CreER activation transiently impairs angiogenesis by slowing endothelial proliferation

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Abstract

Tamoxifen-inducible gene targeting in mice with estrogen receptor-dependent Cre (CreER) recombinase has enormously advanced vascular biology research. However, CreER activation under the control of vascular endothelial promoters is now recognized to cause off-target effects that impair angiogenesis in the widely used perinatal mouse retina model. Although ubiquitously expressed CreER is also used to study retinal angiogenesis, it remains unknown whether it causes similar or more severe off-target effects compared to endothelial-selective CreER activation. Moreover, the cellular processes disrupted by CreER-induced endothelial toxicity remain to be identified. Here, we demonstrate that ubiquitous CreER activation in postnatal mice decreases body growth throughout the period of retinal angiogenesis and impairs retinal angiogenesis in a tamoxifen dose-dependent manner. We further show that CreER activation from both endothelial and ubiquitously expressed CreER transgenes suppresses endothelial cell proliferation downstream of p21/CDKNA1 upregulation. By contrast, we find that p21/CDKNA1 is not upregulated in quiescent adult retinal endothelium, and that CreER-induced postnatal angiogenesis defects recover two weeks after tamoxifen discontinuation. Altogether, our findings indicate that ubiquitous promoters should be avoided for CreER expression when studying endothelial genes, and that short-term retinal angiogenesis studies require endothelial CreER toxicity controls that may be less critical for adult vascular studies.

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