4.4 Article

The LIM-homeodomain transcription factor Islet2a promotes angioblast migration

Journal

DEVELOPMENTAL BIOLOGY
Volume 414, Issue 2, Pages 181-192

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ydbio.2016.04.019

Keywords

Islet2a; Vein; Notch; Artery; Angioblast

Funding

  1. CIHR [MOP 97787]
  2. Tier II Canada Research Chair
  3. AHFMR Senior Scholar award
  4. HSFC Doctoral Research Award
  5. AHFMR
  6. CIHR Training Grant on Genetics
  7. Child Health and Development
  8. Heart and Stroke Foundation of Canada
  9. AIHS
  10. NSERC

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Angioblasts of the developing vascular system require many signaling inputs to initiate their migration, proliferation and differentiation into endothelial cells. What is less studied is which intrinsic cell factors interpret these extrinsic signals. Here, we show the Lim homeodomain transcription factor islet2a (isl2a) is expressed in the lateral posterior mesoderm prior to angioblast migration. isl2a deficient angioblasts show disorganized migration to the midline to form axial vessels and fail to spread around the tailbud of the embryo. Isl2a morphants have fewer vein cells and decreased vein marker expression. We demonstrate that isl2a is required cell autonomously in angioblasts to promote their incorporation into the vein, and is permissive for vein identity. Knockout of isl2a results in decreased migration and proliferation of angioblasts during intersegmental artery growth. Since Notch signaling controls both artery-vein identity and tip-stalk cell formation, we explored the interaction of isl2a and Notch. We find that isl2a expression is negatively regulated by Notch activity, and that isl2a positively regulates flt4, a VEGF-C receptor repressed by Notch during angiogenesis. Thus Isl2a may act as an intermediate between Notch signaling and genetic programs controlling angioblast number and migration, placing it as a novel transcriptional regulator of early angiogenesis. (C) 2016 Elsevier Inc. All rights reserved.

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