spinous process, through a bore through the tissue expander, over an upper spinous process, and through an upper bore in the first wing; and anchoring the second end of the tether to the upper bore in the first wing, the first end of the tether anchored to a lower bore in the first wing.
12. The method of claim 8, further comprising a second wing located at the distal end of the central body, wherein the spacer is between the stop and the second wing.
13. The method of claim 12 further comprising tethering the spinous processes and the device wherein the device already is inserted between the spinous processes, and wherein the device has a bioresorbable tether anchored at a first end to the device.
14. The method of claim 13 wherein the tethering step further comprises using a tool to guide a second end of the tether over an upper spinous process, through a bore through the tissue expander, under a lower spinous process, and through a lower bore in the first wing; and anchoring the second end of the tether to the lower bore in the first wing, the first end of the tether anchored to an upper bore in the first wing.
15. The method of claim 13 wherein the tethering step further comprises using a tool to guide a second end of the tether under a lower spinous process, through a bore through the tissue expander, over an upper spinous process, and through an upper bore in the first wing; and anchoring the second end of the tether to the upper bore in the first wing, the first end of the tether anchored to a lower bore in the first wing.
16. A method for remediation of a damaged intervertebral disk, comprising:
- accessing the intervertebral space;
- inserting a device between the spinous processes of the spinal column using the steps of: accessing adjacent first and second spinal processes of the vertebrae; distracting the first and second spinous processes; implanting the device between the spinous processes; and where the distracting and implanting steps are done in any order or simultaneously; and
- replacing the intervertebral disk; and
- wherein the steps of inserting and replacing are done in any order.
17. A method for remediation of a damaged intervertebral disk, comprising:
- accessing the intervertebral space;
- inserting a device between the spinous processes of the spinal column using the steps of: accessing adjacent first and second spinal processes of the vertebrae; distracting the first and second spinous processes; implanting the device between the spinous processes; and where the distracting and implanting steps are done in any order or simultaneously; and
- repairing the intervertebral disk; and
- wherein the steps of inserting and repairing are done in any order.
18. In a method for remediation of an intervertebral disk, the improvement including the step of temporarily distracting spinous processes with the implantation of a bioresorbable spacer between the spinous processes.
19. In a method for remediation of an intervertebral disk, the improvement including the step of temporarily maintaining a minimum spacing between the spinous processes with the implantation of a bioresorbable spacer between the spinous processes.
20. The method of claim 16 wherein the inserting step includes inserting a bioresorbable device.
21. The method of claim 17 wherein the inserting step includes inserting a bioresorbable device.
22. A method for remediation of a damaged intervertebral disk, comprising the steps of:
- accessing an intervertebral space;
- restoring the damaged disk;
- inserting a device between spinous processes of the spinal column; and
- wherein the steps of restoring and inserting are done in any order.
23. The method as in claim 22 further comprising the step of tethering the spinous processes with a bioresorbable suture after the inserting step.
24. The method as in claim 22 further comprising the step of tethering the spinous processes and the device with a bioresorbable suture after the inserting step.
25. In a method for remediation of an intervertebral disk, the improvement including the step of temporarily distracting spinous processes with the implantation of a spacer between the spinous processes.
26. In a method for remediation of an intervertebral disk, the improvement including the step of temporarily maintaining a minimum spacing between the spinous processes with the implantation of a spacer between the spinous processes.
Type: Application
Filed: Nov 23, 2004
Publication Date: Sep 22, 2005
Applicant: St. Francis Medical Technologies, Inc. (Alameda, CA)
Inventors: James Zucherman (San Francisco, CA), Ken Hsu (San Francisco, CA)
Application Number: 10/996,996