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¹ Department of Pharmacology and Biological Chemistry, Mount Sinai School of Medicine, New York, NY 10029
² Department of Microbiology and Molecular Genetics, University of Dentistry and Medicine of New Jersey, New Jersey Medical School, Newark, NJ 07103

Address correspondence to Avrom J. Caplan, Department of Pharmacology and Biological Chemistry, Box 1603, Mount Sinai School of Medicine, One Gustave L. Levy Place, New York, NY 10029. Tel.: (212) 241-6563. Fax: (212) 860-1174. E-mail: avrom.caplan{at}mssm.edu

Cdc37 is a molecular chaperone required for folding of protein kinases. It functions in association with Hsp90, although little is known of its mechanism of action or where it fits into a folding pathway involving other Hsp90 cochaperones. Using a genetic approach with Saccharomyces cerevisiae, we show that CDC37 overexpression suppressed a defect in v-Src folding in yeast deleted for STI1, which recruits Hsp90 to misfolded clients. Expression of CDC37 truncation mutants that were deleted for the Hsp90-binding site stabilized v-Src and led to some folding in both sti1 and hsc82 strains. The protein kinase–binding domain of Cdc37 was sufficient for yeast cell viability and permitted efficient signaling through the yeast MAP kinase–signaling pathway. We propose a model in which Cdc37 can function independently of Hsp90, although its ability to do so is restricted by its normally low expression levels. This may be a form of regulation by which cells restrict access to Cdc37 until it has passed through a triage involving other chaperones such as Hsp70 and Hsp90.

Key Words: chaperone; Cdc37; v-Src; Hsp90; yeast

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