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表达flk-1的胚胎肾细胞是内在的、血管生成性成血管细胞的证据。

Evidence that embryonic kidney cells expressing flk-1 are intrinsic, vasculogenic angioblasts.

作者信息

Robert B, St John P L, Hyink D P, Abrahamson D R

机构信息

Department of Comparative Medicine, University of Alabama at Birmingham 35294-0019, USA.

出版信息

Am J Physiol. 1996 Sep;271(3 Pt 2):F744-53. doi: 10.1152/ajprenal.1996.271.3.F744.

DOI:10.1152/ajprenal.1996.271.3.F744
PMID:8853438
Abstract

Renal glomerular capillary tufts have been believed to arise from angiogenic ingrowth of extrinsic vessels. We found, however, that when embryonic day 12 (E12) mouse kidneys were maintained in culture for 6 days and then grafted into anterior eye chambers of adult transgenic ROSA26 host mice (which carry the beta-galactosidase transgene), glomerular endothelial cells within the grafts were predominantly of intrinsic, kidney origin. To identify potential endothelial precursors, we immunolabled kidneys with antibodies against the vascular endothelial growth factor receptor, flk-1. Numerous discrete cells expressing flk-1 were scattered throughout the nephrogenic mesenchyme of both E12 and newborn kidneys, and with development these cells became concentrated in microvessels, glomerular vascular clefts, and glomerular tufts. In adults, flk-1 was weakly expressed in glomeruli but absent elsewhere. To examine abilities of flk-1-positive cells to establish glomeruli, E12 kidneys were grafted into kidney cortices of adult and newborn ROSA26 hosts. Grafts into adults resulted in few glomeruli containing host-derived endothelium, whereas a majority of glomeruli grafted into newborns contained host cells. Cells of graft origin were found in vessels forming in renal cortices of newborn hosts, but not in adults. Our findings indicate that embryonic kidney cells expressing flk-1 are angioblasts that create microvessels and glomeruli by vasculogenesis.

摘要

肾肾小球毛细血管丛一直被认为是由外部血管的血管生成性向内生长形成的。然而,我们发现,当将胚胎第12天(E12)的小鼠肾脏在培养物中培养6天,然后移植到成年转基因ROSA26宿主小鼠(携带β-半乳糖苷酶转基因)的前房时,移植肾内的肾小球内皮细胞主要来源于肾脏自身。为了鉴定潜在的内皮前体细胞,我们用抗血管内皮生长因子受体flk-1的抗体对肾脏进行免疫标记。大量表达flk-1的离散细胞散布在E12和新生小鼠肾脏的肾发生间充质中,随着发育,这些细胞集中在微血管、肾小球血管裂隙和肾小球丛中。在成年小鼠中,flk-1在肾小球中弱表达,而在其他部位则不存在。为了检测flk-1阳性细胞形成肾小球的能力,将E12肾脏移植到成年和新生ROSA26宿主的肾皮质中。移植到成年宿主中的肾脏形成的肾小球中含有宿主来源内皮细胞的很少,而移植到新生宿主中的大多数肾小球含有宿主细胞。在新生宿主肾皮质中正在形成的血管中发现了移植来源的细胞,但在成年宿主中未发现。我们的研究结果表明,表达flk-1的胚胎肾细胞是通过血管生成形成微血管和肾小球的成血管细胞。

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