WO2002068006A2

WO2002068006A2 - Cross-linked ultra-high molecular weight polyethylene for use as medical implant

Info

Publication number: WO2002068006A2
Application number: PCT/US2002/005511
Authority: WO
Inventors: Marcus Lee Scott; Shilesh Chandrakant Jani
Original assignee: Smith & Nephew, Inc.
Priority date: 2001-02-23
Filing date: 2002-02-25
Publication date: 2002-09-06
Also published as: EP1379288A2; EP2272542A3; EP2272542A2; JP2004524900A; US20030130743A1; WO2002068006A3; KR101079923B1; KR100913029B1; US6709464B2; US6547828B2; JP2010088908A; US20030127778A1; US6726727B2; CA2439270C; AU2002245513B2; CA2439270A1; CN1503682A; US20020161438A1; JP5301417B2; KR20030080025A

Abstract

The present invention relates to the prevention and decrease of osteolysis produced by wear of the ultrahigh molecular weight polyethylene (UHMWPE). Methods are disclosed for the isolation of wear particles, preparation of implants exhibiting decreased wear in comparison to conventional UHMWPE and preparation of implants that cause decreased biological response in comparison to conventional UHMWPE. The implants created by these methods are also included in the present invention.

Description

CROSS-LINKED ULTRA-HIGH MOLECULAR WEIGHT POLYETHYLENE FOR MEDICAL IMPLANT USE

BACKGROUND OF THE INVENTION Field of the Invention

The invention generally relates to the field of orthopaedic implants. Specifically the prevention and decrease of osteolysis produced by wear of ultrahigh molecular weight polyethylene (UHMWPE) bearing components. Methods are disclosed for the isolation of wear particles, preparation of implants having decreased wear and preparation of implants causing decreased biological response. The implants created by these methods are also included in the present invention.

Related Art Ultrahigh molecular weight polyethylene (UHMWPE) is commonly used as an articulating, load-bearing surface in total joint arthoplasty due to its unique array of properties. UHMWPE offers toughness, low friction coefficient, and biocompatibility. (Baker et al, 1999) Total joint prosthesis, composed of various combinations of metal, ceramic, and polymeric components, suffer from limited service lives and wear of UHMWPE is the limiting factor. It has become apparent that wear debris from UHMWPE components may be a primary contributor to osteolysis, loosening and eventual revision surgery. With steady increases in human life expectancy, there is a driving need to significantly increase the effective lifetime of a single implant. A desire to use prosthetic implants in younger patients is another strong incentive for improving the wear resistance of UHMWPE. The present invention discloses a process to improve long term wear characteristics of prostlietic implants made with UHMWPE.

When a human joint is destroyed or damaged by disease or injury, surgical replacement (arthoplasty) is normally required. A total joint replacement includes components that simulate a natural human joint, typically:

(a) a more-or-less spherical ceramic or metal ball, often made of cobalt chromium alloy;

(b) attachment of a "stem", which is generally implanted into the core of the adjacent long bone; and

(c) a hemispherical socket which takes the place of the acetabular cup and retains the spherical ball. This hemispherical joint typically is a metal cup affixed into the joint socket by mechanical attachments and is lined with UHMWPE. In this way, the ball can rotate, pivot, and articulate within the socket, and the stem, via the ball, can pivot and articulate.

One of the difficulties in constructing any device for implantation into the human body is the need to avoid adverse host biological responses. The probability of adverse host reaction is reduced when certain synthetic materials are used. For example, synthetic UHMWPE implants have minimal immunogenicity and are not toxic. However, the wear and breakdown of the UHMWPE components are known in the art to cause host cellular responses, which ultimately lead to revision surgery.

Histologic studies have demonstrated that wear of UHMWPE from orthopaedic inserts leads to several reactions. First, the tissue surrounding implants that were constructed with UHMWPE has been shown to contain extremely small particles of UHMWPE that range from sub-micron to a few microns in size. While large particles of UHMWPE appear to be tolerated by the body, as is the intact solid wall of the UHMWPE implant, the body apparently does not tolerate smaller particles of UHMWPE. In fact, the small particles of UHMWPE can cause histiocytic reactions by which the body attempts to eliminate the foreign material. Agents released during this process cause wear debris induced osteolysis. This in turn can lead to loss of fixation and loosening of he prosthesis.

Numerous techniques have been proposed to improve wear resistance of UHMWPE in orthopaedic implants. In these instances, however, many of the new versions of articulating polymers have generally failed to demonstrate significant reduction in wear and often prove to be inferior to conventional polyethylene. Recent attempts at improving wear properties of UHMWPE use special pressure/temperature processing techniques, surface treatments, formation of composites with high modulus fibers, and cross-linking via ionizing irradiation or chemical agents. Some of these attempts are summarized below.

Temperature/Pressure Treatments

Special thermal and pressure treatments have been used to increase physical performance and wear resistance of UHMWPE (e.g., U.S. Patent Nos. 5,037,928 and

5,037,938). For example, "Hipping" (Hot Isostatic Pressing), produces material alleged to comprise fewer fusion defects, increased crystallinity, density, stiffness, hardness, yield strength and resistance to creep, oxidation, and fatigue. Clinical studies, however, indicate that "Hipping" treated UHMWPE may possess inferior wear resistance in comparison to conventional UHMWPE. The inferior wear resistance being due to increased stiffness which leads to increased contact stresses during articulation (Livingston et al., Trans. ORS, 22, 141- 24, 1997).

Post-consolidation temperature and pressure treatment, such as solid phase compression molding (Zachariades, U.S. Patent No. 5,030,402), have also been attempted. Zachariades utilized solid state processing to further consolidate and orient UHMWPE chains. Resistance to wear in orthopaedic implants, however, was not improved.

Surface Treatments Focusing upon the surface of UHMWPE components, attempts have been made to decrease wear by increasing smoothness and/or lubricity of the UHMWPE components surface. A group from Howmedica used a heat pressing technique to melt the articulating surface and remove machine marks from the surface of UHMWPE components such that the "wearing in" of rough machine marks could be avoided. This modification, however, resulted in delamination and high wear due to the fact that high articulation - induced stresses were located in regions where there was a sharp transition in crystalline morphology (Bloebaum et al., Clin. Orthop. 269, 120-127, 1991).

Andrade et al. (U.S. Patent No. 4,508,606) suggested oxidizing the surface of a wet hydrophobic polymer surface to reduce sliding friction. The preferred means included applying a radio frequency glow discharge to the surface. With this technique, surface chemistries were altered by changing the time of gas plasma exposure and by altering the gas composition. The invention was proposed for the treatment of catheters to decrease surface friction properties while in a wet state. Similarly, Farrar (World Patent Application No. WO 95 212212) proposed using gas plasma treatments to cross-link the surface of UHMWPE and, thereby, increase its wear resistance. None ofthe plasma treatments, however, were practical because any perceived benefit would most likely wear away with articulation.

Composites

Because creep may be a contributor to UHMWPE wear, investigators have also included high modulus fibers in polyethylene matrices to reduce plastic deformation. (U.S. Patent No. 4,055,862 discloses a "poly-to-carbon polyethylene composite" which failed significantly via delamination. Recently, Howmedica reported that a PET/carbon fiber composite exhibited 99% less hip simulated wear than conventional polyethylene over ten million cycles. (Polineni, N.K. et al., J. 44^th Annual ORS, 49, 1998.)

Cross-Linking

Radiation Induced Cross-Linking In the absence of oxygen, the predominant effect of ionizing radiation on UHMWPE is cross-linking (Rose et al., 1984, Streicher et al., 1988). Cross-linking of UHMWPE forms covalent bonds between polymer chains which inhibit cold flow (creep) of individual polymer chains. Free radicals formed during irradiation, however, can exist indefinitely if termination by cross-linking or other forms of recombination do not occur. Furthermore, reacted intermediates are continuously formed and decayed. Exposure of these free radical species at any time (e.g., during irradiation, shelf-aging, or in vivo aging) to molecular oxygen or any other reactive oxidizing agent can result in their oxidation. Extensive oxidation leads to a reduction in molecular weight, and subsequent changes in physical properties, including wear resistance.

To reduce oxidation after gamma sterilization, some orthopaedic manufacturers have implemented techniques to irradiate their materials under conditions that encourage cross- linking and reduce oxidation. These techniques include use of inert gas atmospheres during all stages of processing, use of vacuum packaging, and post sterilization thermal treatments. Specific examples of these techniques are given below.

Howmedica has developed various means for reducing UHMWPE oxidation associated with processing, i.e., the continual use of an inert gas during processing (see U.S. Patents Νos. 5,728,748; 5,650,485; 5,543,471; 5,414,049; and 5,449,745). These patents also describe thermal annealing ofthe polymer to reduce or eliminate free radicals. The annealing temperature which is claimed (room temperature to 135 °C), however, avoids complete melting of UHMWPE.

Johnson & Johnson has disclosed in a European patent application (EP 0737481 Al) a vacuum packaging method with subsequent irradiation sterilization to promote cross-linking and reduce short- and long-term oxidative degradation. The packaging environment can contain an inert gas and/or hydrogen to "quench" free radicals. The cross- linking/sterilization method is claimed to enhance UHMWPE wear resistance (Hamilton, J.N. et al, Scientific Exhibit, 64^th AAOS Meeting, February 1997; Hamilton, J. V. et al, Trans 43^rd ORS, 782, 1997.).

Biomet's World Patent Application No. 97/29787 discloses the gamma irradiation of a prosthetic component in an oxygen resistant container partially filled with a gas capable of combining with free radicals (e.g., hydrogen).

Oonishi/Mizuho Medical Company-Japan and other investigators from Mizuho Medical Company began cross-linking PE (polyethylene) by gamma irradiation in 1971 for their SOM hip implants. Since then, they have studied the effect of a wide range of sterilization doses up to 1,000 MegaRad (MRad) on the mechanical, thennal, and wear properties of UHMWPE. They have also studied the effects of different interface materials on wear and found that alumina or zirconia heads on 200 MRad irradiated UHMWPE liners produced the lowest wear rates (Oonishi, H. et al, Radiat. Phys. Chem., 39(6), 495, 1992; Oonishi, H. et ah, Mat. Sci: Materials in Medicine, 7, 753-63, 1966; Oonishi, H. et ah, J. Mat. Sci: Materials in Medicine, 8, 11-18, 1997).

Massachusetts General Hospital/Massachusetts Institute of Technology (MGH/MIT) has used irradiation (especially electron beam) treatments to cross-link UHMWPE. These treatments reduced simulator wear rates of hip components by 80 to 95% in comparison to non-sterilized controls (see, e.g., WO97/29793). This technology enables UHMWPE to be cross-linked to a high degree; however, the degree of cross-linking is dependent upon whether the irradiated UHMWPE is in a solid or molten state. Massachusetts General Hospital/Massachusetts Institute of Technology (MGH/MIT) has also disclosed the crosslinking of UHMWPE at greater than about 1 MRad, preferably greater than about 20 MRad to reduce the production of fine particles (U.S. Patent No. 5,879,400). They disclosed a wear rate of 8 mg/million cycles for the unirradiated pin and 0.5 mg/million cycles for the irradiated (20MRad) UHMWPE pin.

Orthopaedic Hospital/University of Southern California has disclosed patent applications which seek to increase the wear resistance of UHMWPE hip components using irradiation followed by thermal treatment, such as remelting or annealing (see, U.S. Patent

No. 6,228,900; and WO 98/01085). Irradiation of the UHMWPE was disclosed at 1-100 MRad, more preferably 5-25 MRad, and most preferably 5-10 MRad. Wear rates were disclosed for various doses of irradiation. Using this method, UHMWPE cross-linking was optimized such that the physical properties were above ASTM limits.

In U.S. Patent No. 6,165,220, McKellop et al, has disclosed the crosslinking of UHMWPE at 1-25 MRad, more preferably 1-15 MRad, and most preferably 10 MRad. Oxidation profiles were given for UHMWPE crosslinked with 5, 10, or 15 MRad. They did not look at the size or number of wear particles.

BMG's European Application (EP 0729981 Al) discloses a unique processing method for decreasing friction and abrasive wear of UHMWPE used in artificial joints. The method involves irradiating UHMWPE at a low dose to introduce a small number of cross- linldng points. Irradiation is followed by uniaxial compression of melted material to achieve molecular and crystallite orientation. BMG's material demonstrated a significant reduction in pin-on-disk wear, but the reduction was not as significant as with highly cross-linked versions of UHMWPE (Oka, M. et al, "Wear-resistant properties of newly improved UHMWPE," Trans. 5^th World Biomaterials Congress, 520, 1996).

