4.7 Review

Structural determinants of multimerization and dissociation in 2-Cys peroxiredoxin chaperone function

Journal

STRUCTURE
Volume 29, Issue 7, Pages 640-654

Publisher

CELL PRESS
DOI: 10.1016/j.str.2021.04.007

Keywords

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Funding

  1. Wallenberg Center for Molecular and Translational Medicine, University of Gothenburg
  2. Cancerfonden
  3. Swedish Research Council
  4. Knut och Alice Wallenberg Foundation through a Wallenberg Academy Fellowship
  5. Wallenberg Centre for Molecular and Translational Medicine, University of Gothenburg

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This review focuses on the structural studies and mechanisms underlying the chaperone function of 2-Cys PRDX systems, highlighting the coordination with other molecular chaperones. It also discusses the remarkable structural similarities between 2-Cys PRDXs, small HSPs, and J-domain-independent Hsp40 holdases in terms of their functions and dynamic equilibria.
Peroxiredoxins (PRDXs) are abundant peroxidases present in all kingdoms of life. Recently, they have been shown to also carry out additional roles as molecular chaperones. To address this emerging supplementary function, this review focuses on structural studies of 2-Cys PRDX systems exhibiting chaperone activity. We provide a detailed understanding of the current knowledge of structural determinants underlying the chaperone function of PRDXs. Specifically, we describe the mechanisms which may modulate their quaternary structure to facilitate interactions with client proteins and how they are coordinated with the functions of other molecular chaperones. Following an overview of PRDX molecular architecture, we outline structural details of the presently best-characterized peroxiredoxins exhibiting chaperone function and highlight common denominators. Finally, we discuss the remarkable structural similarities between 2-Cys PRDXs, small HSPs, and J-domain-independent Hsp40 holdases in terms of their functions and dynamic equilibria between lowand high-molecular-weight oligomers.

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