HAND transcription factors cooperatively specify the aorta and pulmonary trunk

Congenital heart defects (CHDs) affecting the cardiac outflow tract (OFT) constitute a significant cause of morbidity and mortality. The OFT develops from migratory cell populations which include the cardiac neural crest cells (cNCCs) and secondary heart field (SHF) derived myocardium and endocardiu...

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Published in:Developmental biology 2021-08, Vol.476, p.1-10
Main Authors: Vincentz, Joshua W., Firulli, Beth A., Toolan, Kevin P., Osterwalder, Marco, Pennacchio, Len A., Firulli, Anthony B.
Format: Article
Language:English
Subjects:
BASIC BIOLOGICAL SCIENCES
bHLH transcription factors
Cardiac neural crest
Cardiac outflow track
Congenital heart defects
HAND1
HAND2
Second heart field
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cited_by cdi_FETCH-LOGICAL-c486t-a3837320ba8769ab1100dfd26e8081bd4389a5ca63335865e2002d98a5aacc3e3
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container_title Developmental biology
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creator Vincentz, Joshua W.
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description Congenital heart defects (CHDs) affecting the cardiac outflow tract (OFT) constitute a significant cause of morbidity and mortality. The OFT develops from migratory cell populations which include the cardiac neural crest cells (cNCCs) and secondary heart field (SHF) derived myocardium and endocardium. The related transcription factors HAND1 and HAND2 have been implicated in human CHDs involving the OFT. Although Hand1 is expressed within the OFT, Hand1 NCC-specific conditional knockout mice (H1CKOs) are viable. Here we show that these H1CKOs present a low penetrance of OFT phenotypes, whereas SHF-specific Hand1 ablation does not reveal any cardiac phenotypes. Further, HAND1 and HAND2 appear functionally redundant within the cNCCs, as a reduction/ablation of Hand2 on an NCC-specific H1CKO background causes pronounced OFT defects. Double conditional Hand1 and Hand2 NCC knockouts exhibit persistent truncus arteriosus (PTA) with 100% penetrance. NCC lineage-tracing and Sema3c in situ mRNA expression reveal that Sema3c-expressing cells are mis-localized, resulting in a malformed septal bridge within the OFTs of H1CKO;H2CKO embryos. Interestingly, Hand1 and Hand2 also genetically interact within the SHF, as SHF H1CKOs on a heterozygous Hand2 background exhibit Ventricular Septal Defects (VSDs) with incomplete penetrance. Previously, we identified a BMP, HAND2, and GATA-dependent Hand1 OFT enhancer sufficient to drive reporter gene expression within the nascent OFT and aorta. Using these transcription inputs as a probe, we identify a novel Hand2 OFT enhancer, suggesting that a conserved BMP-GATA dependent mechanism transcriptionally regulates both HAND factors. These findings support the hypothesis that HAND factors interpret BMP signaling within the cNCCs to cooperatively coordinate OFT morphogenesis. •HAND1 and HAND2 genetically interact within the cardiac neural crest.•HAND1 and HAND2 double mutants reveal a mis-organization of cardiac neural crest.•Prediction of a ​Hand2 ​cNCC enhancer based on an identified ​Hand1 ​enhancer shows conservation in upstream transcriptional regulation.
doi_str_mv 10.1016/j.ydbio.2021.03.011
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1095-564X
language eng
recordid cdi_pubmedcentral_primary_oai_pubmedcentral_nih_gov_8172455
source Elsevier
subjects BASIC BIOLOGICAL SCIENCES
bHLH transcription factors
Cardiac neural crest
Cardiac outflow track
Congenital heart defects
HAND1
HAND2
Second heart field
Transcription
title HAND transcription factors cooperatively specify the aorta and pulmonary trunk
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