Differential Interactions of P23 and the TPR-containing Proteins Hop, Cyp40, FKBP52 and FKBP51 with Hsp90 Mutants

Overview

Journal Cell Stress Chaperones

Publisher Elsevier

Specialty Cell Biology

Date 1998 Jul 22

PMID 9672247

Citations 70

Authors

S Chen

W P SULLIVAN

D O Toft

D F Smith

Affiliations

Soon will be listed here.

Abstract

Hsp90 is required for the normal function of steroid receptors, but its binding to steroid receptors is mediated by Hsc70 and several hsp-associated accessory proteins. An assortment of Hsp90 mutants were tested for their abilities to interact with each of the following accessories: Hop, Cyp40, FKBP52, FKBP51, and p23. Of the 11 Hsp90 mutants tested, all were defective to some extent in associating with progestin (PR) complexes. In every case, however, reduced PR binding correlated with a defect in binding of one or more accessories. Co-precipitation of mutant Hsp90 forms with individual accessories was used to map Hsp90 sequences required for accessory protein interactions. Mutation of Hsp90's highly conserved C-terminal EEVD to AAVD resulted in diminished interactions with several accessory proteins, most particularly with Hop. Deletion of amino acids 661-677 resulted in loss of Hsp90 dimerization and also caused diminished interactions with all accessory proteins. Binding of p23 mapped most strongly to the N-terminal ATP-binding domain of Hsp90 while binding of TPR proteins mapped to the C-terminal half of Hsp90. These results and others further suggest that the N- and C-terminal regions of Hsp90 maintain important conformational links through intramolecular interactions and/or intermolecular influences in homodimers.

Citing Articles

Anti-cancer properties of Sansalvamide A, its derivatives, and analogs: an updated review.

Chagaleti B, Baby K, Pena-Corona S, Leyva-Gomez G, S M S, Naveen N Naunyn Schmiedebergs Arch Pharmacol. 2024; 397(10):7337-7351.

PMID: 38739152 DOI: 10.1007/s00210-024-03129-0.

Hsp90, a team player in protein quality control and the stress response in bacteria.

Wickramaratne A, Wickner S, Kravats A Microbiol Mol Biol Rev. 2024; 88(2):e0017622.

PMID: 38534118 PMC: 11332350. DOI: 10.1128/mmbr.00176-22.

The Histone Chaperone Network Is Highly Conserved in .

Poulet A, Rousselot E, Teletchea S, Noirot C, Jacob Y, van Wolfswinkel J Int J Mol Sci. 2023; 24(2).

PMID: 36674565 PMC: 9864664. DOI: 10.3390/ijms24021051.

Drug resistance in metastatic castration-resistant prostate cancer: an update on the status quo.

Yehya A, Ghamlouche F, Zahwe A, Zeid Y, Wakimian K, Mukherji D Cancer Drug Resist. 2022; 5(3):667-690.

PMID: 36176747 PMC: 9511807. DOI: 10.20517/cdr.2022.15.

With or without You: Co-Chaperones Mediate Health and Disease by Modifying Chaperone Function and Protein Triage.

Altinok S, Sanchez-Hodge R, Stewart M, Smith K, Schisler J Cells. 2021; 10(11).

PMID: 34831344 PMC: 8619055. DOI: 10.3390/cells10113121.