Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease

OBJECTIVE: Pathologic ribonuclease H1 (RNase H1) causes aberrant mitochondrial DNA (mtDNA) segregation and is associated with multiple mtDNA deletions. We aimed to determine the prevalence of RNase H1 gene (RNASEH1) mutations among patients with mitochondrial disease and establish clinically meaning...

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Autores principales: Bugiardini, Enrico, Poole, Olivia V., Manole, Andreea, Pittman, Alan M., Horga, Alejandro, Hargreaves, Iain, Woodward, Cathy E., Sweeney, Mary G., Holton, Janice L., Taanman, Jan-Willem, Plant, Gordon T., Poulton, Joanna, Zeviani, Massimo, Ghezzi, Daniele, Taylor, John, Smith, Conrad, Fratter, Carl, Kanikannan, Meena A., Paramasivam, Arumugam, Thangaraj, Kumarasamy, Spinazzola, Antonella, Holt, Ian J., Houlden, Henry, Hanna, Michael G., Pitceathly, Robert D.S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wolters Kluwer 2017
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5413961/
https://www.ncbi.nlm.nih.gov/pubmed/28508084
http://dx.doi.org/10.1212/NXG.0000000000000149
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author Bugiardini, Enrico
Poole, Olivia V.
Manole, Andreea
Pittman, Alan M.
Horga, Alejandro
Hargreaves, Iain
Woodward, Cathy E.
Sweeney, Mary G.
Holton, Janice L.
Taanman, Jan-Willem
Plant, Gordon T.
Poulton, Joanna
Zeviani, Massimo
Ghezzi, Daniele
Taylor, John
Smith, Conrad
Fratter, Carl
Kanikannan, Meena A.
Paramasivam, Arumugam
Thangaraj, Kumarasamy
Spinazzola, Antonella
Holt, Ian J.
Houlden, Henry
Hanna, Michael G.
Pitceathly, Robert D.S.
author_facet Bugiardini, Enrico
Poole, Olivia V.
Manole, Andreea
Pittman, Alan M.
Horga, Alejandro
Hargreaves, Iain
Woodward, Cathy E.
Sweeney, Mary G.
Holton, Janice L.
Taanman, Jan-Willem
Plant, Gordon T.
Poulton, Joanna
Zeviani, Massimo
Ghezzi, Daniele
Taylor, John
Smith, Conrad
Fratter, Carl
Kanikannan, Meena A.
Paramasivam, Arumugam
Thangaraj, Kumarasamy
Spinazzola, Antonella
Holt, Ian J.
Houlden, Henry
Hanna, Michael G.
Pitceathly, Robert D.S.
author_sort Bugiardini, Enrico
collection PubMed
description OBJECTIVE: Pathologic ribonuclease H1 (RNase H1) causes aberrant mitochondrial DNA (mtDNA) segregation and is associated with multiple mtDNA deletions. We aimed to determine the prevalence of RNase H1 gene (RNASEH1) mutations among patients with mitochondrial disease and establish clinically meaningful genotype-phenotype correlations. METHODS: RNASEH1 was analyzed in patients with (1) multiple deletions/depletion of muscle mtDNA and (2) mendelian progressive external ophthalmoplegia (PEO) with neuropathologic evidence of mitochondrial dysfunction, but no detectable multiple deletions/depletion of muscle mtDNA. Clinicopathologic and molecular evaluation of the newly identified and previously reported patients harboring RNASEH1 mutations was subsequently undertaken. RESULTS: Pathogenic c.424G>A p.Val142Ile RNASEH1 mutations were detected in 3 pedigrees among the 74 probands screened. Given that all 3 families had Indian ancestry, RNASEH1 genetic analysis was undertaken in 50 additional Indian probands with variable clinical presentations associated with multiple mtDNA deletions, but no further RNASEH1 mutations were confirmed. RNASEH1-related mitochondrial disease was characterized by PEO (100%), cerebellar ataxia (57%), and dysphagia (50%). The ataxia neuropathy spectrum phenotype was observed in 1 patient. Although the c.424G>A p.Val142Ile mutation underpins all reported RNASEH1-related mitochondrial disease, haplotype analysis suggested an independent origin, rather than a founder event, for the variant in our families. CONCLUSIONS: In our cohort, RNASEH1 mutations represent the fourth most common cause of adult mendelian PEO associated with multiple mtDNA deletions, following mutations in POLG, RRM2B, and TWNK. RNASEH1 genetic analysis should also be considered in all patients with POLG-negative ataxia neuropathy spectrum. The pathophysiologic mechanisms by which the c.424G>A p.Val142Ile mutation impairs human RNase H1 warrant further investigation.
