Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.

Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.

Defects of atrial and ventricular septation are the most frequent form of congenital heart disease, accounting for almost 50% of all cases. We previously reported that a heterozygous G296S missense mutation of GATA4 caused atrial and ventricular septal defects and pulmonary valve stenosis in humans....

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Main Authors: Chaitali Misra, Nita Sachan, Caryn Rothrock McNally, Sara N Koenig, Haley A Nichols, Anuradha Guggilam, Pamela A Lucchesi, William T Pu, Deepak Srivastava, Vidu Garg
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC3349729?pdf=render
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spelling doaj-8e619ecf80d14f26a44be5766806ce462020-11-25T02:29:18ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042012-01-0185e100269010.1371/journal.pgen.1002690Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.Chaitali MisraNita SachanCaryn Rothrock McNallySara N KoenigHaley A NicholsAnuradha GuggilamPamela A LucchesiWilliam T PuDeepak SrivastavaVidu GargDefects of atrial and ventricular septation are the most frequent form of congenital heart disease, accounting for almost 50% of all cases. We previously reported that a heterozygous G296S missense mutation of GATA4 caused atrial and ventricular septal defects and pulmonary valve stenosis in humans. GATA4 encodes a cardiac transcription factor, and when deleted in mice it results in cardiac bifida and lethality by embryonic day (E)9.5. In vitro, the mutant GATA4 protein has a reduced DNA binding affinity and transcriptional activity and abolishes a physical interaction with TBX5, a transcription factor critical for normal heart formation. To characterize the mutation in vivo, we generated mice harboring the same mutation, Gata4 G295S. Mice homozygous for the Gata4 G295S mutant allele have normal ventral body patterning and heart looping, but have a thin ventricular myocardium, single ventricular chamber, and lethality by E11.5. While heterozygous Gata4 G295S mutant mice are viable, a subset of these mice have semilunar valve stenosis and small defects of the atrial septum. Gene expression studies of homozygous mutant mice suggest the G295S protein can sufficiently activate downstream targets of Gata4 in the endoderm but not in the developing heart. Cardiomyocyte proliferation deficits and decreased cardiac expression of CCND2, a member of the cyclin family and a direct target of Gata4, were found in embryos both homozygous and heterozygous for the Gata4 G295S allele. To further define functions of the Gata4 G295S mutation in vivo, compound mutant mice were generated in which specific cell lineages harbored both the Gata4 G295S mutant and Gata4 null alleles. Examination of these mice demonstrated that the Gata4 G295S protein has functional deficits in early myocardial development. In summary, the Gata4 G295S mutation functions as a hypomorph in vivo and leads to defects in cardiomyocyte proliferation during embryogenesis, which may contribute to the development of congenital heart defects in humans.http://europepmc.org/articles/PMC3349729?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Chaitali Misra
Nita Sachan
Caryn Rothrock McNally
Sara N Koenig
Haley A Nichols
Anuradha Guggilam
Pamela A Lucchesi
William T Pu
Deepak Srivastava
Vidu Garg
spellingShingle Chaitali Misra
Nita Sachan
Caryn Rothrock McNally
Sara N Koenig
Haley A Nichols
Anuradha Guggilam
Pamela A Lucchesi
William T Pu
Deepak Srivastava
Vidu Garg
Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
PLoS Genetics
author_facet Chaitali Misra
Nita Sachan
Caryn Rothrock McNally
Sara N Koenig
Haley A Nichols
Anuradha Guggilam
Pamela A Lucchesi
William T Pu
Deepak Srivastava
Vidu Garg
author_sort Chaitali Misra
title Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
title_short Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
title_full Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
title_fullStr Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
title_full_unstemmed Congenital heart disease-causing Gata4 mutation displays functional deficits in vivo.
title_sort congenital heart disease-causing gata4 mutation displays functional deficits in vivo.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2012-01-01
description Defects of atrial and ventricular septation are the most frequent form of congenital heart disease, accounting for almost 50% of all cases. We previously reported that a heterozygous G296S missense mutation of GATA4 caused atrial and ventricular septal defects and pulmonary valve stenosis in humans. GATA4 encodes a cardiac transcription factor, and when deleted in mice it results in cardiac bifida and lethality by embryonic day (E)9.5. In vitro, the mutant GATA4 protein has a reduced DNA binding affinity and transcriptional activity and abolishes a physical interaction with TBX5, a transcription factor critical for normal heart formation. To characterize the mutation in vivo, we generated mice harboring the same mutation, Gata4 G295S. Mice homozygous for the Gata4 G295S mutant allele have normal ventral body patterning and heart looping, but have a thin ventricular myocardium, single ventricular chamber, and lethality by E11.5. While heterozygous Gata4 G295S mutant mice are viable, a subset of these mice have semilunar valve stenosis and small defects of the atrial septum. Gene expression studies of homozygous mutant mice suggest the G295S protein can sufficiently activate downstream targets of Gata4 in the endoderm but not in the developing heart. Cardiomyocyte proliferation deficits and decreased cardiac expression of CCND2, a member of the cyclin family and a direct target of Gata4, were found in embryos both homozygous and heterozygous for the Gata4 G295S allele. To further define functions of the Gata4 G295S mutation in vivo, compound mutant mice were generated in which specific cell lineages harbored both the Gata4 G295S mutant and Gata4 null alleles. Examination of these mice demonstrated that the Gata4 G295S protein has functional deficits in early myocardial development. In summary, the Gata4 G295S mutation functions as a hypomorph in vivo and leads to defects in cardiomyocyte proliferation during embryogenesis, which may contribute to the development of congenital heart defects in humans.
url http://europepmc.org/articles/PMC3349729?pdf=render
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