Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome

Here we demonstrate association of variants in the mitochondrial asparaginyl-tRNA synthetase NARS2 with human hearing loss and Leigh syndrome. A homozygous missense mutation ([c.637G>T; p.Val213Phe]) is the underlying cause of nonsyndromic hearing loss (DFNB94) and compound heterozygous mutations...

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Autores principales: Simon, Mariella, Richard, Elodie M., Wang, Xinjian, Shahzad, Mohsin, Huang, Vincent H., Qaiser, Tanveer A., Potluri, Prasanth, Mahl, Sarah E., Davila, Antonio, Nazli, Sabiha, Hancock, Saege, Yu, Margret, Gargus, Jay, Chang, Richard, Al-sheqaih, Nada, Newman, William G., Abdenur, Jose, Starr, Arnold, Hegde, Rashmi, Dorn, Thomas, Busch, Anke, Park, Eddie, Wu, Jie, Schwenzer, Hagen, Flierl, Adrian, Florentz, Catherine, Sissler, Marie, Khan, Shaheen N., Li, Ronghua, Guan, Min-Xin, Friedman, Thomas B., Wu, Doris K., Procaccio, Vincent, Riazuddin, Sheikh, Wallace, Douglas C., Ahmed, Zubair M., Huang, Taosheng, Riazuddin, Saima
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4373692/
https://www.ncbi.nlm.nih.gov/pubmed/25807530
http://dx.doi.org/10.1371/journal.pgen.1005097
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author Simon, Mariella
Richard, Elodie M.
Wang, Xinjian
Shahzad, Mohsin
Huang, Vincent H.
Qaiser, Tanveer A.
Potluri, Prasanth
Mahl, Sarah E.
Davila, Antonio
Nazli, Sabiha
Hancock, Saege
Yu, Margret
Gargus, Jay
Chang, Richard
Al-sheqaih, Nada
Newman, William G.
Abdenur, Jose
Starr, Arnold
Hegde, Rashmi
Dorn, Thomas
Busch, Anke
Park, Eddie
Wu, Jie
Schwenzer, Hagen
Flierl, Adrian
Florentz, Catherine
Sissler, Marie
Khan, Shaheen N.
Li, Ronghua
Guan, Min-Xin
Friedman, Thomas B.
Wu, Doris K.
Procaccio, Vincent
Riazuddin, Sheikh
Wallace, Douglas C.
Ahmed, Zubair M.
Huang, Taosheng
Riazuddin, Saima
author_facet Simon, Mariella
Richard, Elodie M.
Wang, Xinjian
Shahzad, Mohsin
Huang, Vincent H.
Qaiser, Tanveer A.
Potluri, Prasanth
Mahl, Sarah E.
Davila, Antonio
Nazli, Sabiha
Hancock, Saege
Yu, Margret
Gargus, Jay
Chang, Richard
Al-sheqaih, Nada
Newman, William G.
Abdenur, Jose
Starr, Arnold
Hegde, Rashmi
Dorn, Thomas
Busch, Anke
Park, Eddie
Wu, Jie
Schwenzer, Hagen
Flierl, Adrian
Florentz, Catherine
Sissler, Marie
Khan, Shaheen N.
Li, Ronghua
Guan, Min-Xin
Friedman, Thomas B.
Wu, Doris K.
Procaccio, Vincent
Riazuddin, Sheikh
Wallace, Douglas C.
Ahmed, Zubair M.
Huang, Taosheng
Riazuddin, Saima
author_sort Simon, Mariella
collection PubMed
description Here we demonstrate association of variants in the mitochondrial asparaginyl-tRNA synthetase NARS2 with human hearing loss and Leigh syndrome. A homozygous missense mutation ([c.637G>T; p.Val213Phe]) is the underlying cause of nonsyndromic hearing loss (DFNB94) and compound heterozygous mutations ([c.969T>A; p.Tyr323*] + [c.1142A>G; p.Asn381Ser]) result in mitochondrial respiratory chain deficiency and Leigh syndrome, which is a neurodegenerative disease characterized by symmetric, bilateral lesions in the basal ganglia, thalamus, and brain stem. The severity of the genetic lesions and their effects on NARS2 protein structure cosegregate with the phenotype. A hypothetical truncated NARS2 protein, secondary to the Leigh syndrome mutation p.Tyr323* is not detectable and p.Asn381Ser further decreases NARS2 protein levels in patient fibroblasts. p.Asn381Ser also disrupts dimerization of NARS2, while the hearing loss p.Val213Phe variant has no effect on NARS2 oligomerization. Additionally we demonstrate decreased steady-state levels of mt-tRNA(Asn) in fibroblasts from the Leigh syndrome patients. In these cells we show that a decrease in oxygen consumption rates (OCR) and electron transport chain (ETC) activity can be rescued by overexpression of wild type NARS2. However, overexpression of the hearing loss associated p.Val213Phe mutant protein in these fibroblasts cannot complement the OCR and ETC defects. Our findings establish lesions in NARS2 as a new cause for nonsyndromic hearing loss and Leigh syndrome.