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spelling pubmed-54139612017-05-15 Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease Bugiardini, Enrico Poole, Olivia V. Manole, Andreea Pittman, Alan M. Horga, Alejandro Hargreaves, Iain Woodward, Cathy E. Sweeney, Mary G. Holton, Janice L. Taanman, Jan-Willem Plant, Gordon T. Poulton, Joanna Zeviani, Massimo Ghezzi, Daniele Taylor, John Smith, Conrad Fratter, Carl Kanikannan, Meena A. Paramasivam, Arumugam Thangaraj, Kumarasamy Spinazzola, Antonella Holt, Ian J. Houlden, Henry Hanna, Michael G. Pitceathly, Robert D.S. Neurol Genet Article OBJECTIVE: Pathologic ribonuclease H1 (RNase H1) causes aberrant mitochondrial DNA (mtDNA) segregation and is associated with multiple mtDNA deletions. We aimed to determine the prevalence of RNase H1 gene (RNASEH1) mutations among patients with mitochondrial disease and establish clinically meaningful genotype-phenotype correlations. METHODS: RNASEH1 was analyzed in patients with (1) multiple deletions/depletion of muscle mtDNA and (2) mendelian progressive external ophthalmoplegia (PEO) with neuropathologic evidence of mitochondrial dysfunction, but no detectable multiple deletions/depletion of muscle mtDNA. Clinicopathologic and molecular evaluation of the newly identified and previously reported patients harboring RNASEH1 mutations was subsequently undertaken. RESULTS: Pathogenic c.424G>A p.Val142Ile RNASEH1 mutations were detected in 3 pedigrees among the 74 probands screened. Given that all 3 families had Indian ancestry, RNASEH1 genetic analysis was undertaken in 50 additional Indian probands with variable clinical presentations associated with multiple mtDNA deletions, but no further RNASEH1 mutations were confirmed. RNASEH1-related mitochondrial disease was characterized by PEO (100%), cerebellar ataxia (57%), and dysphagia (50%). The ataxia neuropathy spectrum phenotype was observed in 1 patient. Although the c.424G>A p.Val142Ile mutation underpins all reported RNASEH1-related mitochondrial disease, haplotype analysis suggested an independent origin, rather than a founder event, for the variant in our families. CONCLUSIONS: In our cohort, RNASEH1 mutations represent the fourth most common cause of adult mendelian PEO associated with multiple mtDNA deletions, following mutations in POLG, RRM2B, and TWNK. RNASEH1 genetic analysis should also be considered in all patients with POLG-negative ataxia neuropathy spectrum. The pathophysiologic mechanisms by which the c.424G>A p.Val142Ile mutation impairs human RNase H1 warrant further investigation. Wolters Kluwer 2017-05-02 /pmc/articles/PMC5413961/ /pubmed/28508084 http://dx.doi.org/10.1212/NXG.0000000000000149 Text en Copyright © 2017 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology. This is an open access article distributed under the terms of the Creative Commons Attribution License 4.0 (CC BY) (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Article
Bugiardini, Enrico
Poole, Olivia V.
Manole, Andreea
Pittman, Alan M.
Horga, Alejandro
Hargreaves, Iain
Woodward, Cathy E.
Sweeney, Mary G.
Holton, Janice L.
Taanman, Jan-Willem
Plant, Gordon T.
Poulton, Joanna
Zeviani, Massimo
Ghezzi, Daniele
Taylor, John
Smith, Conrad
Fratter, Carl
Kanikannan, Meena A.
Paramasivam, Arumugam
Thangaraj, Kumarasamy
Spinazzola, Antonella
Holt, Ian J.
Houlden, Henry
Hanna, Michael G.
Pitceathly, Robert D.S.
Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title_full Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title_fullStr Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title_full_unstemmed Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title_short Clinicopathologic and molecular spectrum of RNASEH1-related mitochondrial disease
title_sort clinicopathologic and molecular spectrum of rnaseh1-related mitochondrial disease
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5413961/
https://www.ncbi.nlm.nih.gov/pubmed/28508084
http://dx.doi.org/10.1212/NXG.0000000000000149
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