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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >BMP9 and BMP10 are critical for postnatal retinal vascular remodeling
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BMP9 and BMP10 are critical for postnatal retinal vascular remodeling

机译:BMP9和BMP10对于产后视网膜血管重塑至关重要

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ALK1 is a type I receptor of the TGF-β family that is involved in angiogenesis. Circulating BMP9 was identified as a specific ligand for ALK1 inducing vascular quiescence. In this work, we found that blocking BMP9 with a neutralizing antibody in newborn mice significantly increased retinal vascular density. Surprisingly, Bmp9-KO mice did not show any defect in retinal vascularization. However, injection of the extracellular domain of ALK1 impaired retinal vascularization in Bmp9-KO mice, implicating another ligand for ALK1. Interestingly, we detected a high level of circulating BMP10 in WTand Bmp9-KO pups. Further, we found that injection of a neutralizing anti-BMP10 antibody to Bmp9-KO pups reduced retinal vascular expansion and increased vascular density, whereas injection of this antibody to WT pups did not affect the retinal vasculature. These data suggested that BMP9 and BMP10 are important in postnatal vascular remodeling of the retina and that BMP10 can substitute for BMP9. In vitro stimulation of endothelial cells by BMP9 and BMP10 increased the expression of genes involved in the Notch signaling pathway (Jagged1, Dll4, Hey1, Hey2, Hes1) and decreased apelin expression, suggesting a possible cross-talk between these pathways and the BMP pathway.
机译:ALK1是TGF-β家族的I型受体,参与血管生成。循环中的BMP9被确定为ALK1诱导血管静止的特异性配体。在这项工作中,我们发现新生小鼠用中和抗体阻断BMP9会显着增加视网膜血管密度。出乎意料的是,Bmp9-KO小鼠在视网膜血管形成中未显示任何缺陷。但是,注射ALK1的细胞外结构域会损害Bmp9-KO小鼠的视网膜血管形成,暗示ALK1的另一种配体。有趣的是,我们在WT和Bmp9-KO幼犬中检测到高水平的循环BMP10。此外,我们发现向Bmp9-KO幼犬注射中和性抗BMP10抗体可降低视网膜血管扩张并增加血管密度,而向WT幼犬注射该抗体不会影响视网膜血管。这些数据表明BMP9和BMP10在视网膜的产后血管重塑中很重要,并且BMP10可以替代BMP9。 BMP9和BMP10体外刺激内皮细胞增加了Notch信号通路中涉及的基因的表达(Jagged1,Dll4,Hey1,Hey2,Hes1),并且降低了apelin的表达,表明这些通路与BMP通路之间可能存在相互影响。

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