In U.S. Patent No. 6,017,975, Saum et al, has disclosed the crosslinking of

UHMWPE at 0.5-10 MRad, and more preferably 1.5-6 MRad to improve wear properties. They determined the wear rate for MRad up to 5 MRad but did not look at the size and number of wear particles. See also, U.S. Patent No. 6,242,507 to Saum et al. U.S. Patent No. 6,316,158 to Saum et al., a related application, a UHMWPE preform is pre-heated to increase the percent elongation to break and subsequently irradiated.

Yamamoto et al. discloses an analysis of the wear mode and morphology of wear particles from crosslinked ultrahigh molecular weight polyethylene. The ultrahigh molecular weight polyethylene was crosslinked at 0-150 MRad gamma irradiation. Yamamoto et al. stated that the size of both cup surface fibrils and wear debris decrease in proportion to the dose of gamma irradiation. (Yamamoto et al., Trans. 6^{1 World Biomaterials Congress, 485, 2000).

Importantly, for these methods, thermal annealing of the polymer during or after irradiation causes the free radicals (generated during irradiation) to recombine and/or form a more highly cross-linked material. Reducing or quenching free radicals is extremely important because a lack of free radicals can prevent significant UHMWPE aging. B. Chemical Cross-Linking

Like irradiation cross-linking, chemical cross-linking of UHMWPE has been investigated as a method for increasing wear resistance. Chemical cross-linking provides the benefit of cross-linking while avoiding the degradative effects of ionizing irradiation.

U.S. Patent No. 6,281,264 to Salvoey et al. teaches cross-linking, in particular chemical cross-linking, UHMWPE to increase wear resistance in orthopaedics (European Patent Application EP 0722973 Al), wliich is effected by a reduction in crystallinity as a consequence of crosslinking. Further, the crosslinked UHMWPE is taught to require a subsequent step of annealing to stabilize the size (i.e., pre-snrink the polymer). Residuals from the chemical cross-linking reaction, however, are a regulatory concern and may contribute to long-term oxidative degradation.

It remains an object of the present invention, therefore, to provide a process for treating UHMWPE for use in orthopaedic implants such that the long-term wear properties of the UHMWPE are improved.

It is another object of the present invention to provide a process for treating

UHMWPE for use in orthopaedic implants in vivo such that the performance of the implants in situ is improved.

It is well known in the published clinical literature that fine (micrometer and sub- micrometer sized) wear debris produced from bearing articulation of orthopaedic implants can elicit a macrophage cell-mediated response in the host body, wliich eventually leads to aseptic loosening of the implants and need for revision surgery. In general, bearing couples are formed from a combination of a soft material-ultra high molecular weight polyethylene (UHMWPE)-articulating against a hard material -metal or ceramic. It is the soft UHMWPE material which suffers the predominant wear in this soft-on-hard wear couple. Improvements in the wear resistance of UHMWPE, therefore, are expected to reduce the generation of fine particulate debris during articulation.

Although related art explicitly acknowledges the role particulate wear debris in the cell-mediated cascade which ultimately leads to aseptic loosening and revision surgery, it only anticipates a one-to-one relationship between improvements in gravimetric wear resistance and reduction in wear particulate debris numbers. The art explicitly or implicitly assumes a reduction in gravimetric wear will result in a concomitant reduction in the generation of wear particles. The teachings of the art do not necessarily result in the desired reductions in the generation of wear particles.

The prior art teaches that increased crosslinking energy corresponds to a decreased gravimetric wear. It presumes that this corresponds to a decrease in the number of wear particles. It also presumes that this corresponds to a decrease in the biological reaction to the wear debris produced, which may be false. The inventors ofthe present invention have found that decreased gravimetric wear does not necessarily correlate with decreased particle number and therefore may not correlate to decreased biological reaction. The present invention illustrates that there is not a continuum between crosslinking energy dose and the generation of wear particles.

The art is inadequate in having established a relationship between the absorbed radiation dose and generation of wear debris in hip simulator testing. Within the range of acceptable dose, ranging from 5 MRad (significant reduction in gravimetric wear) to 15 MRad (acceptable upper limit for material strength considerations), the 10 MRad dose has been shown to fulfill the requirement for reduced wear debris generation.

Recently, Green et al. (Green et al, 2000) found that smaller UHMWPE particles (0.24 μm) produced bone resorbing activity in vitro at a lower volumetric dose than larger particles (0.45 μm and 1.71 μm). This evidence suggests that finer wear particles may elicit a greater macrophage response than larger particles. Thus, finer wear debris generated at orthopaedic bearing couples should be fully characterized to accurately predict macrophage response. This is particularly important for new bearing materials, such as crosslinked UHMWPE, which have been reported by Bhambri et al. (Bhambri et al., 1999) to generate smaller wear particles (mean diameter of less than 0.1 μm) than conventional UHWMPE liners when tested in a hip simulator.

Because the cellular response to wear debris has been found to be dependent upon particle number and size, among other factors, the introduction of a new orthopaedic bearing material should be supported by an accurate description of wear particle parameters. The present invention teaches that filter membranes with pore sizes of no greater than 0.05 μm ensure an accurate description of particle characteristics and an indication of the biological response in vivo ofthe prosthesis comprised ofthe crosslinked UHMWPE. Prior to the present invention, an accurate method to predict the number and size of wear particles of UHMWPE generated during in vivo wear was not realized. Ηiere was an assumption in the art that increasing the radiation dose led to decreased wear resistance in vivo. However, the methods used in the art employed filters having large pore sizes (0.2 μm or greater) and, consequently, many of the smaller particles pass through the filter and were not detected. As a result, a large number of wear particles generated from wear of the UHMWPE component were over-looked, and worse, not considered by the prior art analysis methods.

SUMMARY OF THE INVENTION Therefore, it is an objective of the present invention to provide methods and medical implants related to the prevention and decrease of osteolysis produced by wear of the ultrahigh molecular weight polyethylene (UHMWPE).

An embodiment ofthe present invention is a method for isolating wear particles from an ultrahigh molecular weight polyethylene (UHMWPE) medical implant for use in the body comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting wear particles; and filtering the particles using a filter having a pore size of 0.05 μm or smaller. In other embodiments, the filter has a pore size of 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about 0.06 μm. The machining may be performed before crosslinking. The crosslinking may be performed using electromagnetic radiation or energetic subatomic particles. The crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation. In another aspect of the invention, the crosslinking may be performed using chemical crosslinking. The radiation crosslinking may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or at a dose of greater than five but less than or equal to ten MegaRad (MRad). Annealing may be performed in the melt stage. In a further aspect ofthe invention, the annealing may be performed in an inert or ambient environment. The annealing may be performed below or equal to 150°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect ofthe present invention, the annealing is performed below about 150°C and above about 140°C and the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect, the annealing may be performed at 147°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect of the present invention, the amiealing may be performed at 140°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In other embodiments of the present invention, the annealing is performed at about 141°C, at about 142°C, at about 143°C, at about 144°C, at about 145°C, at about 146°C, at about 147°C, at about 148°C, or at about 149°C. Wear testing may occur on a joint simulator. The joint simulator may simulate the hip joint or knee joint of a human. In other embodiments, the present invention may be used in other joints in the body, such as in the finger, ankle, elbow, shoulder, jaw or spine. The wear testing may occur in vivo. The harvesting may be performed using acid digestion, base digestion, or enzymatic digestion. The implant may have a polymeric structure with greater than about 300 angstrom lamellar thickness.

Another embodiment of the present invention is a method of preparing an UHMWPE medical implant for use in the body having a decreased wear particle number comprismg the steps of: crosslinking the UHMWPE; annealing the UHMWPE; and machining UHMWPE to form an implant; wherein the wear particles that are decreased in number have a diameter of 0.2 μm or less. In other embodiments, the filter employed to determine the number of wear particles has a pore size of 0.05 μm or smaller, 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about

0.06 μm. The machining may be performed before crosslinking. The crosslinking may be performed using electromagnetic radiation or energetic subatomic particles. The crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation. In another aspect of the invention, the crosslinking may be performed using chemical crosslinking. The radiation crosslinking may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or at a dose of greater than five but less than or equal to ten MegaRad (MRad). Annealing may be performed in the melt stage. In a further aspect ofthe invention, the annealing may be performed in an inert or ambient environment. The annealing may be performed below or equal to 150°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than • about 0.15 and less than about 0.20. In another aspect ofthe present invention, the annealing is performed below about 150°C and above about 140°C and the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect, the annealing may be performed at 147°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect of the present invention, the annealing may be performed at 140°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In other embodiments ofthe present invention, the annealing is performed at about 141 °C, at about 142°C, at about 143°C, at about 144°C, at about 145°C, at about 146°C, at about 147°C, at about 148°C, or at about 149°C. Wear testing may occur on a joint simulator. The joint simulator may simulate the hip joint or knee joint of a human. In other embodiments, the present invention may be used in other joints in the body, such as in the finger, ankle, elbow, shoulder, jaw or spine. The wear testing may occur in vivo. The harvesting may be performed using acid digestion, base digestion, or enzymatic digestion. The implant may have a polymeric structure with greater than about 300 angstrom lamellar thickness.

Yet another embodiment of the present invention is a method of decreasing macrophage response to an UHMWPE medical implant for use in the body comprising the steps of: performing wear particle analysis on the UHMWPE; and crosslinking the UHMWPE at a dose exhibiting the lowest particle number per million cycles of the hip simulator wherein the number of particles present was determined using a filter having a pore size of 0.05 μm or smaller. In other embodiments, the filter has a pore size of 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about 0.06 μm.

Still another embodiment of the present invention is a method of decreasing macrophage response to an UHMWPE medical implant in the body comprising crosslinking UHMWPE prior to implantation in a patient wherein the total volume of wear particles is decreased and the total number of wear particles is decreased as compared to conventional UHMWPE. The crosslinking may be performed using electromagnetic radiation or energetic subatomic particles. In an aspect of the present invention, crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation or chemical crosslinking. In another aspect of the invention, the radiation crosslinking may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or greater than five but less than or equal to ten MegaRad (MRad).

Another embodiment of the present invention is a method of decreasing osteolysis of an UHMWPE medical implant for use in the body comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the particles using a filter having a pore size of 0.05 μm or smaller; determining the number of wear particles generated; and selecting the crosslinking dose to crosslink that provides the implant having a less than about 5 x 10¹² wear particles generated per Mega cycle. The wear particles have a diameter of 1.0 μm or less, or preferably a diameter of less than 0.2 μm. In other embodiments, the filter has a pore size of 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about 0.06 μm. The machining may be performed before crosslinking. The crosslinking may be performed using electromagnetic radiation or energetic subatomic particles. The crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation. In another aspect of the invention, the crosslinking may be performed using chemical crosslinking. The radiation crosslinking may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or at a dose of greater than five but less than or equal to ten MegaRad (MRad). Annealing may be performed in the melt stage. In a further aspect ofthe invention, the annealing may be performed in an inert or ambient environment. The annealing may be performed below or equal to 150°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect ofthe present invention, the annealing is performed below about 150°C and above about 140°C and the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect, the annealing may be performed at 147°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect of the present invention, the annealing may be performed at 140°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In other embodiments of the present invention, the annealing is performed at about 141 °C, at about 142°C, at about 143°C, at about 144°C, at about 145°C, at about 146°C, at about 147°C, at about 148°C, or at about 149°C. Wear testing may occur on a joint simulator. The joint simulator may simulate the hip joint or knee joint of a human. In other embodiments, the present invention may be used in other joints in the body, such as in the finger, ankle, elbow, shoulder, jaw or spine. The wear testing may occur in vivo. The harvesting may be performed using acid digestion, base digestion, or enzymatic digestion. The implant may have a polymeric structure with greater than about 300 angstrom lamellar thickness. Characterization may be by a Mgh resolution microscopic method including, but not limited to, scanning electron microscopy, or an automatic particle counter.

Another embodiment of the present invention is a method of decreasing osteolysis of an UHMWPE medical implant for use in the body comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the particles using a filter having a pore size of 0.05 μm or smaller; determining a total particle surface area or the wear particles; and selecting the crosslinking dose that provides the implant having a less than about 1.17 m²/Mega cycle total particle surface area less. Machining is performed before said crosslinking. In other embodiments, the filter has a pore size of 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about 0.06 μm.

