Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin

Type I chaperonins (cpn60/Hsp60) are essential proteins that mediate the folding of proteins in bacteria, chloroplast and mitochondria. Despite the high sequence homology among chaperonins, the mitochondrial chaperonin system has developed unique properties that distinguish it from the widely-studie...

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Autores principales: Parnas, Avital, Nisemblat, Shahar, Weiss, Celeste, Levy-Rimler, Galit, Pri-Or, Amir, Zor, Tsaffrir, Lund, Peter A., Bross, Peter, Azem, Abdussalam
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3514286/
https://www.ncbi.nlm.nih.gov/pubmed/23226518
http://dx.doi.org/10.1371/journal.pone.0050318
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author Parnas, Avital
Nisemblat, Shahar
Weiss, Celeste
Levy-Rimler, Galit
Pri-Or, Amir
Zor, Tsaffrir
Lund, Peter A.
Bross, Peter
Azem, Abdussalam
author_facet Parnas, Avital
Nisemblat, Shahar
Weiss, Celeste
Levy-Rimler, Galit
Pri-Or, Amir
Zor, Tsaffrir
Lund, Peter A.
Bross, Peter
Azem, Abdussalam
author_sort Parnas, Avital
collection PubMed
description Type I chaperonins (cpn60/Hsp60) are essential proteins that mediate the folding of proteins in bacteria, chloroplast and mitochondria. Despite the high sequence homology among chaperonins, the mitochondrial chaperonin system has developed unique properties that distinguish it from the widely-studied bacterial system (GroEL and GroES). The most relevant difference to this study is that mitochondrial chaperonins are able to refold denatured proteins only with the assistance of the mitochondrial co-chaperonin. This is in contrast to the bacterial chaperonin, which is able to function with the help of co-chaperonin from any source. The goal of our work was to determine structural elements that govern the specificity between chaperonin and co-chaperonin pairs using mitochondrial Hsp60 as model system. We used a mutagenesis approach to obtain human mitochondrial Hsp60 mutants that are able to function with the bacterial co-chaperonin, GroES. We isolated two mutants, a single mutant (E321K) and a double mutant (R264K/E358K) that, together with GroES, were able to rescue an E. coli strain, in which the endogenous chaperonin system was silenced. Although the mutations are located in the apical domain of the chaperonin, where the interaction with co-chaperonin takes place, none of the residues are located in positions that are directly responsible for co-chaperonin binding. Moreover, while both mutants were able to function with GroES, they showed distinct functional and structural properties. Our results indicate that the phenotype of the E321K mutant is caused mainly by a profound increase in the binding affinity to all co-chaperonins, while the phenotype of R264K/E358K is caused by a slight increase in affinity toward co-chaperonins that is accompanied by an alteration in the allosteric signal transmitted upon nucleotide binding. The latter changes lead to a great increase in affinity for GroES, with only a minor increase in affinity toward the mammalian mitochondrial co-chaperonin.
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spelling pubmed-35142862012-12-05 Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin Parnas, Avital Nisemblat, Shahar Weiss, Celeste Levy-Rimler, Galit Pri-Or, Amir Zor, Tsaffrir Lund, Peter A. Bross, Peter Azem, Abdussalam PLoS One Research Article Type I chaperonins (cpn60/Hsp60) are essential proteins that mediate the folding of proteins in bacteria, chloroplast and mitochondria. Despite the high sequence homology among chaperonins, the mitochondrial chaperonin system has developed unique properties that distinguish it from the widely-studied bacterial system (GroEL and GroES). The most relevant difference to this study is that mitochondrial chaperonins are able to refold denatured proteins only with the assistance of the mitochondrial co-chaperonin. This is in contrast to the bacterial chaperonin, which is able to function with the help of co-chaperonin from any source. The goal of our work was to determine structural elements that govern the specificity between chaperonin and co-chaperonin pairs using mitochondrial Hsp60 as model system. We used a mutagenesis approach to obtain human mitochondrial Hsp60 mutants that are able to function with the bacterial co-chaperonin, GroES. We isolated two mutants, a single mutant (E321K) and a double mutant (R264K/E358K) that, together with GroES, were able to rescue an E. coli strain, in which the endogenous chaperonin system was silenced. Although the mutations are located in the apical domain of the chaperonin, where the interaction with co-chaperonin takes place, none of the residues are located in positions that are directly responsible for co-chaperonin binding. Moreover, while both mutants were able to function with GroES, they showed distinct functional and structural properties. Our results indicate that the phenotype of the E321K mutant is caused mainly by a profound increase in the binding affinity to all co-chaperonins, while the phenotype of R264K/E358K is caused by a slight increase in affinity toward co-chaperonins that is accompanied by an alteration in the allosteric signal transmitted upon nucleotide binding. The latter changes lead to a great increase in affinity for GroES, with only a minor increase in affinity toward the mammalian mitochondrial co-chaperonin. Public Library of Science 2012-12-04 /pmc/articles/PMC3514286/ /pubmed/23226518 http://dx.doi.org/10.1371/journal.pone.0050318 Text en © 2012 Parnas et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Parnas, Avital
Nisemblat, Shahar
Weiss, Celeste
Levy-Rimler, Galit
Pri-Or, Amir
Zor, Tsaffrir
Lund, Peter A.
Bross, Peter
Azem, Abdussalam
Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title_full Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title_fullStr Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title_full_unstemmed Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title_short Identification of Elements That Dictate the Specificity of Mitochondrial Hsp60 for Its Co-Chaperonin
title_sort identification of elements that dictate the specificity of mitochondrial hsp60 for its co-chaperonin
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3514286/
https://www.ncbi.nlm.nih.gov/pubmed/23226518
http://dx.doi.org/10.1371/journal.pone.0050318
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