An Nkx2-5/Bmp2/Smad1 negative feedback loop controls heart progenitor specification and proliferation

作者:Prall Owen W J; Menon Mary K; Solloway Mark J; Watanabe Yusuke; Zaffran Stephane; Bajolle Fanny; Biben Christine; McBride Jim J; Robertson Bronwyn R; Chaulet Herve; Stennard Fiona A; Wise Natalie; Schaft Daniel; Wolstein Orit; Furtado Milena B; Shiratori Hidetaka; Chien Kenneth R; Hamada Hiroshi; Black Brian L; Saga Yumiko; Robertson Elizabeth J; Buckingham Margaret E; Harvey Richard P*
来源:Cell, 2007, 128(5): 947-959.
DOI:10.1016/j.cell.2007.01.042

摘要

During heart development the second heart field (SHF) provides progenitor cells for most cardiomyocytes and expresses the homeodomain factor Nkx2-5. We now show that feedback repression of Bmp2/Smad1 signaling by Nkx2-5 critically regulates SHF proliferation and outflow tract (OFT) morphology. In the cardiac fields of Nkx2-5 mutants, genes controlling cardiac specification (including Bmp2) and maintenance of the progenitor state were upregulated, leading initially to progenitor overspecification, but subsequently to failed SHF proliferation and OFT truncation. In Smad1 mutants, SHF proliferation and deployment to the OFT were increased, while Smad1 deletion in Nkx2-5 mutants rescued SHF proliferation and OFT development. In Nkx2-5 hyponnorphic mice, which recapitulate human congenital heart disease (CHD), OFT anomalies were also rescued by Smad1 deletion. Our findings demonstrate that Nkx2-5 orchestrates the transition between periods of cardiac induction, progenitor proliferation, and OFT morphogenesis via a Smadl dependent negative feedback loop, which may be a frequent molecular target in CHD.