Yet another embodiment of the present invention is a method of decreasing macrophage response to a UHMWPE medical implant for use in the body comprising the steps of crosslinking the UHMWPE; simulating use in a host; and testing serum for wear particles using a filter having a pore size of 0.05 μm, wherein the number of wear particles having a diameter of less than 0.2 μm are decreased as compared to conventional UHMWPE. In other embodiments, the filter has a pore size of 0.04 μm, of 0.03 μm, of 0.02 μm, or 0.01 μm. In certain embodiments, the filter has a pore size that is less than 0.2 μm, including a pore size of about 0.19 μm, about 0.18 μm, about 0.17 μm, about 0.16 μm, about 0.15 μm, about 0.14μm, about 0.13 μm, about 0.12 μm„ about 0.11 μm, about 0.10 μm, about 0.09 μm, about 0.08 μm, about 0.07 μm, or about 0.06 μm.The machining may be performed before crosslinking. The crosslinking may be performed using electromagnetic radiation or energetic subatomic particles. The crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation. In another aspect of the invention, the crosslinking may be performed using chemical crosslinking. The crosslinking may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or at a dose of greater than five but less than or equal to ten MegaRad (MRad). The annealing step is performed below or equal to 150 °C. In other embodiments of the present invention, the annealing is performed at about 141°C, at about 142°C, at about 143°C, at about 144°C, at about 145°C, at about 146°C, at about 147°C, at about 148°C, or at about 149°C. Wear testing may occur on a joint simulator. The joint simulator may simulate the hip joint or knee joint of a human. In other embodiments, the present invention may be used in other joints in the body, such as in the finger, ankle, elbow, shoulder, jaw or spine.

Still another embodiment of the present invention is a cross-linked UHMWPE medical implant for use in the body that exhibits decreased osteolysis (or macrophage response) in comparision to conventional treatment of UHMWPE due to a particle number of less than 5 X 10¹² per Mega cycle upon testing for wear resistance.

Another embodiment of the present invention is an UHMWPE medical implant for use in the body having a decreased wear particle number of particles created by the steps comprising of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the wear particles using a filter having a pore size of 0.05 μm or smaller; determining the number of wear particles; and selecting the crosslinldng dose to crosslink the implant to provide a number of wear particles generated less than about 5 x 10¹² per Mega cycle. The wear particles generated and are decreased in number having a diameter of 0.2 μm or less. In other embodiments, the filter has a pore size of 0.04 μm or smaller, of 0.03 μm or smaller, of 0.02 μm or smaller, or 0.01 μm or smaller. The machining may be performed before crosslinldng. The crosslinldng may be performed using electromagnetic radiation or energetic subatomic particles. The crosslinking may be performed using gamma radiation, electron beam radiation, or x-ray radiation. In another aspect of the invention, the crosslinking may be performed using chemical crosslinking. The crosslinking by radiation may be at a dose of greater than five but less than or equal to fifteen MegaRad (MRad) or at a dose of greater than five but less than or equal to ten MegaRad (MRad). Annealing may be performed in the melt stage. In a further aspect of the invention, the annealing may be performed in an inert or ambient environment. The annealing may be performed below or equal to 150°C. The crosslinldng may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect of the present invention, the annealing is performed below about 150°C and above about 140°C and the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect, the annealing may be performed at 147°C. The crosslinking may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In another aspect ofthe present invention, the annealing may be performed at 140°C. The crosslinldng may be sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10 or greater than about 0.15 and less than about 0.20. In other embodiments of the present invention, the annealing is performed at about 141°C, at about 142°C, at about 143°C, at about 144°C, at about 145°C, at about 146°C, at about 147°C, at about 148°C, or at about 149°C. Wear testing may occur on a joint simulator. The joint simulator may simulate the hip joint or knee joint of a human. In other embodiments, the present invention may be used in other joints in the body, such as in the finger, ankle, elbow, shoulder, jaw or spine. The wear testing may occur in vivo. The harvesting may be performed using acid digestion, base digestion, or enzymatic digestion. The implant may have a polymeric structure with greater than about 300 angstrom lamellar thickness. In another aspect of the invention, the characterization may be by a high resolution microscopic method or an automatic particle counter. In a further aspect of the present invention, the characterization may be by scanning electron microscopy or automatic particle counter.

One embodiment of the present invention provides a total joint prosthesis comprising a bearing surface comprised of crosslinked UHMWPE that generates less than about 5 x 10¹² wear particles per Mega cycle of wear; and a counterb earing surface comprised of ceramic. The bearing surface and the counterbearmg surface articulate directly and, as a result of the articulation, generate wear particles. The ceramic counterbearmg surface comprises zirconia. The wear particle analysis ofthe present invention predicts the wear in vivo of the total joint prosthesis and indicates the crosslinldng dose that provides the bearing surface therein. The joint prosthesis ofthe present invention includes, but is not limited to, a joint in the hip, knee, finger, ankle, elbow, shoulder, jaw or spine.

As used herein the specification, "a" or "an" may mean one or more. As used herein in the claim(s), when used in conjunction with the word "comprising", the words "a" or "an" may mean one or more than one. As used herein "another" may mean at least a second or more.

Other objects, features and advantages of the present invention will become apparent from the following detailed description. It should be understood, however, that the detailed description and the specific examples, while indicating preferred embodiments of the invention, are given by way of illustration only, since various changes and modifications within the spirit and scope of the invention will become apparent to those skilled in the art from this detailed description.

BRIEF SUMMARY OF THE DRAWINGS

The following drawings form part of the present specification and are included to further demonstrate certain aspects of the present invention. The invention may be better understood by reference to one or more of these drawings in combination with the detailed description of specific embodiments presented herein: Figure 1. SEM micrographs at 10,000X of (a) digested and filtered deionized water and (b) digested and filtered knee simulator serum.

Figure 2. Number of particles per field vs. measured UHMWPE wear for simulator- tested tibial inserts.

Figure 3. Average particle volume per field (V_FIELD) vs. UHMWPE wear for simulator-tested tibial inserts.

Figure 4. Fourier transform infrared spectra of particles recovered from serum, HDPE reference material, and the KBr background.

Figure 5. Scanning electron micrograph of wear debris isolated from hip simulator serum and recovered on a 0.2 μm pore size filter membrane.

Figure 6. Scanning electron micrograph of wear debris isolated from hip simulator serum and recovered on a 0.05 μm pore size filter membrane.

Figure 7. Size distribution of the particles recovered on the 0.2 μm pore size filter membranes.

Figure 8. Size distribution of the particles recovered on the 0.05 μm filter pore size membranes.

Figure 9. Particles generated per million cycles using 0.2 μm filtration.

Figure 10. Particles generated per million cycles using 0.05 μm filtration.

Figure 11. SEM micrographs of UHMWPE particles extracted from serum

Figure 12. Particle number vs. size histogram.

Figure 13. Particle volume vs. size histogram.

Figure 14. Trans-vinylene indices for gamma-irradiated and subsequently annealed UHMWPE.

Figure 15. Cumulative gravimetric wear vs. cycle count for 140-XLPE liners tested against CoCr and zirconia femoral heads. Figure 16. Representative SEM micrograph of wear particles generated from 140- XLPE liners tested against CoCr and zirconia femoral heads.

Figure 17. Mean numer of particles generated per cycle of testing for 140-XLPE liners.

Figure 18. Number of wear particles generated per cycle as a function of particle diamert for C-PE, 147-XLPE and 140-XLPE liners tested against CoCr femoral heads.

Figure 19. Number of wear particles generated per cycle as a function of particle diamert for C-PE, 147-XLPE and 140-XLPE liners tested against zirconia femoral heads.

Figure 20. SEM micrographs of wear particles generated from C-PE liners articulated against smooth CoCr (A), smooth zirconia (B), and roughened CoCr (C) femoral heads.

Figure 21. SEM micrographs of wear particles generated from 10-XLPE liners articulated against smooth CoCr (A), smooth zirconia (B), and roughened CoCr (C) femoral heads.

DETAILED DESCRIPTION OF THE INVENTION

Definitions

Annealing, as used herein, refers to heating a sample, such as UHMWPE, and then allowing the sample to cool. Thermal annealing of the sample during or after crosslinldng by, for example, gamma radiation causes the free radicals (generated during gamma radiation) to recombine and/or form a more highly cross-linked material.

Characterizing the wear particles, as used herein, refers to determining the size, shape, number, and concentration of the wear particles. It may include the use of, but is not limited to, using a microscopic method such as scanning electron microscopy, or an automatic particle counter.

Decreased or increased, as used herein, refers to a decrease or increase in a parameter in comparison to that parameter in conventional (not crosslinked) polyethylene.

Dose, as used herein, refers to the amount of radiation absorbed by the sample, such as UHMWPE. Gravimetric, as used herein, refers to the measuring of weight loss.

In vivo, as used herein, refers to an activity occurring within the body of a subject, preferably a human subject.

Lamellar thickness, as used herein, is the depth of the layers of alternate amorphous and crystalline regions. The lamellar thickness (1) is the calculated thickness of assumed lamellar structures in the polymer using the following expression:

/ = (2 -σ_e ^■ T_m°) I (ΛH-(T_m° - T_m)φ)

where σ_e is the end free surface energy of polyethylene (2.22 x 10^"6 cal/cm²), - H is the heat of melting of polyethylene crystals (69.2 cal g), p is the density of the crystalline regions (1.005 g/cm³), and T_m° is the melting point of a perfect polyethylene crystal (418.15 K).

Macrophage response, as used herein, refers to an adverse reaction that may lead to osteolysis of an implant.

Medical implant, as used herein, refers to a synthetic replacement device for a body and all the components thereof.

MegaRad (MRad), as used herein, refers to a unit of measure for the energy absorbed per unit mass of material processed by radiation (absorbed dose). The radiation dose may be within an error of ± 10%. A MegaRad is equivalent to 10 kiloGray (kGy). As used herein, the term "radiation" is used interchangeably with the term "irradiation."

Osteolysis, as used herein, refers to the reabsorption of bone.

Trans-vinylene index (TVI), as used herein, is a based upon the concentration of trans-vinylene units (TNU) which have been shown to be linear with absorbed radiation dose for polyethylene at low dose levels. The concentration of TNU and thus the TNI, can be used to determine the level of crosslinking in UHMWPE. It can be used to determine the absolute dose level received during the crosslinldng of UHMWPE. The TNI is calculated by normalizing the area under the trans-vinylene vibration at 965 cm^"1 to that under the 1900 cm^" ¹ vibration. Ultra high molecular weight polyethylene, as used herein, refers to polyethylene having a molecular weight greater than 1.75 million.

Wear debris, as used herein, refers to particles generated from the articulation of joint components, specifically a bearing surface and a counterbearing surface, and is used interchangeably with the terms "wear particles" and "particulate debris".

Wear resistance, as used herein, refers to the property of resisting physical changes in the material due to articulation.

Wear testing, as used herein, articulating joint components. Wear testing includes testing in water, synovial fluid, or any lubricant.

Crosslinked ultrahigh molecular weight polyethylene (UHMWPE) and implants are useful as prostheses for various parts of the body, such as components of a joint in the body. For example, in the hip joints, a component of an implant can be a prosthetic acetabular cup (as exemplified above), or the insert or liner ofthe cup, or a component of a hirnnion bearing (e.g. between the modular head and the stem). In the knee joint, they can be a prosthetic tibial plateau (femoro-tibial articulation), patellar button (patello-femoral articulation), and trunnion or other bearing components, depending on the design of the artificial knee joint. For example, in knees of the meniscal bearing type, both the upper and lower surfaces of the UHMWPE component may be surface-crosslinlced, i.e., those surfaces that articulate against metallic or ceramic surfaces. In the anlde joint, they can be the prosthetic talar surface (tibio- talar articulation) and other bearing components. In the elbow joint, they can be the prosthetic radio-humeral joint, ulno-humeral joint, and other bearing components. In the shoulder joint, they can be used in the glenoro-humeral articulation, and other bearing components. In the spine, they can be used in intervertebral disk replacement and facet joint replacement. They can also be made into temporo-mandibular joint (jaw) and finger joints. The above are by way of example, and are not meant to be limiting. This application often uses UHMWPE and acetabular cup implants as examples of UHMWPE and implants, respectively. However, it is to be understood that the present invention would be applicable to PE in general; and to implants in general. Osteolysis is a common long-term complication in total hip replacement (THR) (Harris, 1995) and has been linked to wear debris generated from ultra high molecular weight polyethylene (UHMWPE) acetabular liners (Amstutz et al, 1992; Schmalzried et al, 1992; Willert et al, 1990; and Goldring et al, 1983). While the response of periprosthetic tissue to wear debris is not fully understood, macrophage response to particulate wear debris is believed to be an important factor in osteolysis (Goodman et al, 1998; Jasty et al, 1994; Chiba et al, 1994; and Jiranek et al, 1993). It is well established that the cellular response to wear debris is dependent upon particle number, shape, size, surface area, and material chemistry, among other factors (Green et al, 1998; Gonzalez et al, 1996; and Shanbhag et al, 1994). The introduction of new bearing materials, such as crosslinked UHMWPE, should therefore be supported by accurate descriptions ofthe number, size distribution, surface area, and volume of wear particles generated.

