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Development ePress online publication date 5 Nov 2008
doi: 10.1242/dev.029736


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Attribution of vascular phenotypes of the murine Egfl7 locus to the microRNA miR-126


Frank Kuhnert, Michael R. Mancuso, Jessica Hampton, Kryn Stankunas, Tomoichiro Asano, Chang-Zheng Chen, and Calvin J. Kuo*
* Author for correspondence (e-mail: cjkuo{at}stanford.edu)

Intronic microRNAs have been proposed to complicate the design and interpretation of mouse knockout studies. The endothelial-expressed Egfl7/miR-126 locus contains miR-126 within Egfl7 intron 7, and angiogenesis deficits have been previously ascribed to Egfl7 gene-trap and lacZ knock-in mice. Surprisingly, selectively floxed Egfl7{Delta} and miR-126{Delta} alleles revealed that Egfl7{Delta}/{Delta} mice were phenotypically normal, whereas miR-126{Delta}/{Delta} mice bearing a 289-nt microdeletion recapitulated previously described Egfl7 embryonic and postnatal retinal vascular phenotypes. Regulation of angiogenesis by miR-126 was confirmed by endothelial-specific deletion and in the adult cornea micropocket assay. Furthermore, miR-126 deletion inhibited VEGF-dependent Akt and Erk signaling by derepression of the p85{beta} subunit of PI3 kinase and of Spred1, respectively. These studies demonstrate the regulation of angiogenesis by an endothelial miRNA, attribute previously described Egfl7 vascular phenotypes to miR-126, and document inadvertent miRNA dysregulation as a complication of mouse knockout strategies


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