Journal
DEVELOPMENTAL CELL
Volume 10, Issue 6, Pages 783-795Publisher
CELL PRESS
DOI: 10.1016/j.devcel.2006.03.012
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Funding
- NHLBI NIH HHS [HL62289, HL53793, HL067960] Funding Source: Medline
- NIAMS NIH HHS [T32 AR007576] Funding Source: Medline
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Branching morphogenesis is a key process in the formation of vascular networks. To date, little is known regarding the molecular events regulating this process. We investigated the involvement of synectin in this process. In zebrafish embryos, synectin knockdown resulted in a hypoplastic dorsal aorta and hypobranched, stunted, and thin intersomitic vessels due to impaired migration and proliferation of angioblasts and arterial endothelial cells while not affecting venous development. Synectin(-/-) mice demonstrated decreased body and organ size, reduced numbers of arteries, and an altered pattern of arterial branching in multiple vascular beds while the venous system remained normal. Murine synectin(-/-) primary arterial, but not venous, endothelial cells showed decreased in vitro tube formation, migration, and proliferation and impaired polarization due to abnormal localization of activated Rac1. We conclude that synectin is involved in selective regulation of arterial, but not venous, growth and branching morphogenesis and that Rac1 plays an important role in this process.
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