Various techniques have been developed to isolate UHMWPE wear particles from periprosthetic tissue and joint simulator serum. Common protocols involve digestion of tissue or serum samples in either a strong base or acid, followed by filtration of the digests through filter membranes with a pore size of 0.2 μm (McKellop et al, 1995; Campbell et al, 1995; and Niedzwiecld et al, 1999). A scanning electron microscope (SEM) is used to determine the numbers, sizes, and shapes of particles deposited on the filter membrane. Previous analyses of particles recovered from the periprosthetic tissues of THR patients and from hip simulator serum indicated that the mode of the particle size distribution was at or below the pore size (0.2 μm) of the filter membrane (McKellop et al, 1995). Thus, a significant number of particles having a diameter below 0.2 μm may have passed through the filter pores and not been detected during the analyses. It is therefore hypothesized that the number of UHMWPE particles generated by THR bearing components are underestimated by particle isolation techniques wliich involve filtration of debris through a 0.2 μm filter membrane.

In the present invention, hip simulator testing was conducted on three classes of materials (1) conventional (non-irradiated) UHMWPE (C-PE), (2) 5 MRad gamma irradiation crosslinked UHMWPE (5-XLPE), and (3) 10 MRad gamma irradiation crosslinlced UHMWPE (10-XLPE). According to published literature, 5-XLPE and 10-XLPE are both expected to exhibit enhanced wear resistance compared to C-PE, with the degree of improvement increasing with increasing radiation dose. Gravimetric analyses showed the expected trends to hold up to a duration of 15 million cycles tested to-date. However, when analyzed for particulate debris, it was discovered that the 5-XLPE material began to generate more wear debris than C-PE approximately at approximately 5 million cycle. The 10-XLPE material, on the other hand, showed fewer particles for the entire duration of testing. Crosslinldng affects the size of particles. It is ideal to decrease the total volume of particles and the number of particles at all sizes.

Crosslinking of UHMWPE

The wear process in an artificial joint is a multi-directional process. Crosslinking is achieved by using high doses of radiation. In the absence of oxygen, crosslinldng is the predominant effect of ionizing radiation on UHMWPE (Rose et al, 1984, Streicher et al, 1988). Crosslinking of UHMWPE forms covalent bonds between polymer chains which inhibit cold flow (creep) of individual polymer chains. Crosslinldng UHMWPE provides a lower wear rate because the polymer chains form a network that is more stable to multidirectional movements. When irradiated at temperatures above 150°C, a permanent intermolecular homogeneous network is formed. Exposure of UHMWPE to radiation results in the cleavage of carbon-carbon and carbon-hydrogen bonds within the polyethylene chains. Such radiation includes but is not limited to energetic subatomic particles, gamma, electron beam, or x-ray radiation. Gamma radiation is known to break polymer chains and create free radicals, that react with oxygen in the atmosphere or synovial fluid. This oxidation reaction causes further chain scission and leads to the formation of an embrittled region close to the polymer surface (Buchanan et al, 1998, Materials Congress 1998, p.148). Oxidation of free radicals formed during the step of radiation crosslinldng leads to a reduction in molecular weight, and subsequent changes in physical properties, including wear resistance. Formation of free radicals during the step of radiation crosslinking primarily include a combination of alkyl and allyl type free radicals. In the presence of oxygen, however, a small fraction of peroxy radicals are also formed. To reduce the formation of peroxy radicals, the process is performed under vacuum or in the presence of an inert gas, such as argon. Free radicals can be removed through either addition of antioxidants or through remelting. Remelting is a process in which the implants are reheated to increase chain mobility, so the free radicals can recombine or terminate. The overall industrial process is to radiate polymer sheets, which are remelted. From the remelted sheets implants are machined and thereafter sterilized. It is well known in the art that crosslinldng of UHMWPE by a number of means, including radiation with energetic beams (gamma rays, electron beams, x-rays, etc.,) or by chemical means, such as a chemical crosslinking compound that initiates formation of free radicals in the sample, improves the wear resistance ofthe material. Although clinical use of crosslinked UHMWPE was first reported in the 1970's it was not until the mid 1990's that anatomic joint (hip and knee) simulator tests were conducted to demonstrate the enhanced wear resistance of crosslinked UHMWPE. The extant literature and art teaches methods by which UHMWPE can be crosslinked to varying degrees and demonstrates improvements in wear resistance in joint simulator testing.

The present invention includes all forms of crosslinldng, crosslinldng at all temperatures, crosslinldng in the presence or absence of an inert environment, and in the presence or absence of free-radical scavengers. Crosslinldng may occur before or after the implant is formed (machined).

Macrophage response and osteolysis The major cause of late-term implant failure is implant induced osteolysis and aseptic loosening of hip replacements. Osteolysis is the reabsorption of bone, in this case due to a reaction to polyethylene wear debris. The majority of wear particles produced by implants are thought to be submicron in size. Patient tissue examined in revision operations show a periprosthetic pseudo-membrane containing macrophages and multinucleated giant cells (osteoclasts, which can be viewed as specialized macrophages) associated with polyethylene particles. The wear debris stimulates macrophages to produce mediators of osteolysis which causes aseptic loosening ofthe implant. Mediators produced by the macrophages include IL- lβ, IL-6, TNFα, GM-CSF, PGE₂, and enzymes such as collagenase. IL-6 stimulates the formation of osteoclasts and thus stimulates bone resorption. IL-lβ stimulates proliferation and maturation of progenitor cells into osteoclasts. IL-lβ also stimulates osteoblasts causing maturation of the osteoclast into multinucleate bone reabsorbing cells. TNFα has much the same function as ILlβ in this situation (Green et al, 1998). The ruffled border of osteoclasts releases acids and hydrolytic enzymes that dissolve proteins and minerals. Osteoblasts create bone by synthesizing proteins. Osteoblasts secrete collagenase, which may facilitate osteoclast activation. Osteoblasts produce TGFβ, IGFl, IGF2, PDGF, ILl, FGF, TNFα that regulate growth and differentiation of bone (Pathology, Rubin, Second Ed. 1994; Essential Medical Physiology, Johnson, 1992). The biological activity of polyethylene wear debris is dependent upon the size and number of particles present (Matthews et al, 2000 Biomaterials, p. 2033). Matthews et al. found particles ofthe size 0.24, 0.45, and 1.7 μm to be the most biologically active. This finding was based on cell studies in which the wear debris was filtered over 10, 1.0, 0.4, and 0.1 μm pore size filters. Wear particles were co- cultured with donor macrophages and the production of mediators was measured. The specific biological activity (SB A) ofthe wear debris is calculated using the equation:

SBA=[B(r) x C(c)]₀.ι-ι.oμm + [B(r) x C(c)] ₀ μm + [B(r) x C(c)]₁₀-₁₀₀ μm

Where B(r) is the biological activity function of a given particle size and C(c) is the volumetric concentration of the wear debris for a given particle size. The functional biological activity (FBA) is the product of he wear volume and the SB A (Fisher et al, 2000 46^th ORS Meeting).

Methods of wear analysis

Joint simulator wear testing of orthopaedic bearing components reproduces in vivo wear mechanisms. A common means of verifying the reproduction of clinical wear mechanisms is to compare the wear debris of laboratory and retrieved specimens (McKellop et al., 1995). UHMWPE debris can be isolated from both retrieved periprosthetic tissue and simulator-tested serum using a method developed by Campbell et al. (Campbell et al, 1995).

This widely accepted method uses base digestion of the serum, centrifugation, and density gradients to isolate UHMWPE debris. However, the process is labor intensive and expensive.

An alternative method for isolating UHMWPE wear debris from simulator-tested serum includes an acid treatment and vacuum filtration to isolate particles (Scott et al, 2000).

Collected wear debris can then be mounted, sputter coated with gold, and analyzed by scanning electron microscopy (SEM). SEM can be used to determine the numbers, size, and shapes of particles. FTIR spectra of the debris can be compared with those of a control substance, such as HDPE, to determine the identity ofthe wear debris.

Gravimetric measurement

Wear resistance can also be defined and determined by gravimetric means, by measuring the weight loss ofthe UHMWPE component at fixed intervals ofthe test duration. Gravimetric measurement provides the change in weight from before testing to after testing. The gravimetric wear rate is defined in milligrams/million cycles of the simulator. It provides a measurement ofthe total mass of debris generated from wear surfaces. It does not give any information regarding the size and number of wear particles. This method is not accurate when the material absorbs fluid. UHMWPE does absorb fluid. It was previously believed that gravimetrically measured reduction in wear translated into reduction in particle generation. Thus, it was assumed that a decrease in weight loss correlated with decreased wear and decreased particle characteristics. Therefore, it would be expected that there would be a decrease in osteolysis as well. There is no predictable relationship between total wear mass and particulate number. This is explained by the following equation:

N V total wear ⁼ __j Y each particle

H

where N is the number of particles. For instance, if crosslinldng reduces the average volume of individual particles, then a greater number of particles will be produced per unit volume of total wear. On the other hand, if crosslinldng increases the average particle volume, then there are fewer particles per unit volume of total wear. Thus, particle size dictates the number of particles produced per unit volume of total wear. Gravimetric methods cannot measure individual particle parameters such as size, volume and number. Thus, gravimetric techniques are limited and do not provide a means to measure and evaluate these individual particle characteristics.

Joint simulators Joint simulators include hip simulators, knee simulators and other joint simulators. In one use of a hip simulator, UHMWPE acetabular liners are articulated against CoCrMo heads. Commercially available acetabular liners are machined from ram-extruded UHMWPE and sterilized using ethylene oxide. The liners were inserted into Ti-6A1-4V acetabular shells and tested against 32 mm diameter CoCr femoral heads. The bearing couples are tested under physiological loading and motion conditions (Bergmann et al, 1993; Johnston and Schmidt, 1969; and ISO/CD 14242-1.2) on a 12-station hip simulator. Test duration can range from 1 million to 30 million cycles (Mcycles) at a cyclic frequency of 1 Hz, representing 1 to 30 years of normal service in the human host. The test lubricant is bovine serum containing 0.2% sodium azide and 20 mM EDTA. The test serum is replaced approximately every 500,000 cycles. EXAMPLES

The following examples are included to demonstrate preferred embodiments of the invention. It should be appreciated by those skilled in the art that the techniques disclosed in the examples which follow represent techniques discovered by the inventor to function well in the practice of the invention, and thus can be considered to constitute preferred modes for its practice. However, those of skill in the art should, in light of the present disclosure, appreciate that many changes can be made in the specific embodiments which are disclosed and still obtain a like or similar result without departing from the concept, spirit and scope of the invention. More specifically, it will be apparent that certain agents that are both chemically and physiologically related may be substituted for the agents described herein while the same or similar results would be achieved. All such similar substitutes and modifications apparent to those skilled in the art are deemed to be within the spirit, scope and concept ofthe invention as defined by the appended claims.

Example 1. Validation of an Acid Digestion Method for Isolating UHMWPE Wear Debris from Joint Simulator Serum

The particle isolation method was performed on the following samples: (1) deionized water; (2) untested bovine calf serum; (3) deionized water pumped through silicone tubing at 37°C for one week; and (4) simulator-tested serum from four separate stations on an AMTI knee simulator. The sera from the knee simulator were harvested at about 500,000 cycles and contained between 1 and 20 mg of UHMWPE debris (as determined by weight loss of UHMWPE tibial inserts). Ten ml of each sample was added to 40 ml of 37% HC1. A magnetic stir bar was added to the solution and stirred at 350 rpm at 50°C for approximately one hour. At this time, 1 ml of the solution was removed and added to 100 ml of methanol. This solution was then filtered through a 0.2 μm pore size polycarbonate filter membrane. The filter membranes were mounted on metal microscope stubs, sputter coated with gold, and imaged using a scanning electron microscope (SEM). Image analysis was performed at 10,000X in order to determine contamination levels ("blank" samples 1 though 3) and to correlate observed wear with particle count density (simulator-tested sera). For each of the simulator-tested samples, a minimum of 500 particles and 20 fields of view were analyzed, and the particle count density was expressed in average number of particles per field. Additionally, the average particle volume per field (V_FIELD) was calculated by dividing the total volume of analyzed particles in a sample by the number of fields needed to image all the particles. The volume of each particle was estimated using the following equation:

V_PARTICLE = 4/3 TC (ECR)³,

where ECR is the radius of a circle having the same area as the measured feature.

A representative SEM image of the filter membrane through which the digested deionized water sample was passed is shown in Figure la. At 10,000X, no particles were seen on the filter membrane, indicating an absence of contaminants within the reagents used in the procedure. The filter membrane through which the digested untested serum was passed had a similar appearance, indicating that the proteins in the serum were completely digested by the HC1. Filtration of the water sample that was pumped through silicone tubing also resulted in an absence of particles. This suggests that the tubing though which serum is circulated in joint simulators releases insignificant levels of silicone debris. The digested sera from the knee simulator showed particulate material that was comprised of two predominant morphologies, spheroids and fibrils (Figure lb).

