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Journal of Bone and Joint Surgery - British Volume, Vol 88-B, Issue SUPP_III, 371.  
Copyright © 2006 by British Editorial Society of Bone and Joint Surgery
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British Orthopaedic Research Society


Edinburgh – 1–2 September, 2003

President – Professor D. Marsh


DIFFERENT EFFECTS OF PARTICLE SIZE ON MUTAGENIC, INFLAMMATORY AND TOXIC PROPERTIES OF COBALT CHROME ALLOY

I Papageorgiou; E. Ingham; J. Fisher; E. Jones; I. Learmonth; and C.P. Case

Bristol Implant Research Centre, Department Orthopaedic Surgery, University of Bristol, Southmead Hospital

Introduction: Joint replacement surgery is one of the most common operations that take place in United Kingdom. The major problem in total hip arthroplasty is the generation of particulate wear debris and the subsequent biological responses. Wear debris induces osteolysis and a subsequent failure of the implant that lead to the liberation of greater quantities of particulate and soluble debris to bone marrow, blood, lymph nodes, liver and spleen. Recently, it has been suggested that these adverse effects depend not only on the chemical composition but also on the particulate nature of the material (size and shape). Particle size has been shown to influence the inflammatory response of macrophages to wear debris. This study evaluated whether particle size also influences the viability and mutagenic damage.

Methods: Cobalt chrome alloy particles of two sizes (large 2.9±1.1µm, small 0.07±0.04 µm) were generated and characterised by Scanning Electron Microscopy. Different concentrations of particles were added to primary human fibroblasts in tissue culture. The release of cytokines in the medium was assayed by Enzyme-Linked ImunnoSorbent Assay (ELISA). Cell viability was determined by MTT conversion and the degree of DNA damage was quantitatively analysed by the Alkaline Single Cell Gel Electrophoresis (COMET) assay with image analysis.

Results: Small particles initialise DNA damage at much lower volumetric concentrations (0.05 and 0.5 µm3/cell) than larger particles (500 µm3/cell). The difference in the doses was approximately related to the difference in surface area of the particles. DNA damage was related to a delayed decrease in cell viability, which was noted after three days of exposure.

In contrast, the release of the inflammatory cytokine TNF-{alpha} and the multifunctional growth factor TGF-ß-2 occurred at lower doses (0.0005 to 5 µm3/cell for TNF-{alpha} and 0.5 to 50 µm3/cell for TGF-ß-2). No release of IL-6 was detected at any dose. Only growth factor FGF-23 was increased in similar pattern to the DNA damage.

Conclusions: This study has demonstrated important differences between the mutagenicity, toxicity and inflammatory potential of small (nanometre sized) and large (micrometer sized) chrome particles.

Correspondence should be addressed to Mr Carlos Wigderowitz, Honorary Secretary BORS, University Dept of Orthopaedic & Trauma Surgery, Ninewells Hospital & Medical School, Dundee DD1 9SY.






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Hip, Knee, Trauma, Upper limb, Foot & Ankle, Paediatrics, Oncology, Spine, Arthroplasty, General