Large nucleotide-dependent movement of the N-terminal domain of the ClpX chaperone

Guillaume Thibault; Yulia Tsitrin; Toni Davidson; Anna Gribun; Walid A. Houry

doi:10.1038/sj.emboj.7601223

Large nucleotide-dependent movement of the N-terminal domain of the ClpX chaperone

Guillaume Thibault, Yulia Tsitrin, Toni Davidson, Anna Gribun, Walid A. Houry^*

^*Corresponding author for this work

University of Toronto

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

26 Citations (Scopus)

Abstract

The ClpXP ATPase-protease complex is a major component of the protein quality control machinery in the cell. A ClpX subunit consists of an N-terminal zinc binding domain (ZBD) and a C-terminal AAA⁺ domain. ClpX oligomerizes into a hexamer with the AAA⁺ domains forming the base of the hexamer and the ZBDs extending out of the base. Here, we report that ClpX switches between a capture and a feeding conformation. ZBDs in ClpX undergo large nucleotide-dependent block movement towards ClpP and into the AAA ⁺ ring. This motion is modulated by the ClpX cofactor, SspB. Evidence for this movement was initially obtained by the surprising observation that an N-terminal extension on ClpX is clipped by bound ClpP in functional ClpXP complexes. Protease-protection, crosslinking, and light scattering experiments further support these findings.

Original language	English
Pages (from-to)	3367-3376
Number of pages	10
Journal	EMBO Journal
Volume	25
Issue number	14
DOIs	https://doi.org/10.1038/sj.emboj.7601223
Publication status	Published - Jul 26 2006
Externally published	Yes

ASJC Scopus Subject Areas

General Neuroscience
Molecular Biology
General Biochemistry,Genetics and Molecular Biology
General Immunology and Microbiology

Keywords

ClpP
ClpX
Nucleotide-dependent domain movement
Translocation

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10.1038/sj.emboj.7601223

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title = "Large nucleotide-dependent movement of the N-terminal domain of the ClpX chaperone",

abstract = "The ClpXP ATPase-protease complex is a major component of the protein quality control machinery in the cell. A ClpX subunit consists of an N-terminal zinc binding domain (ZBD) and a C-terminal AAA+ domain. ClpX oligomerizes into a hexamer with the AAA+ domains forming the base of the hexamer and the ZBDs extending out of the base. Here, we report that ClpX switches between a capture and a feeding conformation. ZBDs in ClpX undergo large nucleotide-dependent block movement towards ClpP and into the AAA + ring. This motion is modulated by the ClpX cofactor, SspB. Evidence for this movement was initially obtained by the surprising observation that an N-terminal extension on ClpX is clipped by bound ClpP in functional ClpXP complexes. Protease-protection, crosslinking, and light scattering experiments further support these findings.",

keywords = "ClpP, ClpX, Nucleotide-dependent domain movement, Translocation",

author = "Guillaume Thibault and Yulia Tsitrin and Toni Davidson and Anna Gribun and Houry, {Walid A.}",

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doi = "10.1038/sj.emboj.7601223",

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T1 - Large nucleotide-dependent movement of the N-terminal domain of the ClpX chaperone

AU - Thibault, Guillaume

AU - Tsitrin, Yulia

AU - Davidson, Toni

AU - Gribun, Anna

AU - Houry, Walid A.

PY - 2006/7/26

Y1 - 2006/7/26

N2 - The ClpXP ATPase-protease complex is a major component of the protein quality control machinery in the cell. A ClpX subunit consists of an N-terminal zinc binding domain (ZBD) and a C-terminal AAA+ domain. ClpX oligomerizes into a hexamer with the AAA+ domains forming the base of the hexamer and the ZBDs extending out of the base. Here, we report that ClpX switches between a capture and a feeding conformation. ZBDs in ClpX undergo large nucleotide-dependent block movement towards ClpP and into the AAA + ring. This motion is modulated by the ClpX cofactor, SspB. Evidence for this movement was initially obtained by the surprising observation that an N-terminal extension on ClpX is clipped by bound ClpP in functional ClpXP complexes. Protease-protection, crosslinking, and light scattering experiments further support these findings.

AB - The ClpXP ATPase-protease complex is a major component of the protein quality control machinery in the cell. A ClpX subunit consists of an N-terminal zinc binding domain (ZBD) and a C-terminal AAA+ domain. ClpX oligomerizes into a hexamer with the AAA+ domains forming the base of the hexamer and the ZBDs extending out of the base. Here, we report that ClpX switches between a capture and a feeding conformation. ZBDs in ClpX undergo large nucleotide-dependent block movement towards ClpP and into the AAA + ring. This motion is modulated by the ClpX cofactor, SspB. Evidence for this movement was initially obtained by the surprising observation that an N-terminal extension on ClpX is clipped by bound ClpP in functional ClpXP complexes. Protease-protection, crosslinking, and light scattering experiments further support these findings.

KW - ClpP

KW - ClpX

KW - Nucleotide-dependent domain movement

KW - Translocation

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JO - EMBO Journal

JF - EMBO Journal

IS - 14

ER -

Large nucleotide-dependent movement of the N-terminal domain of the ClpX chaperone

Abstract

ASJC Scopus Subject Areas

Keywords

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