Inhibition of PDGF-stimulated and Matrix-mediated Proliferation of Human Vascular Smooth Muscle Cells by SPARC is Independent of Changes in Cell Shape or Cyclin-dependent Kinase Inhibitors

Overview

Journal J Cell Biochem

Specialties Biochemistry
Cell Biology

Date 2002 Feb 9

PMID 11835401

Citations 33

Authors

Kouros Motamed

Sarah E Funk

Hidenori Koyama

Russell Ross

Elaine W Raines

E Helene Sage

Affiliations

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Abstract

Interactions among growth factors, cells, and extracellular matrix regulate proliferation during normal development and in pathologies such as atherosclerosis. SPARC (secreted protein, acidic, and rich in cysteine) is a matrix-associated glycoprotein that modulates the adhesion and proliferation of vascular cells. In this study, we demonstrate that SPARC inhibits human arterial smooth muscle cell proliferation stimulated by platelet-derived growth factor or by adhesion to monomeric type I collagen. Binding studies with SPARC and SPARC peptides indicate specific and saturable interaction with smooth muscle cells that involves the C-terminal Ca2+-binding region of the protein. We also report that SPARC arrests monomeric collagen-supported smooth muscle cell proliferation in the late G1-phase of the cell cycle in the absence of an effect on cell shape or on levels of cyclin-dependent kinase inhibitors. Cyclin-dependent kinase-2 activity, p107 and cyclin A levels, and retinoblastoma protein phosphorylation are markedly reduced in response to the addition of exogenous SPARC and/or peptides derived from specific domains of SPARC. Thus, SPARC, previously characterized as an inhibitor of platelet-derived growth factor binding to its receptor, also antagonizes smooth muscle cell proliferation mediated by monomeric collagen at the level of cyclin-dependent kinase-2 activity.

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