Growth Arrest-specific Protein 1 is a Novel Endogenous Inhibitor of Glomerular Cell Activation and Proliferation

Overview

Journal Kidney Int

Publisher Elsevier

Specialty Nephrology

Date 2012 Dec 21

PMID 23254899

Citations 14

Authors

Claudia R C van Roeyen

Stephanie Zok

Jessica Pruessmeyer

Peter Boor

Yoshikuni Nagayama

Stefan Fleckenstein

Clemens D Cohen

Frank Eitner

Hermann-Josef Grone

Tammo Ostendorf

Andreas Ludwig

Jurgen Floege

Affiliations

Soon will be listed here.

Abstract

Growth arrest-specific protein-1 (GAS1) is a GPI-anchored protein which is highly expressed in embryonic mouse fibroblasts and inhibits their proliferation. Glomerular mesangial cells release soluble GAS1 protein into the supernatant in vitro. Growth arrest led to GAS1 overexpression and increased release. Secretion involved disintegrin and metalloproteinase 10 and 17 as signified by inhibition experiments. Recombinant soluble GAS1 protein inhibited the proliferation of mesangial cells. Conversely, the induction of mesangial cell proliferation by PDGF-BB or -DD led to downregulation of GAS1 mRNA. Specific ligands of the PDGF α-receptor, PDGF-AA and -CC, had no effect. The GAS1 protein was localized in podocytes in kidneys from healthy rats. During the time course of mesangioproliferative glomerulonephritis in anti-Thy1.1-treated rats, glomerular GAS1 expression decreased prior to the onset of mesangial cell proliferation and increased at later stages during glomerular recovery. Finally, a plasmid expressing soluble GAS1 fused to an Fc fragment was systemically overexpressed in rats with mesangioproliferative glomerulonephritis. This ameliorated renal damage was indicated by decreased albuminuria and serum creatinine. Gas1/Fc-transfected rats also exhibited a reduction of the glomerular mesangial cell activation and proliferation. Thus, GAS1 is a novel endogenous inhibitor of glomerular mesangial cell proliferation and may be a novel therapeutic target in mesangioproliferative glomerular diseases.

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