T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system

Rajiv A. Mohan; Fernanda M. Bosada; Jan H. van Weerd; Karel van Duijvenboden; Jianan Wang; Mathilda T. M. Mommersteeg; Ingeborg B. Hooijkaas; Vincent Wakker; Corrie de Gier-de Vries; Ruben Coronel; Gerard J. J. Boink; Jeroen Bakkers; Phil Barnett; Bas J. Boukens; Vincent M. Christoffels

doi:https://doi.org/10.1073/pnas.1919379117

T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system

Rajiv A. Mohan, Fernanda M. Bosada, Jan H. van Weerd, Karel van Duijvenboden, Jianan Wang, Mathilda T. M. Mommersteeg, Ingeborg B. Hooijkaas, Vincent Wakker, Corrie de Gier-de Vries, Ruben Coronel, Gerard J. J. Boink, Jeroen Bakkers, Phil Barnett, Bas J. Boukens, Vincent M. Christoffels

Research output: Contribution to journal › Article › Academic › peer-review

16 Citations (Scopus)

Abstract

Genome-wide association studies have identified noncoding variants near TBX3 that are associated with PR interval and QRS duration, suggesting that subtle changes in TBX3 expression affect atrioventricular conduction system function. To explore whether and to what extent the atrioventricular conduction system is affected by Tbx3 dose reduction, we first characterized electrophysiological properties and morphology of heterozygous Tbx3 mutant (Tbx3+/-) mouse hearts. We found PR interval shortening and prolonged QRS duration, as well as atrioventricular bundle hypoplasia after birth in heterozygous mice. The atrioventricular node size was unaffected. Transcriptomic analysis of atrioventricular nodes isolated by laser capture microdissection revealed hundreds of deregulated genes in Tbx3+/- mutants. Notably, Tbx3+/- atrioventricular nodes showed increased expression of working myocardial gene programs (mitochondrial and metabolic processes, muscle contractility) and reduced expression of pacemaker gene programs (neuronal, Wnt signaling, calcium/ion channel activity). By integrating chromatin accessibility profiles (ATAC sequencing) of atrioventricular tissue and other epigenetic data, we identified Tbx3-dependent atrioventricular regulatory DNA elements (REs) on a genome-wide scale. We used transgenic reporter assays to determine the functionality of candidate REs near Ryr2, an up-regulated chamber-enriched gene, and in Cacna1g, a down-regulated conduction system-specific gene. Using genome editing to delete candidate REs, we showed that a strong intronic bipartite RE selectively governs Cacna1g expression in the conduction system in vivo. Our data provide insights into the multifactorial Tbx3-dependent transcriptional network that regulates the structure and function of the cardiac conduction system, which may underlie the differences in PR duration and QRS interval between individuals carrying variants in the TBX3 locus.

Original language	English
Pages (from-to)	18617-18626
Number of pages	10
Journal	PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume	117
Issue number	31
DOIs	https://doi.org/10.1073/pnas.1919379117
Publication status	Published - 4 Aug 2020

Keywords

Atrioventricular conduction system
Cacna1g
Electrical patterning
Ryr2
Tbx3

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Mohan, R. A., Bosada, F. M., van Weerd, J. H., van Duijvenboden, K., Wang, J., Mommersteeg, M. T. M., Hooijkaas, I. B., Wakker, V., de Gier-de Vries, C., Coronel, R., Boink, G. J. J., Bakkers, J., Barnett, P., Boukens, B. J., & Christoffels, V. M. (2020). T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 117(31), 18617-18626. https://doi.org/10.1073/pnas.1919379117

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title = "T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system",

abstract = "Genome-wide association studies have identified noncoding variants near TBX3 that are associated with PR interval and QRS duration, suggesting that subtle changes in TBX3 expression affect atrioventricular conduction system function. To explore whether and to what extent the atrioventricular conduction system is affected by Tbx3 dose reduction, we first characterized electrophysiological properties and morphology of heterozygous Tbx3 mutant (Tbx3+/-) mouse hearts. We found PR interval shortening and prolonged QRS duration, as well as atrioventricular bundle hypoplasia after birth in heterozygous mice. The atrioventricular node size was unaffected. Transcriptomic analysis of atrioventricular nodes isolated by laser capture microdissection revealed hundreds of deregulated genes in Tbx3+/- mutants. Notably, Tbx3+/- atrioventricular nodes showed increased expression of working myocardial gene programs (mitochondrial and metabolic processes, muscle contractility) and reduced expression of pacemaker gene programs (neuronal, Wnt signaling, calcium/ion channel activity). By integrating chromatin accessibility profiles (ATAC sequencing) of atrioventricular tissue and other epigenetic data, we identified Tbx3-dependent atrioventricular regulatory DNA elements (REs) on a genome-wide scale. We used transgenic reporter assays to determine the functionality of candidate REs near Ryr2, an up-regulated chamber-enriched gene, and in Cacna1g, a down-regulated conduction system-specific gene. Using genome editing to delete candidate REs, we showed that a strong intronic bipartite RE selectively governs Cacna1g expression in the conduction system in vivo. Our data provide insights into the multifactorial Tbx3-dependent transcriptional network that regulates the structure and function of the cardiac conduction system, which may underlie the differences in PR duration and QRS interval between individuals carrying variants in the TBX3 locus.",

