MT-CYB mutations in hypertrophic cardiomyopathy

Christian M Hagen; Frederik H Aidt; Ole Havndrup; Paula L Hedley; Cathrine Jespersgaard; Morten Jensen; Jørgen K. Kanters; Johanna C Moolman-Smook; Daniel V Møller; Henning Bundgaard; Michael Christiansen

doi:10.1002/mgg3.5

MT-CYB mutations in hypertrophic cardiomyopathy

Christian M Hagen, Frederik H Aidt, Ole Havndrup, Paula L Hedley, Cathrine Jespersgaard, Morten Jensen, Jørgen K. Kanters, Johanna C Moolman-Smook, Daniel V Møller, Henning Bundgaard, Michael Christiansen

Physiology of circulation, kidney and lung

15 Citationer (Scopus)

Abstract

Mitochondrial dysfunction is a characteristic of heart failure. Mutations in mitochondrial DNA, particularly in MT-CYB coding for cytochrome B in complex III (CIII), have been associated with isolated hypertrophic cardiomyopathy (HCM). We hypothesized that MT-CYB mutations might play an important causal or modifying role in HCM. The MT-CYB gene was sequenced from DNA isolated from blood from 91 Danish HCM probands. Nonsynonymous variants were analyzed by bioinformatics, molecular modeling and simulation. Two germline-inherited, putative disease-causing, nonsynonymous variants: m.15024G>A; p.C93Y and m.15482T>C; p.S246P were identified. Modeling showed that the p.C93Y mutation leads to disruption of the tertiary structure of Cytb by helix displacement, interfering with protein-heme interaction. The p.S246P mutation induces a diproline structure, which alters local secondary structure and induces a kink in the protein backbone, interfering with macromolecular interactions. These molecular effects are compatible with a leaky phenotype, that is, limited but progressive mitochondrial dysfunction. In conclusion, we find that rare, putative leaky mtDNA variants in MT-CYB can be identified in a cohort of HCM patients. We propose that further patients with HCM should be examined for mutations in MT-CYB in order to clarify the role of these variants.

Originalsprog	Engelsk
Tidsskrift	Molecular genetics & genomic medicine
Vol/bind	1
Udgave nummer	1
Sider (fra-til)	54-65
Antal sider	12
ISSN	2324-9269
DOI	https://doi.org/10.1002/mgg3.5
Status	Udgivet - maj 2013

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10.1002/mgg3.5

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title = "MT-CYB mutations in hypertrophic cardiomyopathy",

abstract = "Mitochondrial dysfunction is a characteristic of heart failure. Mutations in mitochondrial DNA, particularly in MT-CYB coding for cytochrome B in complex III (CIII), have been associated with isolated hypertrophic cardiomyopathy (HCM). We hypothesized that MT-CYB mutations might play an important causal or modifying role in HCM. The MT-CYB gene was sequenced from DNA isolated from blood from 91 Danish HCM probands. Nonsynonymous variants were analyzed by bioinformatics, molecular modeling and simulation. Two germline-inherited, putative disease-causing, nonsynonymous variants: m.15024G>A; p.C93Y and m.15482T>C; p.S246P were identified. Modeling showed that the p.C93Y mutation leads to disruption of the tertiary structure of Cytb by helix displacement, interfering with protein-heme interaction. The p.S246P mutation induces a diproline structure, which alters local secondary structure and induces a kink in the protein backbone, interfering with macromolecular interactions. These molecular effects are compatible with a leaky phenotype, that is, limited but progressive mitochondrial dysfunction. In conclusion, we find that rare, putative leaky mtDNA variants in MT-CYB can be identified in a cohort of HCM patients. We propose that further patients with HCM should be examined for mutations in MT-CYB in order to clarify the role of these variants.",

author = "Hagen, {Christian M} and Aidt, {Frederik H} and Ole Havndrup and Hedley, {Paula L} and Cathrine Jespersgaard and Morten Jensen and Kanters, {J{\o}rgen K.} and Moolman-Smook, {Johanna C} and M{\o}ller, {Daniel V} and Henning Bundgaard and Michael Christiansen",

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T1 - MT-CYB mutations in hypertrophic cardiomyopathy

AU - Hagen, Christian M

AU - Aidt, Frederik H

AU - Havndrup, Ole

AU - Hedley, Paula L

AU - Jespersgaard, Cathrine

AU - Jensen, Morten

AU - Kanters, Jørgen K.

AU - Moolman-Smook, Johanna C

AU - Møller, Daniel V

AU - Bundgaard, Henning

AU - Christiansen, Michael

PY - 2013/5

Y1 - 2013/5

N2 - Mitochondrial dysfunction is a characteristic of heart failure. Mutations in mitochondrial DNA, particularly in MT-CYB coding for cytochrome B in complex III (CIII), have been associated with isolated hypertrophic cardiomyopathy (HCM). We hypothesized that MT-CYB mutations might play an important causal or modifying role in HCM. The MT-CYB gene was sequenced from DNA isolated from blood from 91 Danish HCM probands. Nonsynonymous variants were analyzed by bioinformatics, molecular modeling and simulation. Two germline-inherited, putative disease-causing, nonsynonymous variants: m.15024G>A; p.C93Y and m.15482T>C; p.S246P were identified. Modeling showed that the p.C93Y mutation leads to disruption of the tertiary structure of Cytb by helix displacement, interfering with protein-heme interaction. The p.S246P mutation induces a diproline structure, which alters local secondary structure and induces a kink in the protein backbone, interfering with macromolecular interactions. These molecular effects are compatible with a leaky phenotype, that is, limited but progressive mitochondrial dysfunction. In conclusion, we find that rare, putative leaky mtDNA variants in MT-CYB can be identified in a cohort of HCM patients. We propose that further patients with HCM should be examined for mutations in MT-CYB in order to clarify the role of these variants.

AB - Mitochondrial dysfunction is a characteristic of heart failure. Mutations in mitochondrial DNA, particularly in MT-CYB coding for cytochrome B in complex III (CIII), have been associated with isolated hypertrophic cardiomyopathy (HCM). We hypothesized that MT-CYB mutations might play an important causal or modifying role in HCM. The MT-CYB gene was sequenced from DNA isolated from blood from 91 Danish HCM probands. Nonsynonymous variants were analyzed by bioinformatics, molecular modeling and simulation. Two germline-inherited, putative disease-causing, nonsynonymous variants: m.15024G>A; p.C93Y and m.15482T>C; p.S246P were identified. Modeling showed that the p.C93Y mutation leads to disruption of the tertiary structure of Cytb by helix displacement, interfering with protein-heme interaction. The p.S246P mutation induces a diproline structure, which alters local secondary structure and induces a kink in the protein backbone, interfering with macromolecular interactions. These molecular effects are compatible with a leaky phenotype, that is, limited but progressive mitochondrial dysfunction. In conclusion, we find that rare, putative leaky mtDNA variants in MT-CYB can be identified in a cohort of HCM patients. We propose that further patients with HCM should be examined for mutations in MT-CYB in order to clarify the role of these variants.

U2 - 10.1002/mgg3.5

DO - 10.1002/mgg3.5

M3 - Journal article

C2 - 24498601

SN - 2324-9269

VL - 1

SP - 54

EP - 65

JO - Molecular Genetics & Genomic Medicine

JF - Molecular Genetics & Genomic Medicine

IS - 1

ER -

MT-CYB mutations in hypertrophic cardiomyopathy

Abstract

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