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Yu-2010-TRPC1 is essential f
TRPC1 Is Essential for In Vivo Angiogenesis
in Zebrafish
Peng-chun Yu, Shan-ye Gu,* Ji-wen Bu,* Jiu-lin Du
Rationale: Wiring vascular and neural networks are known to share common molecular signaling pathways.
Activation of transient receptor potential type C channels (TRPCs) has recently been shown to underlie
chemotropic guidance of neural axons. It is thus of interest to examine whether TRPCs are also involved in
vascular development.
Objective: To determine the role of TRPC1 in angiogenesis in vivo during zebrafish development.
Methods and Results: Knockdown of zebrafish trpc1 by antisense morpholino oligonucleotides severely
disrupted angiogenic sprouting of intersegmental vessels (ISVs) in zebrafish larvae. This angiogenic defect
was prevented by overexpression of a morpholino oligonucleotide–resistant form of zebrafish trpc1 mRNA.
Cell transplantation analysis showed that this requirement of Trpc1 for ISV growth was endothelial
cell–autonomous. In vivo time-lapse imaging further revealed that the angiogenic defect was attributable to
impairment of filopodia extension, migration, and proliferation of ISV tip cells. Furthermore, Trpc1 acted
synergistically with vascular endothelial growth factor A (Vegf-a) in controlling ISV growth, and appeared
to be downstream to Vegf-a in controlling angiogenesis, as evidence by the findings that Trpc1 was required
for Vegf-a–induced ectopic angiogenesis of subintestinal veins and phosphorylation of extracellular
signal-regulated kinase.
Conclusions: These results provide the first in vivo evidence that TRPC1 is essential for angiogenesis, reminiscent
of the role of TRPCs in axon guidance. It implicates that TRPC1 may represent a potential target for treating
pathological angiogenesis. (Circ Res. 2010;106:1221-1232.)
Key Words: TRPC1 VEGF ISV angiogenesis zebrafish
The vascular system of vertebrates consists of a stereo-typed and highly branched network of arteries, veins,
and capillaries. This network extends into e
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