Holt–Oram syndrome with intermediate atrioventricular canal defect, and aortic coarctation: Functional characterization of a de novo <i>TBX5</i> mutation

Baban, Anwar; Pitto, Letizia; Pulignani, Silvia; Cresci, Monica; Mariani, Laura; Gambacciani, Carolina; Digilio, María Cristina; Pongiglione, Giacomo; Albanese, Sonia B.

doi:10.1002/ajmg.a.36459

Cited by 24 publications

(15 citation statements)

References 35 publications

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“…At E13.5, Mta1 +/− mice have no apparent cardiac defects (Figure 2C). Tbx5 +/− mice exhibit partially penetrant cardiac defects as previously described, including ASD, VSD, and complete common atrioventricular canal (CCAVC), which includes both ASD and VSD components (Figure 2D) (Baban et al, 2014; Basson et al, 1994; Basson et al, 1999; Benson et al, 1996; Bruneau et al, 1999; Bruneau et al, 2001; McDermott et al, 2005). Tbx5 +/− ; Mta1 +/− heterozygous null embryos all demonstrated septal defects (19/19), a higher frequency of septal defects than either single heterozygote alone (0/14 for Mta1 +/− and 12/16 for Tbx5 +/− ) (p = 7.1E-9 vs. WT and p = 0.035 vs Tbx5 +/− ) (Figure 2E–J).…”

Section: Resultsmentioning

confidence: 70%

“…This hypothesis is further supported by our observations that Tbx5 +/− ; Mta1 +/− compound heterozygous mice have a higher frequency of cardiac septal defects than either single heterozygote alone (Figure 2J). AVSDs have been reported in 18 HOS patients, and 10 have been characterized to date (Baban et al, 2014). Of these, 6 of the mutations lead to the introduction of a stop codon before the TBX5 NID , and one mis-sense mutation maps within the TBX5 NID and ablates the TBX5-NuRD interaction (Figure 5K).…”

Section: Discussionmentioning

confidence: 99%

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The Cardiac TBX5 Interactome Reveals a Chromatin Remodeling Network Essential for Cardiac Septation

et al. 2016

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SUMMARY Human mutations in the cardiac transcription factor gene TBX5 cause Congenital Heart Disease (CHD), however the underlying mechanism is unknown. We report characterization of the endogenous TBX5 cardiac interactome and demonstrate that TBX5, long considered a transcriptional activator, interacts biochemically and genetically with the Nucleosome Remodeling and Deacetylase (NuRD) repressor complex. Incompatible gene programs are repressed by TBX5 in the developing heart. CHD missense mutations that disrupt the TBX5-NuRD interaction cause depression of a subset of repressed genes. Furthermore, the TBX5-NuRD interaction is required for heart development. Phylogenetic analysis showed that the TBX5-NuRD interaction domain evolved during early diversification of vertebrates, simultaneous with the evolution of cardiac septation. Collectively, this work defines a TBX5-NuRD interaction essential to cardiac development and the evolution of the mammalian heart, and when altered may contribute to human CHD.

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Section: Resultsmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 99%

The Cardiac TBX5 Interactome Reveals a Chromatin Remodeling Network Essential for Cardiac Septation

et al. 2016

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“…The spectrum of cardiac malformations in Noonan syndrome is represented classically by pulmonary stenosis, with or without dysplastic pulmonary valve and hypertrophic cardiomyopathy; CAVSD coming on the second place as frequency, being reported in 13.8% of cases [50]. Holt Oram syndrome is characterized by the concomitant presence of heart and limb anomalies, the cardiac malformation could be either ASD, VSD or CAV [51,52]. VACTERL association has also been reported in the presence of a CAVSD [31].…”

Section: Practical Tricks For 3/4d Techniquesmentioning

confidence: 99%

Complete atrioventricular septal defect in the era of prenatal diagnosis

et al. 2016

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Complete atrioventricular septal defect (CAVSD) is a fetal cardiac malformation (5% of all cardiac malformations) that can be detected prenatally with a reserved prognosis. The diagnosis can be suspected early at the end of the first trimester using the transabdominal or transvaginal ultrasound approach. Generally, the diagnostic can be established during the mid-trimester scan at 19-24 weeks of gestation. The percentage of antenatal diagnostic of CAVSD is between 57-92%. This review aims to analyze the anatomical principles and the ultrasound techniques that can improve the prenatal diagnosis of CAVSD. We have also analyzed the structural and genetic anomalies frequently associated with CAVSD.

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“…Holt-Oram syndrome is characterized by radial ray upper limb abnormalities and cardiac septation defects with an autosomal dominant transmission pattern. The septal defects consist of secundum ASD, muscular ventricular septal defects or atrioventricular septal defects and may also be associated with aortic coarctation [57]. Affected patients also present various degrees of conduction disorders, such as sinus bradycardia and atrio-ventricular block, even in the absence of overt structural heart disease [58].…”

Section: Tbx5mentioning

confidence: 99%