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Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation

Biogenesis of respiratory chain complexes depends on the expression of mitochondrial-encoded subunits. Their synthesis occurs on membrane-associated ribosomes and is probably coupled to their membrane insertion. Defects in expression of mitochondrial translation products are among the major causes o...

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Autores principales: Bauerschmitt, Heike, Mick, David U., Deckers, Markus, Vollmer, Christine, Funes, Soledad, Kehrein, Kirsten, Ott, Martin, Rehling, Peter, Herrmann, Johannes M.
Formato: Texto
Lenguaje:English
Publicado: The American Society for Cell Biology 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2883938/
https://www.ncbi.nlm.nih.gov/pubmed/20427570
http://dx.doi.org/10.1091/mbc.E10-02-0101
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author Bauerschmitt, Heike
Mick, David U.
Deckers, Markus
Vollmer, Christine
Funes, Soledad
Kehrein, Kirsten
Ott, Martin
Rehling, Peter
Herrmann, Johannes M.
author_facet Bauerschmitt, Heike
Mick, David U.
Deckers, Markus
Vollmer, Christine
Funes, Soledad
Kehrein, Kirsten
Ott, Martin
Rehling, Peter
Herrmann, Johannes M.
author_sort Bauerschmitt, Heike
collection PubMed
description Biogenesis of respiratory chain complexes depends on the expression of mitochondrial-encoded subunits. Their synthesis occurs on membrane-associated ribosomes and is probably coupled to their membrane insertion. Defects in expression of mitochondrial translation products are among the major causes of mitochondrial disorders. Mdm38 is related to Letm1, a protein affected in Wolf-Hirschhorn syndrome patients. Like Mba1 and Oxa1, Mdm38 is an inner membrane protein that interacts with ribosomes and is involved in respiratory chain biogenesis. We find that simultaneous loss of Mba1 and Mdm38 causes severe synthetic defects in the biogenesis of cytochrome reductase and cytochrome oxidase. These defects are not due to a compromised membrane binding of ribosomes but the consequence of a mis-regulation in the synthesis of Cox1 and cytochrome b. Cox1 expression is restored by replacing Cox1-specific regulatory regions in the mRNA. We conclude, that Mdm38 and Mba1 exhibit overlapping regulatory functions in translation of selected mitochondrial mRNAs.
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spelling pubmed-28839382010-08-30 Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation Bauerschmitt, Heike Mick, David U. Deckers, Markus Vollmer, Christine Funes, Soledad Kehrein, Kirsten Ott, Martin Rehling, Peter Herrmann, Johannes M. Mol Biol Cell Articles Biogenesis of respiratory chain complexes depends on the expression of mitochondrial-encoded subunits. Their synthesis occurs on membrane-associated ribosomes and is probably coupled to their membrane insertion. Defects in expression of mitochondrial translation products are among the major causes of mitochondrial disorders. Mdm38 is related to Letm1, a protein affected in Wolf-Hirschhorn syndrome patients. Like Mba1 and Oxa1, Mdm38 is an inner membrane protein that interacts with ribosomes and is involved in respiratory chain biogenesis. We find that simultaneous loss of Mba1 and Mdm38 causes severe synthetic defects in the biogenesis of cytochrome reductase and cytochrome oxidase. These defects are not due to a compromised membrane binding of ribosomes but the consequence of a mis-regulation in the synthesis of Cox1 and cytochrome b. Cox1 expression is restored by replacing Cox1-specific regulatory regions in the mRNA. We conclude, that Mdm38 and Mba1 exhibit overlapping regulatory functions in translation of selected mitochondrial mRNAs. The American Society for Cell Biology 2010-06-15 /pmc/articles/PMC2883938/ /pubmed/20427570 http://dx.doi.org/10.1091/mbc.E10-02-0101 Text en © 2010 by The American Society for Cell Biology
spellingShingle Articles
Bauerschmitt, Heike
Mick, David U.
Deckers, Markus
Vollmer, Christine
Funes, Soledad
Kehrein, Kirsten
Ott, Martin
Rehling, Peter
Herrmann, Johannes M.
Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title_full Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title_fullStr Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title_full_unstemmed Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title_short Ribosome-binding Proteins Mdm38 and Mba1 Display Overlapping Functions for Regulation of Mitochondrial Translation
title_sort ribosome-binding proteins mdm38 and mba1 display overlapping functions for regulation of mitochondrial translation
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2883938/
https://www.ncbi.nlm.nih.gov/pubmed/20427570
http://dx.doi.org/10.1091/mbc.E10-02-0101
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