An unstructured C-terminal region of the Hsp90 co-chaperone p23 is important for its chaperone function

Tina Weikl; Kerstin Abelmann; Johannes Buchner

doi:10.1006/jmbi.1999.3172

An unstructured C-terminal region of the Hsp90 co-chaperone p23 is important for its chaperone function

Tina Weikl, Kerstin Abelmann, Johannes Buchner

Chair of Biotechnology

Technical University of Munich

Research output: Contribution to journal › Article › peer-review

90 Scopus citations

Abstract

p23 is a co-chaperone of the heat shock protein Hsp90. p23 binds to Hsp90 in its ATP-bound state and, on its own, interacts specifically with non-native proteins. In our attempt to correlate these functions to specific regions of p23 we have identified an unstructured region in p23 that maps to the C-terminal part of the protein sequence. This unstructured region is dispensible for interaction of p23 with Hsp90, since truncated p23 can still form complexes with Hsp90. In contrast, however, truncation of the C-terminal 30 amino acid residues of p23 affects the ability of p23 to bind non-native proteins and to prevent their non-specific aggregation. The isolated C-terminal region itself is not able to act as a chaperone nor is it possible to complement truncated p23 by addition of this peptide. These results imply that the binding site for Hsp90 is contained in the folded domain of p23 and that for efficient interaction of p23 with non-native proteins both the folded domain and the C-terminal unstructured region are required.

Original language	English
Pages (from-to)	685-691
Number of pages	7
Journal	Journal of Molecular Biology
Volume	293
Issue number	3
DOIs	https://doi.org/10.1006/jmbi.1999.3172
State	Published - 29 Oct 1999

Keywords

Aggregation
Heat shock proteins
Molecular chaperones
Protein folding
Steroid hormone receptors

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10.1006/jmbi.1999.3172

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title = "An unstructured C-terminal region of the Hsp90 co-chaperone p23 is important for its chaperone function",

abstract = "p23 is a co-chaperone of the heat shock protein Hsp90. p23 binds to Hsp90 in its ATP-bound state and, on its own, interacts specifically with non-native proteins. In our attempt to correlate these functions to specific regions of p23 we have identified an unstructured region in p23 that maps to the C-terminal part of the protein sequence. This unstructured region is dispensible for interaction of p23 with Hsp90, since truncated p23 can still form complexes with Hsp90. In contrast, however, truncation of the C-terminal 30 amino acid residues of p23 affects the ability of p23 to bind non-native proteins and to prevent their non-specific aggregation. The isolated C-terminal region itself is not able to act as a chaperone nor is it possible to complement truncated p23 by addition of this peptide. These results imply that the binding site for Hsp90 is contained in the folded domain of p23 and that for efficient interaction of p23 with non-native proteins both the folded domain and the C-terminal unstructured region are required.",

keywords = "Aggregation, Heat shock proteins, Molecular chaperones, Protein folding, Steroid hormone receptors",

author = "Tina Weikl and Kerstin Abelmann and Johannes Buchner",

note = "Funding Information: We thank Dr David O. Toft for providing the expression plasmid for human p23 and Dr Susanne Modrow for synthesizing the peptide PEP1. Furthermore, we thank Dr Peter R{\"u}cknagel for mass spectrometry measurements, Dr Rainer Deutzmann for N-terminal sequencing of the proteolytic fragment and Dr Martina Beissinger for helpful discussions. We are grateful to the Experimental Drug Division of the National Cancer Institute for providing geldanamycin. Sf9 cell growth, treatment, and harvesting were conducted by Drs Dean Edwards and Kurt Christensen at the University of Colorado Cancer Center Tissue Culture Core. This work was supported by the Deutsche Forschungsgemeinschaft, the Bundesministerium f{\"u}r Bildung, Wissenschaft, Forschung und Technologie, and the Fonds der chemischen Industrie.",

year = "1999",

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doi = "10.1006/jmbi.1999.3172",

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pages = "685--691",

journal = "Journal of Molecular Biology",

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AU - Weikl, Tina

AU - Abelmann, Kerstin

AU - Buchner, Johannes

N1 - Funding Information: We thank Dr David O. Toft for providing the expression plasmid for human p23 and Dr Susanne Modrow for synthesizing the peptide PEP1. Furthermore, we thank Dr Peter Rücknagel for mass spectrometry measurements, Dr Rainer Deutzmann for N-terminal sequencing of the proteolytic fragment and Dr Martina Beissinger for helpful discussions. We are grateful to the Experimental Drug Division of the National Cancer Institute for providing geldanamycin. Sf9 cell growth, treatment, and harvesting were conducted by Drs Dean Edwards and Kurt Christensen at the University of Colorado Cancer Center Tissue Culture Core. This work was supported by the Deutsche Forschungsgemeinschaft, the Bundesministerium für Bildung, Wissenschaft, Forschung und Technologie, and the Fonds der chemischen Industrie.

PY - 1999/10/29

Y1 - 1999/10/29

N2 - p23 is a co-chaperone of the heat shock protein Hsp90. p23 binds to Hsp90 in its ATP-bound state and, on its own, interacts specifically with non-native proteins. In our attempt to correlate these functions to specific regions of p23 we have identified an unstructured region in p23 that maps to the C-terminal part of the protein sequence. This unstructured region is dispensible for interaction of p23 with Hsp90, since truncated p23 can still form complexes with Hsp90. In contrast, however, truncation of the C-terminal 30 amino acid residues of p23 affects the ability of p23 to bind non-native proteins and to prevent their non-specific aggregation. The isolated C-terminal region itself is not able to act as a chaperone nor is it possible to complement truncated p23 by addition of this peptide. These results imply that the binding site for Hsp90 is contained in the folded domain of p23 and that for efficient interaction of p23 with non-native proteins both the folded domain and the C-terminal unstructured region are required.

AB - p23 is a co-chaperone of the heat shock protein Hsp90. p23 binds to Hsp90 in its ATP-bound state and, on its own, interacts specifically with non-native proteins. In our attempt to correlate these functions to specific regions of p23 we have identified an unstructured region in p23 that maps to the C-terminal part of the protein sequence. This unstructured region is dispensible for interaction of p23 with Hsp90, since truncated p23 can still form complexes with Hsp90. In contrast, however, truncation of the C-terminal 30 amino acid residues of p23 affects the ability of p23 to bind non-native proteins and to prevent their non-specific aggregation. The isolated C-terminal region itself is not able to act as a chaperone nor is it possible to complement truncated p23 by addition of this peptide. These results imply that the binding site for Hsp90 is contained in the folded domain of p23 and that for efficient interaction of p23 with non-native proteins both the folded domain and the C-terminal unstructured region are required.

KW - Aggregation

KW - Heat shock proteins

KW - Molecular chaperones

KW - Protein folding

KW - Steroid hormone receptors

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JO - Journal of Molecular Biology

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ER -

An unstructured C-terminal region of the Hsp90 co-chaperone p23 is important for its chaperone function

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Keywords

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