Association of thrombospondin-1 with osteogenic differentiation of retinal pericytes in vitro

Author:

Canfield A.E.1,Sutton A.B.1,Hoyland J.A.1,Schor A.M.1

Affiliation:

1. University of Manchester, School of Biological Sciences, UK.

Abstract

Vascular pericytes can differentiate into osteoblast-like cells in vitro, suggesting that these cells may represent a potential source of osteoprogenitor cells in the adult. Pericyte differentiation is associated with a characteristic pattern of nodule formation and mineralisation. Nodules are formed in post-confluent cultures by the retraction of multilayered areas. Crystals of hydroxyapatite are deposited on the extracellular matrix of these nodules which then becomes mineralised. We now demonstrate that thrombospondin-1 (TSP-1) gene expression is modulated during pericyte differentiation in vitro. That is, the relative levels of TSP-1 (protein and mRNA) increased markedly during nodule formation and then decreased when mineralisation of the nodules had taken place. TSP-1 was localised throughout non-mineralised nodules but it was largely excluded from the inner mass of mineralised nodules. The production of a mineralised matrix by vascular pericytes was promoted by the presence of antibodies to TSP-1 in the culture medium and was inhibited by exogenous TSP-1. These effects did not appear to be mediated through the activation of latent TGF-beta, since neither exogenous TGF-beta nor neutralising antibodies to TGF-beta had any effect on the rate or extent of mineralisation seen in the pericyte cultures. Taken together these results suggest that high levels of TSP-1 inhibit pericyte mineralisation, supporting the view that this protein plays a role in pericyte differentiation and bone formation.

Publisher

The Company of Biologists

Subject

Cell Biology

Reference47 articles.

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4. Role of active and latent transforming growth factor-in bone formation.;Bonewald;J. Cell. Biochem,1994

5. The pericyte as a possible osteoblast progenitor cell.;Brighton;Clin. Orthop,1992

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