• Ricardo Rodrigues-Pinto, Stephen M Richardson, and Judith A Hoyland.
• Faculty of Medical and Human Sciences, Centre for Tissue Injury and Repair, Institute of Inflammation and Repair, University of Manchester, Stopford Building, Oxford Road, Manchester, M13 9PT, UK, ricardo.rodriguespinto@postgrad.manchester.ac.uk.
• Eur Spine J. 2014 Sep 1; 23 (9): 1803-14.

AbstractCell-based regenerative medicine therapies have been proposed for repairing the degenerated intervertebral disc (a major cause of back pain). However, for this approach to be successful, it is essential to characterise the phenotype of its native cells to guarantee that implanted cells differentiate and maintain the correct phenotype to ensure appropriate cell and tissue function. While recent studies have increased our knowledge of the human nucleus pulposus (NP) cell phenotype, their ontogeny is still unclear. The expression of notochordal markers by a subpopulation of adult NP cells suggests that, contrary to previous reports, notochord-derived cells are retained in the adult NP, possibly coexisting with a second population of cells originating from the annulus fibrosus or endplate. It is not known, however, how these two cell populations interact and their specific role(s) in disc homeostasis and disease. In particular, notochordal cells are proposed to display both anabolic and protective roles; therefore, they may be the ideal cells to repair the degenerate disc. Thus, understanding the ontogeny of the adult NP cells is paramount, as it will inform the medical and scientific communities as to the ideal phenotype to implant into the degenerate disc and the specific pathways involved in stem cell differentiation towards such a phenotype.

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