In silico analysis of GATA4 variants demonstrates main contribution to congenital heart disease

Abbasi, Shiva and Mohsen-Pour, Neda and Naderi, Niloofar and Rahimi, Shahin and Maleki, Majid and Kalayinia, Samira (2021) In silico analysis of GATA4 variants demonstrates main contribution to congenital heart disease. Journal of Cardiovascular and Thoracic Research, 13 (4). pp. 336-354. ISSN 2008-5117

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Abstract

Introduction: Congenital heart disease (CHD) is the most common congenital abnormality and the main cause of infant mortality worldwide. Some of the mutations that occur in the GATA4 gene region may result in different types of CHD. Here, we report our in silico analysis of gene variants to determine the effects of the GATA4 gene on the development of CHD.
Methods: Online 1000 Genomes Project, ExAC, gnomAD, GO-ESP, TOPMed, Iranome, GME, ClinVar, and HGMD databases were drawn upon to collect information on all the reported GATA4 variations.The functional importance of the genetic variants was assessed by using SIFT, MutationTaster, CADD,PolyPhen-2, PROVEAN, and GERP prediction tools. Thereafter, network analysis of the GATA4protein via STRING, normal/mutant protein structure prediction via HOPE and I-TASSER, and phylogenetic assessment of the GATA4 sequence alignment via ClustalW were performed.
Results: The most frequent variant was c.874T>C (45.58%), which was reported in Germany.Ventricular septal defect was the most frequent type of CHD. Out of all the reported variants of GATA4,38 variants were pathogenic. A high level of pathogenicity was shown for p.Gly221Arg (CADD score=31), which was further analyzed.
Conclusion: The GATA4 gene plays a significant role in CHD; we, therefore, suggest that it be accorded priority in CHD genetic screening.

Item Type: Article
Subjects: East India library > Medical Science
Depositing User: Unnamed user with email support@eastindialibrary.com
Date Deposited: 05 May 2023 11:05
Last Modified: 15 Oct 2024 10:36
URI: http://info.paperdigitallibrary.com/id/eprint/1011

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