Cell Reports (Jul 2017)

TGF-β Signaling Is Necessary and Sufficient for Pharyngeal Arch Artery Angioblast Formation

  • Maryline Abrial,
  • Noëlle Paffett-Lugassy,
  • Spencer Jeffrey,
  • Daniel Jordan,
  • Evan O’Loughlin,
  • Charles J. Frederick, III,
  • C. Geoffrey Burns,
  • Caroline E. Burns

DOI
https://doi.org/10.1016/j.celrep.2017.07.002
Journal volume & issue
Vol. 20, no. 4
pp. 973 – 983

Abstract

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The pharyngeal arch arteries (PAAs) are transient embryonic blood vessels that mature into critical segments of the aortic arch and its branches. Although defects in PAA development cause life-threating congenital cardiovascular defects, the molecular mechanisms that orchestrate PAA morphogenesis remain unclear. Through small-molecule screening in zebrafish, we identified TGF-β signaling as indispensable for PAA development. Specifically, chemical inhibition of the TGF-β type I receptor ALK5 impairs PAA development because nkx2.5+ PAA progenitor cells fail to differentiate into tie1+ angioblasts. Consistent with this observation, we documented a burst of ALK5-mediated Smad3 phosphorylation within PAA progenitors that foreshadows angioblast emergence. Remarkably, premature induction of TGF-β receptor activity stimulates precocious angioblast differentiation, thereby demonstrating the sufficiency of this pathway for initiating the PAA progenitor to angioblast transition. More broadly, these data uncover TGF-β as a rare signaling pathway that is necessary and sufficient for angioblast lineage commitment.

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