Quantitative image analysis revealed that the number of particles per field correlated strongly (R² = 0.997) with measured UHMWPE wear for the simulator-tested serum samples (Figure 2). The average particle volume per field of view also correlated strongly (R² = 0.983) with measured UHMWPE wear (Figure 3).

Example 2. Hip Simulator Specimens and Parameters

Commercially available acetabular liners were machined from ram-extruded GUR 1050 UHMWPE (Poly-Hi Solidur, Ft. Wayne, IN) and sterilized using ethylene oxide. The liners were inserted into TΪ-6A1-4V (ISO 5832) acetabular shells and tested against 32 mm diameter CoCr femoral heads (ASTM F799). The bearing couples (n=3) were tested under physiological loading and motion conditions (Bergmann et al, 1993; Johnston and Schmidt, 1969; and ISO/CD 14242-1.2) on a 12-station AMTI (Watertown, MA) hip simulator. Testing was conducted to 12 million cycles (Mcycles) at a cyclic frequency of 1 Hz. The test lubricant was bovine serum (Hyclone Laboratories, Logan, UT) which contained 0.2% sodium azide and 20 mM EDTA. The test serum was replaced approximately every 500,000 cycles.

Example 3. Isolation of UHMWPE Particles Eight serum samples were harvested during the 12 million cycle test. The test interval

(in cycles) for each serum sample is listed in Table 1. Each sample was collected in an Erlenmeyer flask containing a stirbar and stirred overnight at 350 rpm. Ten ml of serum was then added to 40 ml of 37% w/V HCl and stirred for one hour at 50°C. One ml of the digested solution was added to 100 ml of methanol, which was then filtered through a 0.2 μm pore size polycarbonate filter membrane. A replicate digest was filtered through a 0.05 μm pore size membrane for each serum sample.

Table 1. Data on Serum Samples Harvested from a Hip Simulator.

Serum Testing Interval N_F ^" NF^'" Nc⁸ (10°) Nc* (10°) Sample (10⁶ cycles) (0.2 μm (0.05 μm (0.2 μm (0.05 μm pore size pore size pore size pore size filters) filters) filters) filters)

1 0.580 - 1.064 49.6 157.5 2.7 8.7

2 4.021 - 4.461 48.2 173.5 2.9 10.5

3 8.006 - 8.628 54.7 117.9 2.3 5.1

4 9.228 - 9.717 49.2 98.5 2.7 5.4

5 10.289 - 10.837 47.8 137.3 2.3 6.7

6 10.289 - 10.837 44.7 105.3 2.2 5.1

7 11.369 - 11.972 64.9 102.8 2.9 4.5

8 11.369 - 11.972 54.6 117.1 2.4 5.2

Average 51.7 126.2 2.6 6.4

Std. Dev. 6.3 27.4 0.2 2.2

*The mean number of particles per field of view (10,000X magnification) is denoted N_F. §The mean number of particles generated per cycle is denoted N_c.

Example 4. Characterization of Particle Size and Number

Each filter membrane was mounted on an aluminum stub, sputter coated with gold, and examined using a SEM (S360, Leica, Inc., Deerfield, IL). Images were taken at a magnification of 10,000X and transferred to a digital imaging system (eXL II, Oxford Instruments, Ltd., England). A minimum of twenty fields of view were analyzed per filter membrane. Particle diameter (Dp) was calculated based on the projected area (A) of each particle. This parameter was based on circular geometry and calculated as follows:

Dp = 2 (A / π) 1/2

(1)

For each filter membrane, the mean number of particles per field of view (N_F) was determined, and the number of particles generated per cycle of testing (Nc) was calculated as follows:

Nc = N_F (AFILTER / AFIELD) d / C (2) where AFI_LTER = area of filter membrane = 962 mm²; A_FIELD = area of field of view = 9.0xl0^"5 mm²; d = dilution ratio = 2500; and c = number of test cycles. For each type of filter membrane, the data from the different digests were pooled. The particle diameter data were presented as the mean, median, mode, and standard deviation. The number of particles per cycle was presented as the mean and standard deviation. Significant differences (ANOVA; α = 0.05) in mean particle parameters were determined between the particles deposited on the 0.2 μm and 0.05 μm pore size filter membranes. The Kruskal-Wallis test was used to determine significant differences in median particle diameter between the two filter membranes.

Example 5. Reproducibility of Particle Isolation Method For the acid digestion vacuum filtration method used in this study, a strong linear correlation has been demonstrated between measured wear volume (as determined gravimetrically) and the volume of particles recovered from a total joint simulator (Scott et al, 2000). For digests filtered through a 0.05 μm pore size filter membrane, inter-observer reproducibility has been found to be within 10% of the mean value for each of the following parameters: (i) number of particles generated per cycle of testing; and (ii) mean particle diameter (Table 2).

Table 2. Wear Particle Data Demonstrating Interobserver Reproduciblity for Two Serum Samples Harvested from a Hip Simulator (Mean ± Std. Dev.).

Serum Mean Particle Diameter Mean Particle Diameter

Sample N_F ^* NF^* (μm) (μm)

Observer 1 Observer 2 Observer 1 Observer 2

A 123.6 + 20.8 123.8 + 45.0 0.11 + 0.12 0.12 + 0.14 B 76.3 ± 12.0 78.1 ± 21.2 0.20 + 0.29 0.22+ 0.32

*The mean number of particles per field of view (10,0OOX magnification) is denoted N_F.

Example 6. Verification of Particle Identity

Fourier transform infrared spectroscopy (FTIR) was performed to determine the identity of wear debris from tliree ofthe serum samples. In each case, approximately one mg of particles was transferred from the filter membranes onto a KBr disk and identified using a FTLR spectrometer with an attached infrared microscope (FTS165 spectrometer, UMA250 microscope, Bio-Rad Laboratories, Hercules, CA). The FTIR spectra ofthe particles isolated from serum were compared with that of a commercially available HDPE powder (Shamrock Technologies Inc., Newark, NJ).

Example 7. Current Wear Particle Procedure Underestimate the Number of Particles Generated by Prosthetic Bearing Components

UHMWPE liners were articulated against CoCrMo heads on an anatomic hip simulator up to 12 million cycles. Serum samples were periodically harvested and subjected to a validated acid digestion method Scott et al, 2000). Replicate digests were vacuum filtered through either a 0.2 μm or 0.05 μm pore size filter membrane. Relative differences in the particle number and size distribution were determined for each membrane pore size.

The recovered particles were characterized using Fourier transform infrared spectroscopy (FTIR) and scanning electron microscopy. The FTIR spectra of the particles recovered from the hip simulator sera were similar to that of the reference HDPE material and consistent with UHMWPE in that they had major peaks around 2917, 2850, 1470, and 721 cm^"1 (Figure 4) (Painter et al, 1982). Extraneous peaks and valleys were found to correspond with the peak positions of the KBr disk. No evidence of impurities, such as filter material, debris from the tubing through which serum was circulated, or undigested proteins, was found.

SEM analysis revealed that the recovered wear particles were distributed uniformly on both types of filter membranes (Figures 5 and 6). Minimal agglomeration of particles was observed. The wear particles deposited on both the 0.2 μm and 0.05 μm pore size filter membranes were predominantly submicron and round in appearance. Elongated fibrils (3 to 10 μm in length) were occasionally observed on both types of filter membranes. For the data pooled from all eight serum samples, the total numbers of particles imaged on the 0.2 μm and 0.05 μm pore size filters were 8272 and 20197, respectively. The size distributions for the particles deposited on the 0.2 μm and 0.05 μm pore size filters are presented in Figures 7 and 8, respectively. The wear particles recovered on the 0.2 μm and 0.05 μm pore size filter membranes were spatially distributed in an uniform manner. Agglomeration of particles was minimal. Because individual particles were clearly discernable from other particles and distributed uniformly on the filter membranes, sampling errors were niinimized, leading to a more accurate determination of particle count and size distribution.

For particles isolated on the 0.2 μm pore size filters, the mean (0.23 μm) of the size distribution was above the specified membrane pore size, whereas the median (0.19 μm) was below the specified pore size. The peak (mode) of the distribution occurred well below the 0.2 μm pore size at 0.13 μm. Over half (52.2%) ofthe total number of particles detected had diameters below the filter pore size of 0.2 μm. For the particles deposited on the 0.05 μm pore size filters, the mean (0.19 μm) and median mean (0.18 μm) diameters were well above the specified membrane pore size. No single dominant peak occurred in the size distribution, with the majority of particles evenly distributed between 0.08 and 0.25 μm. Only 2.8 percent of the total particles detected had diameters below the filter pore size of 0.05 μm. The mean and median diameters of the particles deposited on the 0.05 μm membranes were significantly lower (pO.OOl) than those of particles on the 0.2 μm pore size filter.

The 0.05 μm pore size filter membranes contained a greater number of wear particles than the 0.2 μm membranes (Table 1). The mean number of particles generated per cycle was 6.4x10⁶ ± 2.2x10⁶ for the serum digests passed through the 0.05 μm pore size filters and was 2.6xl0⁶ + 0.2x10^δ for the digests filtered through the 0.2 μm pore size membranes. This difference was statistically significant (p = 0.002).

The use of 0.2 μm pore size membranes caused an underestimate of the number of wear particles generated per million cycles for both conventional and 5 MRad doses of crosslinlced UHMWPE (Figures 9 and 10).

When vacuum filtration is used to isolate UHMWPE wear debris from digested hip simulator serum, the number and size distribution of recovered particles is strongly dependent upon the pore size of the filter membrane. A substantial number of wear particles passed freely through the pores of the 0.2 μm pore size membranes. Filtering digested serum through a 0.2 μm pore size filter underestimates the number, and consequently the surface area and volume of finer sized particles. A significantly greater number of finer sized particles can be isolated and analyzed by filtering digested serum through a 0.05 μm pore size filters. The entire digestion and filtration procedure took approximately 75 minutes when the digests were filtered through 0.2 μm pore size filter membranes. Filtering the digests through 0.05 μm pore size filter membranes added only 5 minutes to the procedure with no significant increase in the cost of materials and equipment. This increase in procedural time was well justified due to the fact that the number of particles recovered from hip simulator serum, and consequently the size distribution, was strongly dependent upon the pore size of the filter membrane used. Fine wear particles have been found to greatly influence the macrophage response to wear debris. This underscores the importance of using finer pore size (< 0.05 μm) filter membranes to isolate and characterize wear debris generated from new orthopaedic bearing materials.

Example 8. Wear Particle Analyses of Conventional and Crosslinked UHMWPE Tested in an Anatomic Hip Simulator

Numerous forms of crosslinlced UHMWPE, wliich demonstrate dramatic reductions in hip simulator gravimetric wear, have been developed (McKellop et al, 1999; Muratoglu et al, 1999) and used clinically with the intent to reduce particle-induced osteolysis. It is generally believed that gravimetrically measured reductions in wear translate into reductions in particle generation. The relationship between gravimetric wear volume and wear particle characteristics (size, surface area, and volume) was investigated by the comparison of one conventional and two variations of crosslinked UHMWPE.

Anatomic hip simulator (AMTI, Watertown, MA) tests were carried out to 10 million cycles on the following materials: (i) conventional UHMWPE (C-PE), (ii) 5 MRad crosslinlced UHMWPE (5-XPE or 5-XLPE), and (iii) 10 MRad crosslinked UHMWPE (10- XPE or 10-XLPE). Ram extruded GUR 1050 material (PolyHi Solidur, Ft. Wayne, IN) was the starting material for all tests. Crosslinldng was carried out at gamma irradiation doses of 5 and 10 MRad (SteriGenics, Gumee, IL), followed by melt annealing (2 hrs at 150 °C) and slow cooling. Acetabular liners (32 mm ID) were machined from bar stock, followed by EtO sterilization. The 5-XPE and 10-XPE liners were artificially aged at 70 °C and 5 arm O₂ for 3 weeks prior to testing (Sanford et al, 1995). Hip simulator testing (n=3 for each group) was carried out against 32 mm CoCrMo heads in 100% bovine serum. The testing was interrupted periodically for weight measurements and serum replacement. Wear particles were harvested from test serum using a previously validated acid digestion/ vacuum filtration protocol (Scott et al, 2000). The particles deposited on the 0.05-μm pore size filter membranes were characterized under a scanning electron microscope (SEM) at magnifications of 1,000X and 20,000X. A minimum of 20 random, non-overlapping fields and 100 particles were imaged to ensure that the detected particles were representative of the entire particle population within each serum sample. For each material, the mean particle diameter was determined and the following parameters were calculated per million cycles: (i) number of particles, (ii) surface area of particles, and (iii) volume of debris generated. Particle diameter, surface area, and volume were calculated assuming spherical geometry. ANOVA and Duncan's multiple range tests were used to determine significant differences (α = 0.05) in mean particle diameter, number of particles, surface area of particles, and volume of debris generated between the material conditions.

