GCUNC-45 Is a Novel Regulator for the Progesterone Receptor/hsp90 Chaperoning Pathway

Author:

Chadli Ahmed1,Graham J. Dinny2,Abel M. Greg2,Jackson Twila A.2,Gordon David F.2,Wood William M.2,Felts Sara J.1,Horwitz Kathryn B.2,Toft David1

Affiliation:

1. Department of Biochemistry and Molecular Biology, Mayo Clinic, Rochester, Minnesota

2. Division of Endocrinology, Department of Medicine, University of Colorado Health Science Center, Denver, Colorado

Abstract

ABSTRACT The hsp90 chaperoning pathway is a multiprotein system that is required for the production or activation of many cell regulatory proteins, including the progesterone receptor (PR). We report here the identity of GCUNC-45 as a novel modulator of PR chaperoning by hsp90. GCUNC-45, previously implicated in the activities of myosins, can interact in vivo and in vitro with both PR-A and PR-B and with hsp90. Overexpression and knockdown experiments show GCUNC-45 to be a positive factor in promoting PR function in the cell. GCUNC-45 binds to the ATP-binding domain of hsp90 to prevent the activation of its ATPase activity by the cochaperone Aha1. This effect limits PR chaperoning by hsp90, but this can be reversed by FKBP52, a cochaperone that is thought to act later in the pathway. These findings reveal a new cochaperone binding site near the N terminus of hsp90, add insight on the role of FKBP52, and identify GCUNC-45 as a novel regulator of the PR signaling pathway.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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