Crosslinked ultrahigh molecular weight polyethylene (UHMWPE) has been recently approved by the Food and Drug Administration for use in orthopedic implants. The majority of commercially available UHMWPE orthopedic components are crosslinked using e-beam or gamma radiation. The level of crosslinking is controlled with radiation dose and free radicals are eliminated through heat treatments to prevent long-term degradation associated with chain scission or oxidation mechanisms. Laboratory studies have demonstrated a substantial improvement in the wear resistance of crosslinked UHMWPE. However, a concern about the resistance to fatigue damage remains in the clinical community, especially for tibial components that sustain high cyclic contact stresses. The objective of this study was to investigate both the initiation and propagation aspects of fatigue cracks in radiation crosslinked medical-grade UHMWPE. This work evaluated three levels of radiation, which induced three crosslink densities, on the fatigue crack propagation and total fatigue life behavior. Both as-received UHMWPE, as well as those that underwent an identical thermal history as the crosslinked UHMWPE were used as controls. Fractured crack propagation specimens were examined using scanning electron microscopy to elucidate fatigue fracture mechanisms. The results of this work indicated that a low crosslink density may optimize the fatigue resistance from both a crack initiation and propagation standpoint.
With the potential to map mechanical properties of heterogeneous materials on a micrometer scale, there is growing interest in nanoindentation as a materials characterization technique. However, nanoindentation has been developed primarily for characterization of hard, elasto-plastic materials, and the technique has not been validated for very soft materials with moduli less than 5 MPa. The current study attempted to use nanoindentation to characterize the elastic moduli of soft, elastomeric polydimethylsiloxane (PDMS) samples (with different degrees of crosslinking) and determine the effects of adhesion on these measurements using adhesion contact mechanics models. Results indicate that nanoindentation was able to differentiate between elastic moduli on the order of hundreds of kilo-Pascals. Moreover, calculations using the classical Hertz contact model for dry and aqueous environment gave higher elastic modulus values when compared to those obtained from unconfined compression testing. These data seem to suggest that consideration of the adhesion energy at the tip-sample interface is a significantly important parameter and needs to be taken into account for consistent elastic modulus determination of soft materials by nanoindentation.
Soft hydrated materials, such as vascular tissues and other biomaterials, provide a number of challenges in the field of nanoindentation. However, the ability of nanoindentation to probe local, nanoscale mechanical properties of heterogeneous materials makes it desirable to adapt this technique for application to biologic tissues. To develop the field of nanoindentation for the analysis of soft hydrated materials, the goals of this study were fourfold: develop a sample hydration system, select an appropriate tip for soft material indentation, identify a substrate to be used for blunt tip alignment, and determine an appropriate control material for the development of future indentation protocols. A hydration system was developed that maintained sample hydration for over 8 h without completely submerging the sample. Further, a 100-microm radius of curvature conospherical tip was shown to be a suitable tip for indenting a variety of soft hydrated materials and back-illuminated agarose gel was found to be an effective material for use in tip alignment. Finally, agarose gel demonstrated similar qualitative and quantitative nanomechanical behavior to vascular tissue, suggesting that it will be an appropriate control material for the development of future indentation protocols for soft biologic tissues.
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