The gravimetric wear rates decreased as the crosslinking radiation dose increased. For the C-PE, the wear rate was 36.9 mg/Mcycles, which decreased to 9.0 mg/Mcycles for the 5-XPE, which further decreased to -1.1 mg/Mcycles for the 10-XPE (Table 3). Based on SEM micrographs, the C-PE particles were predominantly submicron spheroids, with occasional fibrils 5 to 10 μm in length (Figure 11). The 5-XPE and 10-XPE particles were predominately submicron spheroids (Figure 11).

In addition to the highest gravimetric wear rate, the C-PE material exhibited the largest particle diameter, surface area, and volume of debris generated (p<0.05 for all combinations of pairs, Table 3). Particle diameter and the surface area and volume of particles decreased with increasing crosslinking radiation dose. The 5-XPE material generated the highest number of particles, resulting in twice the number of particles per Mcycles than C-PE (Table 3). The 10-XPE material generated less than half the number of particles per Mcycle compared to C-PE.

TABLE 3. Gravimetric Wear Rate, Particle Diameter, Surface Area, Volume, and Number for the Tested Materials: Mean + 95% Confidence Interval

Increasing the crosslinking radiation dose resulted in a more wear resistant polyethylene as tested in our anatomic hip simulator, consistent with previous reports (McKellop et al, 1999; Muratoglu et al, 1999). The surface area and volume of particles decreased with increasing radiation dose. Particle size (diameter) also decreased with increasing radiation dose. Due to different particle size distributions, a unique relationship between gravimetric wear and particle number existed for each tested material. As a result, the reduction in gravimetric wear for the 5-XPE material did not translate into a reduction in particle number when compared with the C-PE material.

The mass loss due to wear for the 10-XPE liners was less than the fluid absorption that occurred during testing. As a result, the 10-XPE liners showed a net weight gain. Particle analysis, however, showed that small, but measurable volumes of wear particles were generated. Wear particle analysis may thus provide a more direct measurement of the volume and number of particles generated from highly crosslinlced UHMWPE and may be used to supplement gravimetric measurements for low wear materials.

Macrophage response to particulate wear debris is believed to be an important factor in osteolysis. It is well established that the cellular response is dependent upon particle number, size, surface area, and material chemistry, among other factors (Shanbhag et al, 1997; Green et al, 1998; and Gonzalez et al, 1996). Differences in particle number, size, and surface area were observed among conventional and crosslinked UHMWPE. Thus the biological response to the particulate forms of these three materials may differ due to varying particle characteristics. Example 9. Production of Mediators by Macrophages Exposed to UHMWPE Particles

Macrophages are isolated using the method of Green et al, 1998. Human macrophages are co-cultured with conventional UHMWPE, 5 MRad crosslinked UHMWPE, and 10 MRad crosslinlced UHMWPE at various concentrations. The particles are added to 1% agarose and poured into plates. Concentrations of particles that are used are 0, 1 x the amount of particles detected at 1 million cycles, 2 x, 5 x, and 10 x. Lipopolysaccharide is used as a positive control. Macrophages are then added to the top ofthe plates and incubated at 37°C for 24 hours. The amount of ILl-α and TNF-α produced by the macrophages at each particle concentration is measured by ELISA. ILl-α is assayed using paired monoclonal antibodies and TNF-α is measured using a modified double antibody sandwich technique.

Example 10. Particle Size Versus Particle Numbers and Volumes for Conventional and Crosslinked UHMWPE Numerous forms of crosslinlced UHMWPE have demonstrated dramatic reductions in hip simulator gravimetric wear. (McKellop et al, 1999; Muratoglu et al, 1999; and Essner et al, 2000). While gravimetric techniques provide a measurement of the total mass of debris generated from wear surfaces, no information about individual particles is gained. The objectives of this study were to directly determine the number, size distribution, and volume distributions for UHMWPE particles generated during hip simulator testing. One conventional and two variations of crosslinlced UHMWPE were compared in this study.

Anatomic hip simulator (AMTI, Watertown, MA) tests were carried out to 15 million cycles on the following materials: (i) conventional UHMWPE (C-PE), (ii) 5 MRad crosslinlced UHMWPE (5-XPE), and (iii) 10 MRad crosslinlced UHMWPE (10-XPE). Ram extruded GUR 1050 material (PolyHi Solidur, Ft. Wayne, IN) was the starting material for all tests. Crosslinldng was carried out at gamma irradiation doses of 5 and 10 MRad (SteriGenics, Gurnee, IL), followed by melt annealing and slow cooling, Acetabular liners (32 mm ID) were machined from bar stock and EtO sterilized. The 5-XPE and 10-XPE liners were artificially aged at 70 °C and 5 atm O² for 3 weeks prior to testing (Sanford et al, 1995). Hip simulator testing (n=3 for each group) was carried out against 32 mm CoCrMo heads in 100% bovine serum. The testing was interrupted periodically for gravimetric measurements and serum replacement. Wear particles were harvested from test serum using a previously validated acid digestion/ vacuum filtration protocol (Scott et al, 2000). The particles deposited on the 0.05-μm pore size filter membranes were characterized under a scanning electron microscope (SEM) at magnifications of 1,000X and 20,000X. A minimum of 20 random, non-overlapping fields and 100 particles were imaged to ensure that the detected particles were representative of the entire particle population within each serum sample. For each detected particle, an equivalent circular diameter and spherical volume were calculated based the projected area of the particle. For each material condition, the mean number of particles generated per cycle (N) of testing was determined. The following distributions were also plotted: (i) particle number vs. diameter and (ii) total particle volume vs. diameter. Total particle volume was calculated as the sum of individual particle volumes contained within each specified particle diameter interval. ANOVA and Duncan's analyses were used to test for significant differences in particle generation rates between the material conditions.

The gravimetric wear rates decreased as the crosslinldng radiation dose increased. For the C-PE, the mean wear rate ± 95% Cl was 36.9 ± 0.5 mg/Mcycles, which decreased to 9.0 ± 0.6 mg/Mcycles for the 5-XPE, which further decreased to -0.5 ± 0.2 mg/Mcycles for the 10-XPE. Based on SEM micrographs, the C-PE, 5-XPE, and 10-XPE particles had the" same predominant morphology- submicron granules (Figure 11). Fibrils 5 to 10 μm in length were occasionally seen for the C-PE particles (Figure 11).

The 5-XPE material generated the greatest number of particles per cycle (N=l 1.1 x 10⁶

+ 2.5xl0⁶), resulting in 78% more particles per cycle than the C-PE material (N=6.2xl0⁶ ± 1.1x10°) (p < 0.01). The 10-XPE liners (N=2.2xl0⁶ ± 0.2xl0⁶) generated 65% fewer particles per cycle than the C-PE liners (p < 0.01).

The particle number vs. size distributions for the three material conditions are presented in Figure 12. The distributions of total particle volume vs. size are presented in Figure 13. Because the tliree materials produced different numbers and volumes of particles over the duration of testing, the distributions are presented in absolute number instead of percent frequency. The 5-XPE liners produced a greater number and volume of particles below 0.2 μm in diameter than the C-PE liners. Above 0.2 μm, the C-PE particles were greater in number and volume of than the 5-XPE particles. The C-PE andlO-XPE liners generated an equivalent number and volume of particles with diameters less than 0.125 μm. Above 0.125 μm, the C-PE particles were greater in number and volume than 10-XPE particles.

Increasing the crosslinking radiation dose resulted in lower gravimetric wear as tested in our anatomic hip simulator, consistent with previous reports (McKellop et al, 1999; Muratoglu et al, 1999). Increasing radiation dosage also affected the particle size distribution, resulting in a unique relationship between gravimetric wear and particle number for each tested material. As a result, the reduction in gravimetric wear for the 5-XPE material did not translate into a reduction in particle number when compared with the C-PE material.

In vitro cell culture studies have shown that macrophage response is a function of particle morphology, size, number, and volumetric dose, among other factors (Shanbhag et al, 1997; Green et al, 2000; and Gonzalez et al, 1996). Conventional and two crosslinlced

UHMWPE materials produced particles that were similar in morphology. However, differences in the particle number and volumetric distributions existed between the three materials. The 5-XPE material generated the greatest number and volume of particles with diameters below 0.2 μm. Above 0.2 μm, the C-PE material generated the greatest number and volume of particles. For every size interval, the number and volume of 10-XPE particles were less than or equal to that of the C-PE particles. A recent cell culture study showed that smaller UHMWPE particles (0.24 μm) produced bone resorbing activity at a lower volumetric dose (10 μm³/macrophage), while larger particles (0.45 μm and 1.71 μm) produced bone resorbing activity at doses of 100 μm³ per macrophage (Green et al, 2000).

Because the particulate forms of the three materials tested have exhibited different particle size distributions, the biological response to wear debris from these materials may differ.

Example 11. Lamellar Thickness Lamellar thickness values were determined using a TA Instruments 2910 differential scanning calorimeter (DSC). Testing was conducted per ASTM D 3417. Five samples weighing approximately 2.5 mg were taken from the core of the following materials: (i) GUR 1050 UHMWPE barstock that was gamma-irradiated to a dose of 10 MRad and subsequently annealed at 147°C (XL-147); and (ii) GUR 1050 UHMWPE barstock that was gamma-irradiated to a dose of 10 MRad and subsequently annealed at 140°C (XL-140). The samples were crimped into aluminum crucibles and placed in the DSC chamber. The chamber was continuously flushed with mtrogen gas at a flow rate of approximately 30 ml/min. The reference sample was an empty aluminum crucible. A DSC cycle consisted of a 2 minute equilibrating at 30°C followed by heating to 150°C at 10°C/min rate.

The temperature corresponding to the peak of the endotherm was taken as the melting point (E_m). The lamellar thickness (I) was calculated as follows:

1 = (2 -σ_e - T_m ⁰)/(AH-(T_m° - T_m)p)

where σ_e is the end free surface energy of polyethylene (2.22 x 10^"6 cal/cm²), - His the heat of melting of polyethylene crystals (69.2 cal/g), pis the density ofthe crystalline regions (1.005 g/cm³), and T_m° is the melting point of a perfect polyethylene crystal (418.15 K).

The mean lamellar thickness values were 369.0 and 346.9 Angstroms, respectively, for the XL-147 and XL-140 materials (Table 4, Table 5).

Table 4. XL-147 (147 degree annealing, 10 MRad XLPΕ)

Sample Melting Temp (deg lamellar thickness

C) (Angstroms)

1 138.3 398

2 137.4 352

3 137.9 376

4 137.7 365

5 137.5 354 avg 137.8 369.0 std dev 0.4 19.1

Table 5. XL-140 (140 degree annealing, 10 MRad XLPE)

Sample Melting Temp (deg lamellar thickness

C) (Angstroms)

1 138.07 385

2 136.68 321

3 136.89 329

4 136.72 322

5 137.92 377

137.26 346.9 std dev 0.68 31.5

Example 12. Trans-vinylene Index For polyethylene, the concentration of trans-vinylene units (TNU) has been shown to be linear with absorbed radiation dose at low dose levels (<40 Mrad) (Lyons et al, 1993). The concentration of TVU can therefore be used to determine the level of crosslinking in UHMWPE.

Trans-vinylene concentration was determined for the following materials: (i) GUR 1050 UHMWPE barstock that was gamma-irradiated to a dose of 2.5 MRad and subsequently annealed at 150°C (Gamma2.5); (ii) GUR 1050 UHMWPE barstock that was gamma- irradiated to a dose of 5 MRad and subsequently annealed at 150°C (Gamma5); (iii) GUR 1050 UHMWPE barstock that was gamma-irradiated to a dose of 10 MRad and subsequently annealed at 147°C (GammalO-147); and (iv) GUR 1050 UHMWPE barstock that was gamma-irradiated to a dose of 10 MRad and subsequently annealed at 140°C (GammalO- 140). For each material type a rectangular specimen (63.50 x 12.70 x 6.35 mm) was machined, and 200 to 250 μm thick samples were sliced using a sledge microtome and a diamond blade. For each slice, IR spectra were obtained using a Bio-Rad FTS 25 spectrometer equipped with a UMA 500 infrared microscope. The square sampling area for each spectrum was 200 μm² x 200 μm². The trans-vinylene index (TVI) was calculated by normalizing the area under the trans-vinylene vibration at 965 cm^"1 to that under the 1900 cm^"1 vibration. The average TVI for each material type was taken as the average of four measurements taken at depths of 0.5, 1.0, 1.5, and 2.0 mm distances from the surface of the specimens.

