A gain-of-function TBX20 mutation causes congenital atrial septal defects, patent foramen ovale and cardiac valve defects

Posch, Maximilian; Gramlich, Michael; Sunde, Margaret; Schmitt, Katharina; Lee, Stella H Y; Richter, Silke; Kersten, A.H.; Perrot, Andreas; Panek, A.; Khatib, Iman Al; Nemer, Georges; Mégarbané, André; Dietz, Rainer; Stiller, Brigitte; Berger, Felix; Harvey, Richard P.; Özcelik, C.

doi:10.1136/jmg.2009.069997

Cited by 112 publications

(87 citation statements)

References 27 publications

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“…Previous studies have demonstrated that identified ASD-related TBX20 mutations are all in the T-box DNA binding domain (109-288 AA) except p.A63T ( Fig. 3; Table 3) (Kirk et al, 2007;Liu et al, 2008;Qian et al, 2009;Posch et al, 2010a). Therefore, although in vitro assays were not performed in our study, we still believed that the mutation (p.D176N) in this study plays a critical role in CHDs.…”

Section: Discussionmentioning

confidence: 55%

“…TBX20 associated directly with other cardiac transcription factors, namely, the homeodomain factor NKX2-5 and zinc finger factor GATA4 and GATA5 (Stennard et al, 2003). Modification of amino acid from aspartic acid to asparagine may not prevent binding to its target DNA site, but there are other possibilities, such as an influenced rate of scanning of DNA or co-factors for interaction, or abnormal structure stability when bound to co-factors (Posch et al, 2010a). Previous studies have demonstrated that identified ASD-related TBX20 mutations are all in the T-box DNA binding domain (109-288 AA) except p.A63T ( Fig.…”

Section: Discussionmentioning

confidence: 99%

“…Qian et al (2009) reported that two different variants of TBX20 were found in four children with ASD with or without other CHD. Posch et al (2010a) identified a TBX20 missense variant in a patient with ASD with additional TOF and cardiac valve defect (Table 3).…”

Section: Discussionmentioning

confidence: 99%

“…In the developing mouse embryos, tbx20 is expressed in cardiac progenitor cells, as well as in the developing myocardium and endothelial cells associated with endocardial cushions, the precursor structures for the cardiac valves and the atrioventricular septum, which implies that tbx20 is essential for proper heart development. Loss function of tbx20 in the mouse has been found in connection with various forms of congenital heart defects, including defects in septation, valvulogenesis, cardiomyopathy, and arrhythmia (Stennard et al, 2003;Stennard et al, 2005;Kirk et al, 2007;Liu et al, 2008;Posch et al, 2010a;Sotoodehnia et al, 2010;Shen et al, 2011;Zhang et al, 2011;Qiao et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

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A novel variant in TBX20 (p.D176N) identified by whole-exome sequencing in combination with a congenital heart disease related gene filter is associated with familial atrial septal defect

Liu

Fan

Chen

et al. 2014

J. Zhejiang Univ. Sci. B

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Liu et al. / J Zhejiang Univ-Sci B (Biomed & Biotechnol) 2014 15(9):830-837 830 A novel variant in TBX20 (p.D176N) identified by whole-exome sequencing in combination with a congenital heart disease related gene filter is associated with familial atrial septal defect Abstract: Congenital heart disease (CHD) is the leading cause of birth defects, and its etiology is not completely understood. Atrial septal defect (ASD) is one of the most common defects of CHD. Previous studies have demonstrated that mutations in the transcription factor T-box 20 (TBX20) contribute to congenital ASD. Whole-exome sequencing in combination with a CHD-related gene filter was used to detect a family of three generations with ASD. A novel TBX20 mutation, c.526G>A (p.D176N), was identified and co-segregated in all affected members in this family. This mutation was predicted to be deleterious by bioinformatics programs (SIFT, Polyphen2, and MutationTaster). This mutation was also not presented in the current Single Nucleotide Polymorphism Database (dbSNP) or National Heart, Lung, and Blood Institute (NHLBI) Exome Sequencing Project (ESP). In conclusion, our finding expands the spectrum of TBX20 mutations and provides additional support that TBX20 plays important roles in cardiac development. Our study also provided a new and cost-effective analysis strategy for the genetic study in small CHD pedigree.

