Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy

Cockayne syndrome (CS) is a devastating autosomal recessive disease characterized by neurodegeneration, cachexia, and accelerated aging. 80% of the cases are caused by mutations in the CS complementation group B (CSB) gene known to be involved in DNA repair and transcription. Recent evidence indicat...

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Autores principales: Scheibye-Knudsen, Morten, Ramamoorthy, Mahesh, Sykora, Peter, Maynard, Scott, Lin, Ping-Chang, Minor, Robin K., Wilson III, David M., Cooper, Marcus, Spencer, Richard, de Cabo, Rafael, Croteau, Deborah L., Bohr, Vilhelm A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2012
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3328359/
https://www.ncbi.nlm.nih.gov/pubmed/22473955
http://dx.doi.org/10.1084/jem.20111721
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author Scheibye-Knudsen, Morten
Ramamoorthy, Mahesh
Sykora, Peter
Maynard, Scott
Lin, Ping-Chang
Minor, Robin K.
Wilson III, David M.
Cooper, Marcus
Spencer, Richard
de Cabo, Rafael
Croteau, Deborah L.
Bohr, Vilhelm A.
author_facet Scheibye-Knudsen, Morten
Ramamoorthy, Mahesh
Sykora, Peter
Maynard, Scott
Lin, Ping-Chang
Minor, Robin K.
Wilson III, David M.
Cooper, Marcus
Spencer, Richard
de Cabo, Rafael
Croteau, Deborah L.
Bohr, Vilhelm A.
author_sort Scheibye-Knudsen, Morten
collection PubMed
description Cockayne syndrome (CS) is a devastating autosomal recessive disease characterized by neurodegeneration, cachexia, and accelerated aging. 80% of the cases are caused by mutations in the CS complementation group B (CSB) gene known to be involved in DNA repair and transcription. Recent evidence indicates that CSB is present in mitochondria, where it associates with mitochondrial DNA (mtDNA). We report an increase in metabolism in the CSB(m/m) mouse model and CSB-deficient cells. Mitochondrial content is increased in CSB-deficient cells, whereas autophagy is down-regulated, presumably as a result of defects in the recruitment of P62 and mitochondrial ubiquitination. CSB-deficient cells show increased free radical production and an accumulation of damaged mitochondria. Accordingly, treatment with the autophagic stimulators lithium chloride or rapamycin reverses the bioenergetic phenotype of CSB-deficient cells. Our data imply that CSB acts as an mtDNA damage sensor, inducing mitochondrial autophagy in response to stress, and that pharmacological modulators of autophagy are potential treatment options for this accelerated aging phenotype.
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spelling pubmed-33283592012-10-09 Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy Scheibye-Knudsen, Morten Ramamoorthy, Mahesh Sykora, Peter Maynard, Scott Lin, Ping-Chang Minor, Robin K. Wilson III, David M. Cooper, Marcus Spencer, Richard de Cabo, Rafael Croteau, Deborah L. Bohr, Vilhelm A. J Exp Med Article Cockayne syndrome (CS) is a devastating autosomal recessive disease characterized by neurodegeneration, cachexia, and accelerated aging. 80% of the cases are caused by mutations in the CS complementation group B (CSB) gene known to be involved in DNA repair and transcription. Recent evidence indicates that CSB is present in mitochondria, where it associates with mitochondrial DNA (mtDNA). We report an increase in metabolism in the CSB(m/m) mouse model and CSB-deficient cells. Mitochondrial content is increased in CSB-deficient cells, whereas autophagy is down-regulated, presumably as a result of defects in the recruitment of P62 and mitochondrial ubiquitination. CSB-deficient cells show increased free radical production and an accumulation of damaged mitochondria. Accordingly, treatment with the autophagic stimulators lithium chloride or rapamycin reverses the bioenergetic phenotype of CSB-deficient cells. Our data imply that CSB acts as an mtDNA damage sensor, inducing mitochondrial autophagy in response to stress, and that pharmacological modulators of autophagy are potential treatment options for this accelerated aging phenotype. The Rockefeller University Press 2012-04-09 /pmc/articles/PMC3328359/ /pubmed/22473955 http://dx.doi.org/10.1084/jem.20111721 Text en © 2012 Scheibye-Knudsen et al. This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/).
spellingShingle Article
Scheibye-Knudsen, Morten
Ramamoorthy, Mahesh
Sykora, Peter
Maynard, Scott
Lin, Ping-Chang
Minor, Robin K.
Wilson III, David M.
Cooper, Marcus
Spencer, Richard
de Cabo, Rafael
Croteau, Deborah L.
Bohr, Vilhelm A.
Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title_full Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title_fullStr Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title_full_unstemmed Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title_short Cockayne syndrome group B protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
title_sort cockayne syndrome group b protein prevents the accumulation of damaged mitochondria by promoting mitochondrial autophagy
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3328359/
https://www.ncbi.nlm.nih.gov/pubmed/22473955
http://dx.doi.org/10.1084/jem.20111721
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