MRC Molecular Haematology Unit, Weatherall Institute of Molecular Medicine, John Radcliffe Hospital, Oxford University, OX3 9DS Oxford, UK.
Dev Cell. 2013 Jan 28;24(2):144-58. doi: 10.1016/j.devcel.2012.12.004. Epub 2013 Jan 11.
VEGFA signaling is critical for endothelial and hematopoietic stem cell (HSC) specification. However, blood defects resulting from perturbation of the VEGFA pathway are always accompanied by impaired vascular/arterial development. Because HSCs derive from arterial cells, it is unclear whether VEGFA directly contributes to HSC specification. This is an important question for our understanding of how HSCs are formed and for developing their production in vitro. Through knockdown of the regulator ETO2 in embryogenesis, we report a specific decrease in expression of medium/long Vegfa isoforms in somites. This leads to absence of Notch1 expression and failure of HSC specification in the dorsal aorta (DA), independently of vessel formation and arterial specification. Vegfa hypomorphs and isoform-specific (medium/long) morphants not only recapitulate this phenotype but also demonstrate that VEGFA short isoform is sufficient for DA development. Therefore, sequential, isoform-specific VEGFA signaling successively induces the endothelial, arterial, and HSC programs in the DA.
VEGFA 信号对于内皮细胞和造血干细胞(HSC)的特化至关重要。然而,由于 VEGFA 通路的扰动导致的血液缺陷总是伴随着血管/动脉发育受损。由于 HSCs 源自动脉细胞,因此不清楚 VEGFA 是否直接有助于 HSC 的特化。这对于我们理解 HSCs 如何形成以及在体外产生它们是一个重要的问题。通过在胚胎发生中敲低调节剂 ETO2,我们报告了中/长 Vegfa 异构体在体节中的表达特异性下降。这导致 Notch1 表达缺失和背主动脉(DA)中 HSC 特化失败,而与血管形成和动脉特化无关。Vegfa 突变体和同工型特异性(中/长)嵌合体不仅再现了这种表型,还证明了 VEGFA 短同工型足以用于 DA 发育。因此,顺序的、同工型特异性的 VEGFA 信号相继诱导 DA 中的内皮细胞、动脉和 HSC 程序。
Zotero 插件
