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TAK1 operates at the primary cilium in non-canonical TGFB/BMP signaling to control heart development

TAK1 operates at the primary cilium in non-canonical TGFB/BMP signaling to control heart development
TAK1 operates at the primary cilium in non-canonical TGFB/BMP signaling to control heart development
Transforming Growth Factor-Beta-Activated Kinase 1 (TAK1/MAP3K7), along with its upstream regulators TAK1-Binding Protein 2 (TAB2) and the catalytic alpha-subunit of Protein Kinase A (PKA-Cα/PRKACA), has been identified as a pivotal player in regulation of developmental processes. Haploinsufficiency of TAB2 causes Congenital Heart Disease (CHD) and rare variants in PKA-Cα and TAK1 cause cardioacrofacial dysplasia (CAFD), and Frontometaphyseal Dysplasia (FMD) and cardiospondylocarpofacial syndrome (CSCFS), respectively, rare multisystem syndromes, where CHD may appear in the clinical spectrum. We hypothesized that TAK1 plays a significant role in heart development and CHD and addressed this by genetic analysis in CHD patient cohorts and experiments in cell and animal models. Exome sequencing data from 1,471 CHD patients with extracardiac anomalies (syndromic CHD, sCHD), 2,405 patients with nonsyndromic CHD (nsCHD) and 45,082 controls showed increased burden of rare TAB2 and TAK1 variants in sCHD, but not in nsCHD. Detailed characterization of tak1-/-and tab2-/- zebrafish mutants revealed cardiac defects (dilated atrium, trabeculation defects, tachycardia and reduced contractility) as well as extracardiac developmental anomalies. RNA sequencing of tak1-/- mutant hearts showed downregulation of genes encoding core cardiac transcription factors, sarcomeric proteins and extracellular matrix proteins. Experiments with cell cultures and analysis of zebrafish larvae and gastruloids indicated that TAK1 via TAB2 and PKA-Cα is activated at the primary cilium during cardiomyogenesis and that TAK1 activation at this site is enhanced by cardiomyogenic signaling molecules, including ligands of the TGFB/BMP superfamily. Consistent with these findings, CRISPR/Cas9-mediated editing of TAK1 or administration of small molecule inhibitors targeting TAK1 inhibited ciliary signaling and cardiomyocyte differentiation in vitro, while FMD-causing mutations in TAK1 reduced its ciliary localization. In conclusion, our data establishes a central role for TAK1 and its upstream regulators in cardiac development and syndromic CHD, coordinated via the primary cilium.
bioRxiv
Doganli, Canan
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Baird, Daniel A.
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Ali, Yeasmeen
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Thomsen, Oskar Kaaber
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Audain, Enrique
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Jessen, Line
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Truelsen, Pauline Munck
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Mogensen, Johanne Bay
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Holm, Maria Schrøder
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Apolínová, Kateřina
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Buttò, Lorenzo
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Diamanti, Maria
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Fialová, Jindřiška Leischner
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Wade, Emma M.
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Robertson, Stephen P.
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Pedersen, Lotte Bang
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Argiro, Laurent
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Lescroart, Fabienne
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Hitz, Marc-Phillip
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Christensen, Søren Tvorup
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Larsen, Lars Allan
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Doganli, Canan
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Baird, Daniel A.
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Ali, Yeasmeen
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Thomsen, Oskar Kaaber
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Audain, Enrique
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Jessen, Line
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Truelsen, Pauline Munck
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Mogensen, Johanne Bay
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Holm, Maria Schrøder
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Apolínová, Kateřina
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Buttò, Lorenzo
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Diamanti, Maria
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Fialová, Jindřiška Leischner
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Wade, Emma M.
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Robertson, Stephen P.
73dfe348-c5a6-4e7e-851e-55f3b27e4890
Pedersen, Lotte Bang
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Argiro, Laurent
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Lescroart, Fabienne
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Hitz, Marc-Phillip
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Christensen, Søren Tvorup
a1cb5498-ba15-4cdb-8bda-f0cb54544028
Larsen, Lars Allan
fd2c35cc-3917-4f4c-9605-512ada43e049

[Unknown type: UNSPECIFIED]

Record type: UNSPECIFIED

Abstract

Transforming Growth Factor-Beta-Activated Kinase 1 (TAK1/MAP3K7), along with its upstream regulators TAK1-Binding Protein 2 (TAB2) and the catalytic alpha-subunit of Protein Kinase A (PKA-Cα/PRKACA), has been identified as a pivotal player in regulation of developmental processes. Haploinsufficiency of TAB2 causes Congenital Heart Disease (CHD) and rare variants in PKA-Cα and TAK1 cause cardioacrofacial dysplasia (CAFD), and Frontometaphyseal Dysplasia (FMD) and cardiospondylocarpofacial syndrome (CSCFS), respectively, rare multisystem syndromes, where CHD may appear in the clinical spectrum. We hypothesized that TAK1 plays a significant role in heart development and CHD and addressed this by genetic analysis in CHD patient cohorts and experiments in cell and animal models. Exome sequencing data from 1,471 CHD patients with extracardiac anomalies (syndromic CHD, sCHD), 2,405 patients with nonsyndromic CHD (nsCHD) and 45,082 controls showed increased burden of rare TAB2 and TAK1 variants in sCHD, but not in nsCHD. Detailed characterization of tak1-/-and tab2-/- zebrafish mutants revealed cardiac defects (dilated atrium, trabeculation defects, tachycardia and reduced contractility) as well as extracardiac developmental anomalies. RNA sequencing of tak1-/- mutant hearts showed downregulation of genes encoding core cardiac transcription factors, sarcomeric proteins and extracellular matrix proteins. Experiments with cell cultures and analysis of zebrafish larvae and gastruloids indicated that TAK1 via TAB2 and PKA-Cα is activated at the primary cilium during cardiomyogenesis and that TAK1 activation at this site is enhanced by cardiomyogenic signaling molecules, including ligands of the TGFB/BMP superfamily. Consistent with these findings, CRISPR/Cas9-mediated editing of TAK1 or administration of small molecule inhibitors targeting TAK1 inhibited ciliary signaling and cardiomyocyte differentiation in vitro, while FMD-causing mutations in TAK1 reduced its ciliary localization. In conclusion, our data establishes a central role for TAK1 and its upstream regulators in cardiac development and syndromic CHD, coordinated via the primary cilium.

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Published date: 8 May 2024

Identifiers

Local EPrints ID: 500543
URI: http://eprints.soton.ac.uk/id/eprint/500543
DOI: doi:10.1101/2024.05.06.592628
PURE UUID: 8ac42d47-978b-495e-be4e-18f48547e236
ORCID for Kateřina Apolínová: ORCID iD orcid.org/0009-0002-2066-7374

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Date deposited: 06 May 2025 16:33
Last modified: 07 May 2025 02:16

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Contributors

Author: Canan Doganli
Author: Daniel A. Baird
Author: Yeasmeen Ali
Author: Oskar Kaaber Thomsen
Author: Enrique Audain
Author: Line Jessen
Author: Pauline Munck Truelsen
Author: Johanne Bay Mogensen
Author: Maria Schrøder Holm
Author: Kateřina Apolínová ORCID iD
Author: Lorenzo Buttò
Author: Maria Diamanti
Author: Jindřiška Leischner Fialová
Author: Emma M. Wade
Author: Stephen P. Robertson
Author: Lotte Bang Pedersen
Author: Laurent Argiro
Author: Fabienne Lescroart
Author: Marc-Phillip Hitz
Author: Søren Tvorup Christensen
Author: Lars Allan Larsen

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