keywords = "Atrioventricular conduction system, Cacna1g, Electrical patterning, Ryr2, Tbx3",

author = "Mohan, {Rajiv A.} and Bosada, {Fernanda M.} and {van Weerd}, {Jan H.} and {van Duijvenboden}, Karel and Jianan Wang and Mommersteeg, {Mathilda T. M.} and Hooijkaas, {Ingeborg B.} and Vincent Wakker and {de Gier-de Vries}, Corrie and Ruben Coronel and Boink, {Gerard J. J.} and Jeroen Bakkers and Phil Barnett and Boukens, {Bas J.} and Christoffels, {Vincent M.}",

year = "2020",

month = aug,

day = "4",

doi = "https://doi.org/10.1073/pnas.1919379117",

language = "English",

volume = "117",

pages = "18617--18626",

journal = "PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA",

issn = "0027-8424",

publisher = "National Acad Sciences",

number = "31",

}

Mohan, RA , Bosada, FM, van Weerd, JH, van Duijvenboden, K , Wang, J, Mommersteeg, MTM, Hooijkaas, IB, Wakker, V, de Gier-de Vries, C , Coronel, R , Boink, GJJ, Bakkers, J, Barnett, P , Boukens, BJ & Christoffels, VM 2020, 'T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system', PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, vol. 117, no. 31, pp. 18617-18626. https://doi.org/10.1073/pnas.1919379117

T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system. / Mohan, Rajiv A.; Bosada, Fernanda M.; van Weerd, Jan H. et al.
In: PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, Vol. 117, No. 31, 04.08.2020, p. 18617-18626.

Research output: Contribution to journal › Article › Academic › peer-review

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T1 - T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system

AU - Mohan, Rajiv A.

AU - Bosada, Fernanda M.

AU - van Weerd, Jan H.

AU - van Duijvenboden, Karel

AU - Wang, Jianan

AU - Mommersteeg, Mathilda T. M.

AU - Hooijkaas, Ingeborg B.

AU - Wakker, Vincent

AU - de Gier-de Vries, Corrie

AU - Coronel, Ruben

AU - Boink, Gerard J. J.

AU - Bakkers, Jeroen

AU - Barnett, Phil

AU - Boukens, Bas J.

AU - Christoffels, Vincent M.

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AB - Genome-wide association studies have identified noncoding variants near TBX3 that are associated with PR interval and QRS duration, suggesting that subtle changes in TBX3 expression affect atrioventricular conduction system function. To explore whether and to what extent the atrioventricular conduction system is affected by Tbx3 dose reduction, we first characterized electrophysiological properties and morphology of heterozygous Tbx3 mutant (Tbx3+/-) mouse hearts. We found PR interval shortening and prolonged QRS duration, as well as atrioventricular bundle hypoplasia after birth in heterozygous mice. The atrioventricular node size was unaffected. Transcriptomic analysis of atrioventricular nodes isolated by laser capture microdissection revealed hundreds of deregulated genes in Tbx3+/- mutants. Notably, Tbx3+/- atrioventricular nodes showed increased expression of working myocardial gene programs (mitochondrial and metabolic processes, muscle contractility) and reduced expression of pacemaker gene programs (neuronal, Wnt signaling, calcium/ion channel activity). By integrating chromatin accessibility profiles (ATAC sequencing) of atrioventricular tissue and other epigenetic data, we identified Tbx3-dependent atrioventricular regulatory DNA elements (REs) on a genome-wide scale. We used transgenic reporter assays to determine the functionality of candidate REs near Ryr2, an up-regulated chamber-enriched gene, and in Cacna1g, a down-regulated conduction system-specific gene. Using genome editing to delete candidate REs, we showed that a strong intronic bipartite RE selectively governs Cacna1g expression in the conduction system in vivo. Our data provide insights into the multifactorial Tbx3-dependent transcriptional network that regulates the structure and function of the cardiac conduction system, which may underlie the differences in PR duration and QRS interval between individuals carrying variants in the TBX3 locus.

KW - Atrioventricular conduction system

KW - Cacna1g

KW - Electrical patterning

KW - Ryr2

KW - Tbx3

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JF - PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA

IS - 31

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Mohan RA , Bosada FM, van Weerd JH, van Duijvenboden K , Wang J, Mommersteeg MTM et al. T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA. 2020 Aug 4;117(31):18617-18626. doi: https://doi.org/10.1073/pnas.1919379117

T-box transcription factor 3 governs a transcriptional program for the function of the mouse atrioventricular conduction system

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