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Section: Discussionmentioning

confidence: 55%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A novel variant in TBX20 (p.D176N) identified by whole-exome sequencing in combination with a congenital heart disease related gene filter is associated with familial atrial septal defect

Liu

Fan

Chen

et al. 2014

J. Zhejiang Univ. Sci. B

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“…Various mutations in transcription factors and sarcomeric genes were described in different studies [3]. We have analyzed different genes involved in the pathogenesis of CHDs and could identify mutations in ASD patients [4,5,6].…”

Section: Introductionmentioning

confidence: 99%

CCN1 Mutation is Associated with Atrial Septal Defect

et al. 2014

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The genetic basis of congenital heart disease remains unknown in most of the cases. Recently, a novel mouse model shed new light on the role of CCN1/CYR61, a matricellular regulatory factor, in cardiac morphogenesis. In a candidate gene approach, we analyzed a cohort of 143 patients with atrial septal defects (ASD) by sequencing the coding exons of CCN1. In addition to three frequent polymorphisms, we identified an extremely rare novel heterozygous missense mutation (c.139C>T; p.R47W) in one patient with severe ASD. The mutation leads to an exchange of residues with quite different properties in a highly conserved position of the Nterminal insulin-like growth factor binding protein (IGFBP) module. Further bioinformatic analysis, exclusion of known ASD disease genes as well as the exclusion of the mutation in a very high number of ethnically matched controls (more than 1000 individuals) and in public genetic databases indicates that the p.R47W variant is a probable disease-associated mutation. The report about ASD in mice in heterozygous Ccn1 +/-animals strongly supports this notion. Our study is the first to suggest a relationship between a probable CCN1 mutation and ASD. Our purpose here was to draw attention to CCN1, a gene that we believe may be important for genetic analysis in patients with congenital heart disease.

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Novel Association of the NOTCH Pathway Regulator MIB1 Gene With the Development of Bicuspid Aortic Valve

Tessler,

Albuisson,

Piñeiro-Sabarís

et al. 2023

JAMA Cardiol

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ImportanceNonsyndromic bicuspid aortic valve (nsBAV) is the most common congenital heart valve malformation. BAV has a heritable component, yet only a few causative genes have been identified; understanding BAV genetics is a key point in developing personalized medicine.ObjectiveTo identify a new gene for nsBAV.Design, Setting, and ParticipantsThis was a comprehensive, multicenter, genetic association study based on candidate gene prioritization in a familial cohort followed by rare and common association studies in replication cohorts. Further validation was done using in vivo mice models. Study data were analyzed from October 2019 to October 2023. Three cohorts of patients with BAV were included in the study: (1) the discovery cohort was a large cohort of inherited cases from 29 pedigrees of French and Israeli origin; (2) the replication cohort 1 for rare variants included unrelated sporadic cases from various European ancestries; and (3) replication cohort 2 was a second validation cohort for common variants in unrelated sporadic cases from Europe and the US.Main Outcomes and MeasuresTo identify a candidate gene for nsBAV through analysis of familial cases exome sequencing and gene prioritization tools. Replication cohort 1 was searched for rare and predicted deleterious variants and genetic association. Replication cohort 2 was used to investigate the association of common variants with BAV.ResultsA total of 938 patients with BAV were included in this study: 69 (7.4%) in the discovery cohort, 417 (44.5%) in replication cohort 1, and 452 (48.2%) in replication cohort 2. A novel human nsBAV gene, MINDBOMB1 homologue MIB1, was identified. MINDBOMB1 homologue (MIB1) is an E3-ubiquitin ligase essential for NOTCH-signal activation during heart development. In approximately 2% of nsBAV index cases from the discovery and replication 1 cohorts, rare MIB1 variants were detected, predicted to be damaging, and were significantly enriched compared with population-based controls (2% cases vs 0.9% controls; P = .03). In replication cohort 2, MIB1 risk haplotypes significantly associated with nsBAV were identified (permutation test, 1000 repeats; P = .02). Two genetically modified mice models carrying Mib1 variants identified in our cohort showed BAV on a NOTCH1-sensitized genetic background.Conclusions and RelevanceThis genetic association study identified the MIB1 gene as associated with nsBAV. This underscores the crucial role of the NOTCH pathway in the pathophysiology of BAV and its potential as a target for future diagnostic and therapeutic intervention.

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A gain-of-function TBX20 mutation causes congenital atrial septal defects, patent foramen ovale and cardiac valve defects

Cited by 112 publications

References 27 publications

A novel variant in TBX20 (p.D176N) identified by whole-exome sequencing in combination with a congenital heart disease related gene filter is associated with familial atrial septal defect

A novel variant in TBX20 (p.D176N) identified by whole-exome sequencing in combination with a congenital heart disease related gene filter is associated with familial atrial septal defect

CCN1 Mutation is Associated with Atrial Septal Defect

Novel Association of the NOTCH Pathway Regulator MIB1 Gene With the Development of Bicuspid Aortic Valve

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