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Citations to this article

Tbx20 regulates a genetic program essential to adult mouse cardiomyocyte function
Tao Shen, … , Marcelo A. Nobrega, Sylvia M. Evans
Tao Shen, … , Marcelo A. Nobrega, Sylvia M. Evans
Published November 14, 2011
Citation Information: J Clin Invest. 2011;121(12):4640-4654. https://doi.org/10.1172/JCI59472.
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Research Article Cardiology Article has an altmetric score of 4

Tbx20 regulates a genetic program essential to adult mouse cardiomyocyte function

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Abstract

Human mutations in or variants of TBX20 are associated with congenital heart disease, cardiomyopathy, and arrhythmias. To investigate whether cardiac disease in patients with these conditions results from an embryonic or ongoing requirement for Tbx20 in myocardium, we ablated Tbx20 specifically in adult cardiomyocytes in mice. This ablation resulted in the onset of severe cardiomyopathy accompanied by arrhythmias, with death ensuing within 1 to 2 weeks of Tbx20 ablation. Accounting for this dramatic phenotype, we identified molecular signatures that posit Tbx20 as a central integrator of a genetic program that maintains cardiomyocyte function in the adult heart. Expression of a number of genes encoding critical transcription factors, ion channels, and cytoskeletal/myofibrillar proteins was downregulated consequent to loss of Tbx20. Genome-wide ChIP analysis of Tbx20-binding regions in the adult heart revealed that many of these genes were direct downstream targets of Tbx20 and uncovered a previously undescribed DNA-binding site for Tbx20. Bioinformatics and in vivo functional analyses revealed a cohort of transcription factors that, working with Tbx20, integrated multiple environmental signals to maintain ion channel gene expression in the adult heart. Our data provide insight into the mechanisms by which mutations in TBX20 cause adult heart disease in humans.

Authors

Tao Shen, Ivy Aneas, Noboru Sakabe, Ralf J. Dirschinger, Gang Wang, Scott Smemo, John M. Westlund, Hongqiang Cheng, Nancy Dalton, Yusu Gu, Cornelis J. Boogerd, Chen-leng Cai, Kirk Peterson, Ju Chen, Marcelo A. Nobrega, Sylvia M. Evans

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 2014 2013 2012 2011 Total
Citations: 2 2 5 9 10 4 2 5 9 12 5 11 5 7 1 89
Citation information
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Citations to this article in year 2015 (5)

Title and authors Publication Year
NKX2-5 mutations causative for congenital heart disease retain functionality and are directed to hundreds of targets: ( A ) Structure of the human NKX2-5 protein (TN, tinman domain; NK2SD, NK-2 specific domain; YRD, tyrosine-rich domain). Bars and arrows indicate missense and termination mutations associated with congenital heart disease (CHD), respectively. ( B ) Top over-represented motifs discovered de novo in NKX2-5 peaks using Trawler or Weeder . NKX2-5, GATA, and Nuclear Factor 1 (NF1) binding motifs deposited in TRANSFAC are shown. ( C ) Distribution of NKX2-5, GATA, and NF1 binding sequences in NKX2-5 peaks. ( D ) Yeast-two-hybrid assay. NKX2-5 and NF1 proteins were fused to Gal4-activation and DNA-binding domains, respectively. Positive signs (+) show interaction as growth on selective medium from three independent experiments. ( E ) Normalized median expression of NKX2-5-target genes in 91 murine cell types (data collected from BioGPS ). Tissues with the highest median expressions are shown in colour, including heart (red). ( F ) Expression of NKX2-5 target genes and random genes in HL-1 cells. Data collected from (Mace et al., 2009)
R Bouveret, AJ Waardenberg, N Schonrock, M Ramialison, T Doan, D Jong, A Bondue, G Kaur, S Mohamed, H Fonoudi, C Chen, MA Wouters, S Bhattacharya, N Plachta, SL Dunwoodie, G Chapman, C Blanpain, RP Harvey
eLife 2015
Sequential Binding of MEIS1 and NKX2-5 on the Popdc2 Gene: A Mechanism for Spatiotemporal Regulation of Enhancers during Cardiogenesis
L Dupays, C Shang, R Wilson, S Kotecha, S Wood, N Towers, T Mohun
Cell Reports 2015
Novel Mutations in the Transcriptional Activator Domain of the Human TBX20 in Patients with Atrial Septal Defect
IE Monroy-Muñoz, N Pérez-Hernández, JM Rodríguez-Pérez, JE Muñoz-Medina, J Angeles-Martínez, JJ García-Trejo, E Morales-Ríos, F Massó, JP Sandoval-Jones, J Cervantes-Salazar, JA García-Montes, J Calderón-Colmenero, G Vargas-Alarcón
BioMed Research International 2015
VISIONET: intuitive visualisation of overlapping transcription factor networks, with applications in cardiogenic gene discovery
HT Nim, MB Furtado, MW Costa, NA Rosenthal, H Kitano, SE Boyd
BMC bioinformatics 2015
Salvianolic Acid B Down-regulates Matrix Metalloproteinase-9 Activity and Expression in Tumor Necrosis Factor-α-induced Human Coronary Artery Endothelial Cells
ZD Du, L Ma, YQ Guan
Chinese Medical Journal 2015

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