Titanium uptake, induction of RANK-L expression, and enhanced proliferation of human T-lymphocytes

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Abstract

There is increasing evidence that titanium ions are released from orthopedic implants by biocorrosion. Theaim of this study was to investigate titanium uptake by human T-lymphocytes and its effects on phenotype and proliferation. Freshly isolated human nonadherent peripheral blood mononuclear cells (NA-PBMC), were exposed to TiCl4 [Ti(IV)]. Bioavailability and distribution of Ti(IV) in T-lymphocytes was determined by energy-filtered electron microscopy (EFTEM). The effects of Ti(IV) challenge on nonactivated and PHA-activated cells were assessed by flow cytometric analysis of surface markers, RANK-L production, and proliferation assays. EFTEM colocalized Ti(IV) with phosphorus in the nucleus, ribosomes, cytoplasmic membranes, and the surface membrane of T-lymphocytes. Ti(IV) increased significantly the expression of CD69, CCR4, and RANK-L in a concentration-dependent manner. Titanium enters T-lymphocytes through a currently unknown mechanism and binds to phosphorus-rich cell structures. Titanium influences phenotype and function of T-lymphocytes, resulting in activation of a CD69+ and CCR4+ T-lymphocyte population and secretion of RANK-L. These results strongly suggest the involvement of titanium ions challenged T-lymphocytes in the complex pathophysiological mechanisms of aseptic loosening of orthopedic implants. © 2009 Orthopaedic Research Society. Published by Wiley Periodicals, Inc.

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Cadosch, D., Sutanto, M., Chan, E., Mhawi, A., Gautschi, O. P., Von Katterfeld, B., … Filgueira, L. (2010). Titanium uptake, induction of RANK-L expression, and enhanced proliferation of human T-lymphocytes. Journal of Orthopaedic Research, 28(3), 341–347. https://doi.org/10.1002/jor.21013

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