Mitochondrial stress response triggered by defects in protein synthesis quality control

Mitochondria have a compartmentalized gene expression system dedicated to the synthesis of membrane proteins essential for oxidative phosphorylation. Responsive quality control mechanisms are needed to ensure that aberrant protein synthesis does not disrupt mitochondrial function. Pathogenic mutatio...

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Autores principales: Richter, Uwe, Ng, Kah Ying, Suomi, Fumi, Marttinen, Paula, Turunen, Taina, Jackson, Christopher, Suomalainen, Anu, Vihinen, Helena, Jokitalo, Eija, Nyman, Tuula A, Isokallio, Marita A, Stewart, James B, Mancini, Cecilia, Brusco, Alfredo, Seneca, Sara, Lombès, Anne, Taylor, Robert W, Battersby, Brendan J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2019
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6348486/
https://www.ncbi.nlm.nih.gov/pubmed/30683687
http://dx.doi.org/10.26508/lsa.201800219
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author Richter, Uwe
Ng, Kah Ying
Suomi, Fumi
Marttinen, Paula
Turunen, Taina
Jackson, Christopher
Suomalainen, Anu
Vihinen, Helena
Jokitalo, Eija
Nyman, Tuula A
Isokallio, Marita A
Stewart, James B
Mancini, Cecilia
Brusco, Alfredo
Seneca, Sara
Lombès, Anne
Taylor, Robert W
Battersby, Brendan J
author_facet Richter, Uwe
Ng, Kah Ying
Suomi, Fumi
Marttinen, Paula
Turunen, Taina
Jackson, Christopher
Suomalainen, Anu
Vihinen, Helena
Jokitalo, Eija
Nyman, Tuula A
Isokallio, Marita A
Stewart, James B
Mancini, Cecilia
Brusco, Alfredo
Seneca, Sara
Lombès, Anne
Taylor, Robert W
Battersby, Brendan J
author_sort Richter, Uwe
collection PubMed
description Mitochondria have a compartmentalized gene expression system dedicated to the synthesis of membrane proteins essential for oxidative phosphorylation. Responsive quality control mechanisms are needed to ensure that aberrant protein synthesis does not disrupt mitochondrial function. Pathogenic mutations that impede the function of the mitochondrial matrix quality control protease complex composed of AFG3L2 and paraplegin cause a multifaceted clinical syndrome. At the cell and molecular level, defects to this quality control complex are defined by impairment to mitochondrial form and function. Here, we establish the etiology of these phenotypes. We show how disruptions to the quality control of mitochondrial protein synthesis trigger a sequential stress response characterized first by OMA1 activation followed by loss of mitochondrial ribosomes and by remodelling of mitochondrial inner membrane ultrastructure. Inhibiting mitochondrial protein synthesis with chloramphenicol completely blocks this stress response. Together, our data establish a mechanism linking major cell biological phenotypes of AFG3L2 pathogenesis and show how modulation of mitochondrial protein synthesis can exert a beneficial effect on organelle homeostasis.
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spelling pubmed-63484862019-01-29 Mitochondrial stress response triggered by defects in protein synthesis quality control Richter, Uwe Ng, Kah Ying Suomi, Fumi Marttinen, Paula Turunen, Taina Jackson, Christopher Suomalainen, Anu Vihinen, Helena Jokitalo, Eija Nyman, Tuula A Isokallio, Marita A Stewart, James B Mancini, Cecilia Brusco, Alfredo Seneca, Sara Lombès, Anne Taylor, Robert W Battersby, Brendan J Life Sci Alliance Research Articles Mitochondria have a compartmentalized gene expression system dedicated to the synthesis of membrane proteins essential for oxidative phosphorylation. Responsive quality control mechanisms are needed to ensure that aberrant protein synthesis does not disrupt mitochondrial function. Pathogenic mutations that impede the function of the mitochondrial matrix quality control protease complex composed of AFG3L2 and paraplegin cause a multifaceted clinical syndrome. At the cell and molecular level, defects to this quality control complex are defined by impairment to mitochondrial form and function. Here, we establish the etiology of these phenotypes. We show how disruptions to the quality control of mitochondrial protein synthesis trigger a sequential stress response characterized first by OMA1 activation followed by loss of mitochondrial ribosomes and by remodelling of mitochondrial inner membrane ultrastructure. Inhibiting mitochondrial protein synthesis with chloramphenicol completely blocks this stress response. Together, our data establish a mechanism linking major cell biological phenotypes of AFG3L2 pathogenesis and show how modulation of mitochondrial protein synthesis can exert a beneficial effect on organelle homeostasis. Life Science Alliance LLC 2019-01-25 /pmc/articles/PMC6348486/ /pubmed/30683687 http://dx.doi.org/10.26508/lsa.201800219 Text en © 2019 Richter et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Richter, Uwe
Ng, Kah Ying
Suomi, Fumi
Marttinen, Paula
Turunen, Taina
Jackson, Christopher
Suomalainen, Anu
Vihinen, Helena
Jokitalo, Eija
Nyman, Tuula A
Isokallio, Marita A
Stewart, James B
Mancini, Cecilia
Brusco, Alfredo
Seneca, Sara
Lombès, Anne
Taylor, Robert W
Battersby, Brendan J
Mitochondrial stress response triggered by defects in protein synthesis quality control
title Mitochondrial stress response triggered by defects in protein synthesis quality control
title_full Mitochondrial stress response triggered by defects in protein synthesis quality control
title_fullStr Mitochondrial stress response triggered by defects in protein synthesis quality control
title_full_unstemmed Mitochondrial stress response triggered by defects in protein synthesis quality control
title_short Mitochondrial stress response triggered by defects in protein synthesis quality control
title_sort mitochondrial stress response triggered by defects in protein synthesis quality control
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6348486/
https://www.ncbi.nlm.nih.gov/pubmed/30683687
http://dx.doi.org/10.26508/lsa.201800219
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