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spelling pubmed-43736922015-03-27 Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome Simon, Mariella Richard, Elodie M. Wang, Xinjian Shahzad, Mohsin Huang, Vincent H. Qaiser, Tanveer A. Potluri, Prasanth Mahl, Sarah E. Davila, Antonio Nazli, Sabiha Hancock, Saege Yu, Margret Gargus, Jay Chang, Richard Al-sheqaih, Nada Newman, William G. Abdenur, Jose Starr, Arnold Hegde, Rashmi Dorn, Thomas Busch, Anke Park, Eddie Wu, Jie Schwenzer, Hagen Flierl, Adrian Florentz, Catherine Sissler, Marie Khan, Shaheen N. Li, Ronghua Guan, Min-Xin Friedman, Thomas B. Wu, Doris K. Procaccio, Vincent Riazuddin, Sheikh Wallace, Douglas C. Ahmed, Zubair M. Huang, Taosheng Riazuddin, Saima PLoS Genet Research Article Here we demonstrate association of variants in the mitochondrial asparaginyl-tRNA synthetase NARS2 with human hearing loss and Leigh syndrome. A homozygous missense mutation ([c.637G>T; p.Val213Phe]) is the underlying cause of nonsyndromic hearing loss (DFNB94) and compound heterozygous mutations ([c.969T>A; p.Tyr323*] + [c.1142A>G; p.Asn381Ser]) result in mitochondrial respiratory chain deficiency and Leigh syndrome, which is a neurodegenerative disease characterized by symmetric, bilateral lesions in the basal ganglia, thalamus, and brain stem. The severity of the genetic lesions and their effects on NARS2 protein structure cosegregate with the phenotype. A hypothetical truncated NARS2 protein, secondary to the Leigh syndrome mutation p.Tyr323* is not detectable and p.Asn381Ser further decreases NARS2 protein levels in patient fibroblasts. p.Asn381Ser also disrupts dimerization of NARS2, while the hearing loss p.Val213Phe variant has no effect on NARS2 oligomerization. Additionally we demonstrate decreased steady-state levels of mt-tRNA(Asn) in fibroblasts from the Leigh syndrome patients. In these cells we show that a decrease in oxygen consumption rates (OCR) and electron transport chain (ETC) activity can be rescued by overexpression of wild type NARS2. However, overexpression of the hearing loss associated p.Val213Phe mutant protein in these fibroblasts cannot complement the OCR and ETC defects. Our findings establish lesions in NARS2 as a new cause for nonsyndromic hearing loss and Leigh syndrome. Public Library of Science 2015-03-25 /pmc/articles/PMC4373692/ /pubmed/25807530 http://dx.doi.org/10.1371/journal.pgen.1005097 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Simon, Mariella
Richard, Elodie M.
Wang, Xinjian
Shahzad, Mohsin
Huang, Vincent H.
Qaiser, Tanveer A.
Potluri, Prasanth
Mahl, Sarah E.
Davila, Antonio
Nazli, Sabiha
Hancock, Saege
Yu, Margret
Gargus, Jay
Chang, Richard
Al-sheqaih, Nada
Newman, William G.
Abdenur, Jose
Starr, Arnold
Hegde, Rashmi
Dorn, Thomas
Busch, Anke
Park, Eddie
Wu, Jie
Schwenzer, Hagen
Flierl, Adrian
Florentz, Catherine
Sissler, Marie
Khan, Shaheen N.
Li, Ronghua
Guan, Min-Xin
Friedman, Thomas B.
Wu, Doris K.
Procaccio, Vincent
Riazuddin, Sheikh
Wallace, Douglas C.
Ahmed, Zubair M.
Huang, Taosheng
Riazuddin, Saima
Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title_full Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title_fullStr Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title_full_unstemmed Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title_short Mutations of Human NARS2, Encoding the Mitochondrial Asparaginyl-tRNA Synthetase, Cause Nonsyndromic Deafness and Leigh Syndrome
title_sort mutations of human nars2, encoding the mitochondrial asparaginyl-trna synthetase, cause nonsyndromic deafness and leigh syndrome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4373692/
https://www.ncbi.nlm.nih.gov/pubmed/25807530
http://dx.doi.org/10.1371/journal.pgen.1005097
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