Cardiac metabolic pathways affected in the mouse model of barth syndrome.

Cardiac metabolic pathways affected in the mouse model of barth syndrome.

Cardiolipin (CL) is a mitochondrial phospholipid essential for electron transport chain (ETC) integrity. CL-deficiency in humans is caused by mutations in the tafazzin (Taz) gene and results in a multisystem pediatric disorder, Barth syndrome (BTHS). It has been reported that tafazzin deficiency des...

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Main Authors: Yan Huang, Corey Powers, Satish K Madala, Kenneth D Greis, Wendy D Haffey, Jeffrey A Towbin, Enkhsaikhan Purevjav, Sabzali Javadov, Arnold W Strauss, Zaza Khuchua
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4451073?pdf=render
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spelling doaj-dd94a5c23f734988bfe595aef3d980942020-11-25T01:07:19ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01106e012856110.1371/journal.pone.0128561Cardiac metabolic pathways affected in the mouse model of barth syndrome.Yan HuangCorey PowersSatish K MadalaKenneth D GreisWendy D HaffeyJeffrey A TowbinEnkhsaikhan PurevjavSabzali JavadovArnold W StraussZaza KhuchuaCardiolipin (CL) is a mitochondrial phospholipid essential for electron transport chain (ETC) integrity. CL-deficiency in humans is caused by mutations in the tafazzin (Taz) gene and results in a multisystem pediatric disorder, Barth syndrome (BTHS). It has been reported that tafazzin deficiency destabilizes mitochondrial respiratory chain complexes and affects supercomplex assembly. The aim of this study was to investigate the impact of Taz-knockdown on the mitochondrial proteomic landscape and metabolic processes, such as stability of respiratory chain supercomplexes and their interactions with fatty acid oxidation enzymes in cardiac muscle. Proteomic analysis demonstrated reduction of several polypeptides of the mitochondrial respiratory chain, including Rieske and cytochrome c1 subunits of complex III, NADH dehydrogenase alpha subunit 5 of complex I and the catalytic core-forming subunit of F0F1-ATP synthase. Taz gene knockdown resulted in upregulation of enzymes of folate and amino acid metabolic pathways in heart mitochondria, demonstrating that Taz-deficiency causes substantive metabolic remodeling in cardiac muscle. Mitochondrial respiratory chain supercomplexes are destabilized in CL-depleted mitochondria from Taz knockdown hearts resulting in disruption of the interactions between ETC and the fatty acid oxidation enzymes, very long-chain acyl-CoA dehydrogenase and long-chain 3-hydroxyacyl-CoA dehydrogenase, potentially affecting the metabolic channeling of reducing equivalents between these two metabolic pathways. Mitochondria-bound myoglobin was significantly reduced in Taz-knockdown hearts, potentially disrupting intracellular oxygen delivery to the oxidative phosphorylation system. Our results identify the critical pathways affected by the Taz-deficiency in mitochondria and establish a future framework for development of therapeutic options for BTHS.http://europepmc.org/articles/PMC4451073?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yan Huang
Corey Powers
Satish K Madala
Kenneth D Greis
Wendy D Haffey
Jeffrey A Towbin
Enkhsaikhan Purevjav
Sabzali Javadov
Arnold W Strauss
Zaza Khuchua
spellingShingle Yan Huang
Corey Powers
Satish K Madala
Kenneth D Greis
Wendy D Haffey
Jeffrey A Towbin
Enkhsaikhan Purevjav
Sabzali Javadov
Arnold W Strauss
Zaza Khuchua
Cardiac metabolic pathways affected in the mouse model of barth syndrome.
PLoS ONE
author_facet Yan Huang
Corey Powers
Satish K Madala
Kenneth D Greis
Wendy D Haffey
Jeffrey A Towbin
Enkhsaikhan Purevjav
Sabzali Javadov
Arnold W Strauss
Zaza Khuchua
author_sort Yan Huang
title Cardiac metabolic pathways affected in the mouse model of barth syndrome.
title_short Cardiac metabolic pathways affected in the mouse model of barth syndrome.
title_full Cardiac metabolic pathways affected in the mouse model of barth syndrome.
title_fullStr Cardiac metabolic pathways affected in the mouse model of barth syndrome.
title_full_unstemmed Cardiac metabolic pathways affected in the mouse model of barth syndrome.
title_sort cardiac metabolic pathways affected in the mouse model of barth syndrome.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Cardiolipin (CL) is a mitochondrial phospholipid essential for electron transport chain (ETC) integrity. CL-deficiency in humans is caused by mutations in the tafazzin (Taz) gene and results in a multisystem pediatric disorder, Barth syndrome (BTHS). It has been reported that tafazzin deficiency destabilizes mitochondrial respiratory chain complexes and affects supercomplex assembly. The aim of this study was to investigate the impact of Taz-knockdown on the mitochondrial proteomic landscape and metabolic processes, such as stability of respiratory chain supercomplexes and their interactions with fatty acid oxidation enzymes in cardiac muscle. Proteomic analysis demonstrated reduction of several polypeptides of the mitochondrial respiratory chain, including Rieske and cytochrome c1 subunits of complex III, NADH dehydrogenase alpha subunit 5 of complex I and the catalytic core-forming subunit of F0F1-ATP synthase. Taz gene knockdown resulted in upregulation of enzymes of folate and amino acid metabolic pathways in heart mitochondria, demonstrating that Taz-deficiency causes substantive metabolic remodeling in cardiac muscle. Mitochondrial respiratory chain supercomplexes are destabilized in CL-depleted mitochondria from Taz knockdown hearts resulting in disruption of the interactions between ETC and the fatty acid oxidation enzymes, very long-chain acyl-CoA dehydrogenase and long-chain 3-hydroxyacyl-CoA dehydrogenase, potentially affecting the metabolic channeling of reducing equivalents between these two metabolic pathways. Mitochondria-bound myoglobin was significantly reduced in Taz-knockdown hearts, potentially disrupting intracellular oxygen delivery to the oxidative phosphorylation system. Our results identify the critical pathways affected by the Taz-deficiency in mitochondria and establish a future framework for development of therapeutic options for BTHS.
url http://europepmc.org/articles/PMC4451073?pdf=render
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