The average TVI values for each material type are shown in Figure 14. The TVI value was found to increase with increasing radiation dose.

Example 13 Effect on Wear of Crosslinked UHMWPE Annealed Between 140 °C to 150 °C

140-XLPE was prepared by irradiating UHMWPE and subsequently annealing at a nominal temperature of 140°C (range of 138 to 142 °C). The 140-XLPE liners were tested for wear, using the wear analysis process ofthe present invention, against CoCr and zirconia heads on an anatomic hip simulator to approximately 5 million cycles. Gravimetric wear and particle generation rates were determined for both articulating combinations. The results were compared with those of conventional (non-crosslinked) UHMWPE (C-UHMWPE) and 147°C annealed XLPE (147-XLPE) tested against CoCr heads and zirconia heads.

Cumulative mass changes were determined for the tested liners, and soak controls were used to correct for fluid absorption. Mass data was converted to volumetric data by dividing by a density of 0.93 g/cm³ for UHMWPE. Aggregate volumetric wear rates were determined for each condition by linear regression of cumulative wear volume versus cycle count. The aggregate wear rate was taken as the slope ofthe line fit through each entire data set.

Particle isolation and analysis was performed on serum samples as described in Example 3. A total of 30 serum samples were collected and analyzed.

Particle characterization was performed at magnifications of 20,000X and 1,000X. A minimum of twenty fields of view were analyzed per serum sample. The particles contained within each field of view were detected using a fully automated digital imaging system (eXL II Analyzer, Oxford Instruments Ltd., Oak Ridge, TN). Based on grayscale level threshold values, the boundary of each particle was defined and the projected area was calculated by the digital imaging software. Particle diameter (Dp), surface area (Ap), and volume (Vp) were calculated based the projected area of each particle. Dp = 2 (projected area / π)^{1 2} (1)

A_P = π D ² (2)

N_P = (π Dp³) / 6 (3)

For each bearing couple, the data from all serum harvests were combined, and the distribution of number of particles generated as a function of particle diameter was determined. The total number of detected particles was determined for each field of view, and the mean number of particles per field of view (Ν_F) and the number of particles generated per cycle of testing (Νc) was calculated for each serum sample.

Gravimetric wear was determined by raw mass measurements ofthe 140-XLPE liners tested against CoCr and zirconia heads. The wear data are summarized in Table 6.

Cumulative wear as a function of test cycles is shown graphically for both conditions in

Figure 15. Against both CoCr and zirconia heads, the 140-XLPE liners showed a net mass gain (negative gravimetric wear) at the end of testing. The net mass gain was due to two factors: (i) the mass of fluid absorbed by the test liners was greater than the mass absorbed by the soak controls, resulting in a net mass gain for the test liners; and (ii) the net mass gain due to fluid absorption was greater than the net mass loss due to wear for the test liners. The

140-XLPE liners against CoCr heads showed a trend of mass gain due to fluid absorption for the first two million cycles of testing, then showed a trend of mass loss for the remaining three million cycles of testing. The 140-XLPE liners against zirconia heads showed a trend of mass gain throughout the entire test. The aggregate wear rates and 95% confidence intervals were as follows: 140-XLPE / CoCr wear rate was 0.2 ± 0.7 mm³/Mcycles (± 95.

The aggregate gravimetric wear rates ofthe 140-XLPE, 147-XLPE, and C-UHMWPE liners against CoCr heads are summarized in Table 7. The 140-XLPE liners wore at a higher aggregate gravimetric wear rate than 147-XLPE lmers (0.2 vs. -2.0 mm /Mcycles; p < 0.0001); however, both liner types showed significantly lower aggregate gravimetric wear rates than the C-UHMWPE liners (36.4 mm³/Mcycles; p < 0.0001).

Table 8 summarizes the gravimetric rates of the 140-XLPE, 147-XLPE, and C- UHMWPE liners tested against zirconia heads. The gravimetric wear rates ofthe 140-XLPE and 147-XLPE liners were equivalent (-1.8 and -1.7 mm³/Mcycles; p = 0.55) and were significantly lower than that ofthe C-UHMWPE liners (28.8 mm³/Mcycles; p < 0.0001). Wear particle morphology was evaluated by SEM micrographs of 140-XLPE wear particles are shown in Figure 16. Against both CoCr and zirconia femoral heads, the primary morphology of the wear debris generated from the liners was circular and submicron.

Elongated fibrils, as are occasionally seen among the wear particles from C-UHMWPE (or C- PE) liners, were absent among the particles generated from the XLPE liners.

The 140-XLPE / zirconia bearing couple generated fewer particles than the 140- XLPE / CoCr bearing couple throughout the entire test (Figure 17). The mean particle generation rates ofthe two bearing couples were as follows: 140-XLPE / CoCr generated 2.5 x 10⁶ ± 0.4 x 10^δ particles per cycle (± std. dev.); and 140-XLPE / zirconia generatedl.5 x 10⁶ ± 0.6 x 10⁶ particles per cycle.

The particle generation rates of the 140-XLPE, 147-XLPE, and C-UHMWPE liners tested against CoCr heads are summarized in Table 7. The particle generation rates of the

140-XLPE and 147-XLPE liners were statistically equivalent (2.5xl0⁶ vs. 2.2xl0⁶ particles per cycle, respectively; p = 0.50) and were approximately 70% lower (p < 0.0001) than the particle generation rate ofthe C-UHMWPE liners (8.0xl0⁶ particles per cycle).

Shown in Table 8 are the particle generation rates of the 140-XLPE, 147-XLPE, and C-UHMWPE liners tested against zirconia heads. The particle generation rates of the 140- XLPE and 147-XLPE liners were equivalent (1.5x106 vs. 1.3x106 particles per cycle, respectively; p = 0.50) and were approximately 75% lower than the particle generation rate of the C-UHMWPE liners (6.1 x 106 particles per cycle).

Particle size distributions were evaluated by histogram. The number of particles generated as a function particle diameter is shown in Figure 18 for liners tested against CoCr heads. The 140-XLPE and 147-XLPE liners generated fewer particles at every size interval compared to the C-UHMWPE liners. Figure 19 shows the number of particles generated as a function of size for liners tested against zirconia heads. Again, the 140-XLPE and 147-XLPE liners generated fewer particles at every size interval compared to the C-UHMWPE liners. Table 6. Cumulative Volumetric Wear (mm ) vs. Cycles for 140 °C Annealed XLPE Liners.

Table 7. Gravimetric Wear, Particle Generation Rates, and Mean Particle Diameters for C-UHMWPE and XLPE Liners Tested Against CoCr Heads

Table 8. Gravimetric Wear, Particle Generation Rates, and Mean Particle Diameters for C-UHMWPE and XLPE Liners Tested Against Zirconia Heads

Example 14. Crosslinked UHMWPE (XLPE) Bearing Components Articulating on Ceramic Counterbearmg Surfaces Increased Wear Resistance.

Crosslinked UHMWPE (XLPE) of the present invention was gamma irradiated to crosslink and increase wear resistance. However, exposure to ionizing radiation generates free radicals which can combine with oxygen in air, leading to oxidative degradation and embrittlement over time. Following the step of radiation crosslinking (i.e., irradiation), the XLPE material was annealed at a nominal temperature of 147°C, which is above the peak melting temperature of the material, in order to quench free radicals and impart resistance to oxidative degradation. XLPE produced by this process has been shown herein to produce less gravimetric wear and fewer wear particles than conventional non-crosslinked liners when tested in a hip simulator. Annealing at 140°C is slightly below peak melting temperture is taught to effectively quench free radicals created during the irradiation ofthe XLPE material, thereby imparting oxidative stability (see, U.S. patent 5,414,049), however, wear properties have not been determined.

Against CoCr heads the 140-XLPE liners wore at a higher aggregate gravimetric wear rate than 147-XLPE liners (0.2 vs. -2.0 mm³/Mcycles, respectively; p < 0.0001); however, the aggregate gravimetric wear rate of the 140-XLPE liners was significantly lower (p < 0.0001) than that of the C-UHMWPE liners (36.4 mm³/Mcycles). The mean particle generation rates ofthe 140-XLPE and 147-XLPE liners were statistically equivalent (2.5x10⁶ vs. 2.2xl0⁶ particles per cycle, respectively; p = 0.50) and approximately 70% lower (p < 0.0001) than the mean particle generation rate of the C-UHMWPE liners (8.0xl0⁶ particles per cycle). The 140-XLPE and 147-XLPE liners generated fewer particles at every size interval compared to the C-UHMWPE liners.

Against zirconia heads the gravimetric wear rates of the 140-XLPE and 147-XLPE liners were equivalent (-1.8 and -1.7 mm³/Mcycles; p = 0.55) and were significantly lower than that of the C-UHMWPE liners (28.8 mm³/Mcycles; p < 0.0001). The mean particle generation rates ofthe 140-XLPE and 147-XLPE liners were equivalent (1.5xl0⁶ vs. 1.3xl0⁶ particles per cycle, respectively; p = 0.50) and approximately 75% lower (p < 0.0001) than the mean particle generation rate of the C-UHMWPE liners (6.1xl0⁶ particles per cycle). The 140-XLPE and 147-XLPE liners generated fewer particles at every size interval compared to the C-UHMWPE liners. For testing against both CoCr and zirconia heads, the 140-XLPE and 147-XLPE wear particles shared the same predominant morphology in that they were primarily circular and submicron. Elongated fibrils, which were occasionally observed among the particles from C-UHMWPE liners, were absent among the particles generated from the XLPE liners.

The 10 Mrad XLPE (10-XPE or, interchangeably 10-XLPE) liners annealed at 140 °C showed significant reductions in both wear mass and particle number as compared to conventional non-crosslinked liners. These wear reductions were demonstrated when articulating against CoCr femoral heads and zirconia femoral heads. Furtheπnore, the 140 °C annealed XLPE showed similar particulate characteristics to XLPE annealed at 147 °C in that both materials showed reduction in particle number at every size range compared to C- UHMWPE liners. This is particularly important because in vitro macrophage response to wear debris has been found to be a function of both particle size distribution and number (Green et al, 1998; Gonzalez et al., 1996; Shanbhag et al., 1994; Green et al., 2000). Because the 140-XLPE generates fewer particles than C-UHMWPE over the entire particle size range, the use of 140-XLPE material against CoCr and zirconia heads is expected to reduce the inflammatory response in vivo.

Example 15. Wear Debris in Crosslinked UHMWPE (XLPE) under Abrasive Conditions The different forms of XPE have also been tested to improve volumetric wear under abrasive simulation, either by pre-roughening femoral heads (McKellop, 1999) or by adding abrasive alumina particles in the test serum (Laurent, 2000). These studies are particularly important because CoCr heads are known to roughen in vivo, leading to accelerated wear of the polyethylene liners (Jasty, 1994; Hall, 1997). One strategy to ameliorate the effects of abrasive conditions is to use ceramic heads (alumina or zirconia), which are more resistant to scratching than CoCr heads (Fenollosa, 2000). Hip simulator data on ceramic heads coupled to XPE, however, have not been reported to date. Additionally, analyses of wear particulate released from C-PE and XPE liners under abrasive conditions have not been investigated. This study reports hip simulator gravimetric and wear particle data for pre-scratched CoCr and zirconia ceramic heads tested against C-PE and 10 Mrad crosslinlced UHMWPE (10- XPE). C-PE (non-irradiated) and 10 Mrad (gamma irradiated, thermally annealed at 150 °C) crosslinked UHMWPE (10-XPE) 32 mm liners were tested to 5 million cycles in an anatomic hip simulator (AMTI, Watertown, MA). Both types of liners were tested against (1) smooth CoCr, (2) roughened CoCr, and (3) smooth zirconia. Undiluted alpha-fraction bovine serum was used. The roughened femoral heads were produced by tumbling in a centrifugal barrel finisher against polymer cones and 100 grit alumina powder in order to obtain multidirectional scratching as seen clinically (Jasty, 1994). The roughness values ofthe heads were measured with an interferometer (Wylco RST Plus, Veeco, Plainview, NY) and were as follows: (i) smooth CoCr heads (R_a = 0.02 ± 0.01 *μm; R_pk = 0.02 ± 0.01 μm); (ii) smooth zirconia heads (R_a = 0.01 ± 0.01 μm; R_pk = 0.02 + 0.01 μm); and (iii) roughened CoCr heads (R_a = 0.17 ± 0.01 μm; R_pk = 0.47 ± 0.03 μm). The mean R_a value ofthe roughened heads was within the clinical range reported for retrieved CoCr heads measured by interferometry (see, Bauer, 1994). The zirconia heads were not roughened because they do not commonly exhibit in vivo roughening when articulating against UHMWPE cups (Minikawaw, 1998).

