Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization

The human AAA+ ATPase CLPB (SKD3) is a protein disaggregase in the mitochondrial intermembrane space (IMS) and functions to promote the solubilization of various mitochondrial proteins. Loss-of-function CLPB mutations are associated with a few human diseases with neutropenia and neurological disorde...

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Autores principales: Wu, Damu, Liu, Yan, Dai, Yuhao, Wang, Guopeng, Lu, Guoliang, Chen, Yan, Li, Ningning, Lin, Jinzhong, Gao, Ning
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9934407/
https://www.ncbi.nlm.nih.gov/pubmed/36745679
http://dx.doi.org/10.1371/journal.pbio.3001987
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author Wu, Damu
Liu, Yan
Dai, Yuhao
Wang, Guopeng
Lu, Guoliang
Chen, Yan
Li, Ningning
Lin, Jinzhong
Gao, Ning
author_facet Wu, Damu
Liu, Yan
Dai, Yuhao
Wang, Guopeng
Lu, Guoliang
Chen, Yan
Li, Ningning
Lin, Jinzhong
Gao, Ning
author_sort Wu, Damu
collection PubMed
description The human AAA+ ATPase CLPB (SKD3) is a protein disaggregase in the mitochondrial intermembrane space (IMS) and functions to promote the solubilization of various mitochondrial proteins. Loss-of-function CLPB mutations are associated with a few human diseases with neutropenia and neurological disorders. Unlike canonical AAA+ proteins, CLPB contains a unique ankyrin repeat domain (ANK) at its N-terminus. How CLPB functions as a disaggregase and the role of its ANK domain are currently unclear. Herein, we report a comprehensive structural characterization of human CLPB in both the apo- and substrate-bound states. CLPB assembles into homo-tetradecamers in apo-state and is remodeled into homo-dodecamers upon substrate binding. Conserved pore-loops (PLs) on the ATPase domains form a spiral staircase to grip and translocate the substrate in a step-size of 2 amino acid residues. The ANK domain is not only responsible for maintaining the higher-order assembly but also essential for the disaggregase activity. Interactome analysis suggests that the ANK domain may directly interact with a variety of mitochondrial substrates. These results reveal unique properties of CLPB as a general disaggregase in mitochondria and highlight its potential as a target for the treatment of various mitochondria-related diseases.
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spelling pubmed-99344072023-02-17 Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization Wu, Damu Liu, Yan Dai, Yuhao Wang, Guopeng Lu, Guoliang Chen, Yan Li, Ningning Lin, Jinzhong Gao, Ning PLoS Biol Research Article The human AAA+ ATPase CLPB (SKD3) is a protein disaggregase in the mitochondrial intermembrane space (IMS) and functions to promote the solubilization of various mitochondrial proteins. Loss-of-function CLPB mutations are associated with a few human diseases with neutropenia and neurological disorders. Unlike canonical AAA+ proteins, CLPB contains a unique ankyrin repeat domain (ANK) at its N-terminus. How CLPB functions as a disaggregase and the role of its ANK domain are currently unclear. Herein, we report a comprehensive structural characterization of human CLPB in both the apo- and substrate-bound states. CLPB assembles into homo-tetradecamers in apo-state and is remodeled into homo-dodecamers upon substrate binding. Conserved pore-loops (PLs) on the ATPase domains form a spiral staircase to grip and translocate the substrate in a step-size of 2 amino acid residues. The ANK domain is not only responsible for maintaining the higher-order assembly but also essential for the disaggregase activity. Interactome analysis suggests that the ANK domain may directly interact with a variety of mitochondrial substrates. These results reveal unique properties of CLPB as a general disaggregase in mitochondria and highlight its potential as a target for the treatment of various mitochondria-related diseases. Public Library of Science 2023-02-06 /pmc/articles/PMC9934407/ /pubmed/36745679 http://dx.doi.org/10.1371/journal.pbio.3001987 Text en © 2023 Wu et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Wu, Damu
Liu, Yan
Dai, Yuhao
Wang, Guopeng
Lu, Guoliang
Chen, Yan
Li, Ningning
Lin, Jinzhong
Gao, Ning
Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title_full Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title_fullStr Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title_full_unstemmed Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title_short Comprehensive structural characterization of the human AAA+ disaggregase CLPB in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
title_sort comprehensive structural characterization of the human aaa+ disaggregase clpb in the apo- and substrate-bound states reveals a unique mode of action driven by oligomerization
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9934407/
https://www.ncbi.nlm.nih.gov/pubmed/36745679
http://dx.doi.org/10.1371/journal.pbio.3001987
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