The gravimetric wear rates for the head/liner couples tested in this study are shown in

Table 9. The 10-XPE liners showed significantly (p<0.01) lower gravimetric wear than C-PE against all heads. SEM micrographs of particles from each of the six head/liner couples tested are shown in Figures 20 (C-PE) and 21 (10-XPE). Debris from C-PE liners against all femoral head types were predominantly submicron and rounded, with occasional fibrils up to 5 μm long. The particulate debris generated from 10-XPE liners against both smooth CoCr and zirconia heads was almost exclusively submicron and rounded. Only when tested against roughened CoCr heads did the 10-XPE liners generate an appreciable number of fibrils. The particle generation rates are listed in Table 9. The 10-XPE liners generated fewer wear particles than C-PE liners (p<0.01) against smooth CoCr and zirconia heads. However, against roughened CoCr heads, the difference in particle generation rate between C-PE (10.5 particles/10⁶ cycles) and 10-XPE (8.9 particles/10⁶ cycles) was not significant (p=0.17).

Undetectable clean condition gravimetric wear for highly crosslinlced UHMWPE has been reported by Muratoglu et al, 1999. However, it has also been reported that undetectable wear does not necessarily mean no wear particles are generated (Scott et al., 2001). Against roughened CoCr heads, a condition that commonly occurs clinically, 10-XPE showed detectable gravimetric wear (19.0 mm³ Mcycles), and the particle generation rate was not statistically different than for C-PE. Against scratch-resistant zirconia ceramic heads, 10- XPE liners showed undetectable gravimetric wear and particle generation rates lower than all other liner/head couples. Additionally, zirconia heads resulted in lower wear for C-PE liners. This hip simulator study showed that the wear performance advantage of highly crosslinked UHMWPE against CoCr heads diminishes when the heads are scratched in a similar manner as seen in vivo. Although under scratched conditions the gravimetric wear is still greatly lower for 10-XPE than for C-PE, the particle generation rates are statistically equivalent. The data indicates that the use of counterbearmg surfaces that are harder and more scratch-resistant than CoCr, such as ceramic heads, are beneficial by maintaining the superior wear performance of XPE. Further, zirconia heads are viable alternatives to CoCr heads under abrasive conditions and result in lower wear and particle generation rates over extended periods.

Table 9. Mean Gravimetric Wear Rate, Particle Generation Rate, and Equivalent Circular Diameter (ECD) for Six Bearing Couples.

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Claims

CLAIMS We claim:

1. A method for isolating wear particles from an ultrahigh molecular weight polyethylene (UHMWPE) medical implant for use in the body comprising the steps of: crosslinldng the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; and filtering the particles using a filter having a pore size of 0.05 μm or smaller.

2. The method of claim 1 , wherein said annealing is performed at or below 150°C.

3. The method of claim 1, wherein said annealing is performed below about 150°C and above about 140°C.

4. The method of claim 1 , wherein said annealing is performed at 147°C.

5. The method of claim 1, wherein said annealing is performed at 140°C.

6. A method as in any of claims 2, 3, 4 or 5, wherein the crosslinldng is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10.

7. A method as in any of claims 2, 3, 4 or 5, wherein the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than about 0.15 and less than about 0.20.

8. A method of preparing an UHMWPE medical implant for use in the body having a decreased wear particle number comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; and machining UHMWPE to fomi an implant; wherein the wear particles that are decreased in number have a diameter of 0.2 μm or less.

9. A method as in either claim 1 or claim 8, wherein said machining is performed before said crosslinking.

10. A method as in either claim 1 or claim 8, wherein said crosslinking is performed using electromagnetic radiation, energetic subatomic particles, gamma radiation, electron beam radiation, x-ray radiation, or a chemical crosslinking compound.

11. A method as in either claim 1 or claim 8, wherein said crosslinking is performed using gamma radiation.

12. A method as in either claim 1 or claim 8, wherein said crosslinldng is performed using radiation at a dose of greater than five but less than or equal to fifteen MegaRad (MRad).

13. A method as in either claim 1 or claim 8, wherein said crosslinking is performed using radiation at a dose of greater than five but less than or equal to ten MegaRad (MRad).

14. A method as in either claim 1 or claim 8, wherein said annealing is performed in an inert environment or an ambient atmosphere.

15. A method as in either claim 1 or claim 8, wherein said wear testing occurs on a joint simulator.

16. The method of claim 15 , wherein said j oint simulator simulates a hip j oint or a knee joint.

17. A method as in either claim 1 or claim 8, wherein said wear testing occurs in vivo.

18. A method as in either claim 1 or claim 8, wherein said harvesting is performed using acid digestion, base digestion, or an enzymatic digestion.

19. A method as in either claim 1 or claim 8, wherein said harvesting is performed using acid digestion.

20. A method as in either claim 1 or claim 8, wherein said implant has a polymeric structure with greater than about 300 angstrom lamellar thickness.

21. The method of claim 8, wherein said annealing is perfonned at or below 150°C.

22. The method of claim 8, wherein said annealing is perfonned below about 150°C and above about 140°C.

23. The method of claim 8, wherein said annealing is perfonned at 147°C.

24. The method of claim 8, wherein said annealing is performed at 140°C.

25. A method as in any of claims 21, 22, 23, or 24, wherein the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10. A method as in any of claims 21, 22, 23, or 24, wherein the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than about 0.15 and less than about 0.20. A method of decreasing macrophage response to an UHMWPE medical implant for use in the body comprising the steps of: performing wear particle analysis on the UHMWPE; and crosslinking the UHMWPE at a dose exliibiting the lowest particle number per million cycles of the hip simulator, wherein the number of particles present was determined using filter having a pore size of 0.05 μm or smaller.

26. A method of decreasing macrophage response to an UHMWPE medical implant for use in the body comprising crosslinldng UHMWPE prior to implantation in a patient wherein the total volume of wear particles is decreased and the total number of wear particles is decreased as compared to conventional UHMWPE.

27. A method as in either claim 27 or claim 28, wherein said crosslinking is performed using electromagnetic radiation, energetic subatomic particles, gamma radiation, electron beam radiation, x-ray radiation, or a chemical crosslinking compound.

28. A method as in either claim 27 or claim 28, wherein said crosslinking is performed using gamma radiation.A method as in either claim 27 or claim 28, wherein said crosslinldng is perfonned using radiation at a dose of greater than five but less than or equal to fifteen MegaRad (MRad). A method of decreasing osteolysis of an UHMWPE medical implant for use in the body comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the particles using a filter having a pore size of 0.05 μm or smaller; determining a number of wear particles; and selecting the crosslinldng dose that provides the implant having a less than about 5 x 10 wear particles generated per Mega cycle.

29. The method of claim 32, wherein the wear particles have a diameter of 0.2 μm or less.

30. A method of decreasing osteolysis of an UHMWPE medical implant for use in the body comprising the steps of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the particles using a filter having a pore size of 0.05 μm or smaller; determining a total particle surface area; and selecting the crosslinldng dose that provides the implant having a less than about 1.17 m²/Mega cycle total particle surface area.

31. A method as in either claim 32 or claim 34, wherein said crosslinldng is performed using electromagnetic radiation, energetic subatomic particles, gamma radiation, electron beam radiation, x-ray radiation, or a chemical crosslinking compound.

32. A method as in either claim 32 or claim 34, wherein said crosslinking is performed using gamma radiation.

33. A method as in either claim 32 or claim 34, wherein said crosslinldng is at a dose of greater than five but less than or equal to fifteen MegaRad (MRad).

34. A method as in either claim 32 or claim 34, wherein said crosslinldng is at a dose of greater than five but less than or equal to ten MegaRad (MRad).

35. A method as in either claim 32 or claim 34, wherein said annealing is performed in an inert environment or an ambient environment.

36. A method as in either claim 32 or claim 34, wherein said annealing is performed below or equal to 150°C.

37. A method as in either claim 32 or claim 34, wherein said annealing is performed below about 150°C and above about 140°C.

38. A method as in either claim 32 or claim 34, wherein said annealing is performed at 147°C.

39. A method as in either claim 32 or claim 34, wherein said annealing is performed at 140°C.

40. A method as in either claim 32 or claim 34, wherein the crosslinldng is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10.

41. A method as in either claim 32 or claim 34, wherein the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than about 0.15 and less than about 0.20.

42. A method as in either claim 32 or claim 34, wherein said wear testing occurs on a joint simulator.

43. The method of claim 46, wherein said joint simulator simulates a hip joint or a knee joint.

44. A method as in either claim 32 or claim 34, wherein said wear testing occurs in vivo.

45. A method as in either claim 32 or claim 34, wherein said harvesting is performed using acid digestion, base digestion, enzymatic digestion.

46. A method as in either claim 32 or claim 34, wherein said harvesting is performed using acid digestion.

47. A method as in either claim 32 or claim 34, wherein said implant has a polymeric structure with greater than about 300 angstrom lamellar thickness.

48. A method of decreasing macrophage response to a UHMWPE medical implant for use in the body comprising the steps of crosslinldng the UHMWPE; simulating use in a host; and testing serum for wear particles using a filter having a pore size of 0.05 μm, wherein the number of wear particles having a diameter of less than 0.2 μm are decreased as compared to conventional UHMWPE.

49. The method of claim 52, wherein said crosslinking is performed using electromagnetic radiation, energetic subatomic particles, gamma radiation, electron beam radiation, x-ray radiation, or a chemical crosslinking compound.

50. The method of claim 52, wherein said crosslinking is performed using gamma radiation.

51. The method of claim 52, wherein said crosslinldng is performed using radiation at a dose of greater than five but less than or equal to fifteen MegaRad (MRad).

52. The method of claim 52, wherein said crosslinldng is performed using radiation at a dose of greater than five but less than or equal to ten MegaRad (MRad).

53. The method of claim 52, wherein said annealing is performed below or equal to about 150 °C.

54. The method of claim 52, wherein said simulating occurs on a joint simulator.

55. The method of claim 58, wherein said simulating simulates a hip joint or a knee joint.

56. A cross-linked UHMWPE medical implant for use in the body that exhibits decreased osteolysis in comparison to conventional treatment of UHMWPE due to a particle

19 number of less than 5 x 10 per Mega cycle upon testing for wear resistance.

57. An UHMWPE medical implant for use in the body having a decreased wear particle number of particles created by the steps comprising of: crosslinking the UHMWPE; annealing the UHMWPE; machining UHMWPE to form an implant; wear testing the implant to generate wear particles; harvesting the wear particles; filtering the particles using a filter having a pore size of 0.05 μm or smaller; detennining the number of wear particles; and selecting the crosslinking dose that provides the implant having a less than

1 9 about 5 x 10 wear particles generated per Mega cycle.

58. The method of claim 61, wherein the wear particles have a diameter of 0.2 μm or less.

59. The implant of claim 61, wherein said machining is performed before said crosslinldng.

60. The implant of claim 61, wherein said crosslinking is performed using electromagnetic radiation, energetic subatomic particles, gamma radiation, electron beam radiation, x-ray radiation, or a chemical crosslinldng compound.

61. The implant of claim 61 , wherein said crosslinldng is performed using gamma radiation.

62. The implant of claim 61 , wherein said crosslinldng is performed using radiation at a dose of greater than five but less than or equal to fifteen MegaRad (MRad).

63. The implant of claim 61 , wherein said crosslinking is performed using radiation at a dose of greater than five but less than or equal to ten MegaRad (MRad).

64. The implant of claim 61, wherein said annealing is performed below or equal to 150°C.

65. The implant of claim 61, wherein said annealing is performed below about 150°C and above about 140°C.

66. The implant of claim 61 , wherein said annealing is performed at 147°C.

67. The implant of claim 61, wherein said annealing is perfonned at 140°C.

68. A method as in any of claims 68, 69, 70, or 71, wherein the crosslinking is sufficient to form an implant with a trans-vinylene index of greater than or equal to 0.10.

69. A method as in any of claims 68, 69, 70, or 71, wherein the crosslinldng is sufficient to form an implant with a trans-vinylene index of greater than about 0.15 and less than about 0.20.

70. The implant of claim 61, wherein said wear testing occurs in vivo.

11. The implant of claim 61 , wherein said harvesting is performed using acid digestion, base digestion, or an enzymatic digestion.

72. The implant of claim 61 , wherein said harvesting is performed using acid digestion.

73. The implant of claim 61 , wherein said implant has a polymeric structure with greater than about 300 angstrom lamellar thickness.

74. A total j oint prosthesis comprising a bearing surface comprised of crosslinlced UHMWPE that generates less than about 5 x 10¹² wear particles per Mega cycle; and a counterb earing surface comprised of ceramic.

75. The prosthesis of claim 78, wherein the ceramic counterbearmg surface comprises zirconia.