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在胚胎干细胞的体外分化过程中,SHB衔接蛋白是中胚层正常成熟所必需的。

The SHB adapter protein is required for normal maturation of mesoderm during in vitro differentiation of embryonic stem cells.

作者信息

Kriz Vitezslav, Agren Nina, Lindholm Cecilia K, Lenell Samuel, Saldeen Johan, Mares Jaroslav, Welsh Michael

机构信息

Department of Medical Cell Biology, Uppsala University, Uppsala 75123, Sweden.

出版信息

J Biol Chem. 2006 Nov 10;281(45):34484-91. doi: 10.1074/jbc.M604084200. Epub 2006 Sep 12.

DOI:10.1074/jbc.M604084200
PMID:16971391
Abstract

Definitive mesoderm arises from a bipotent mesendodermal population, and to study processes controlling its development at this stage, embryonic stem (ES) cells can be employed. SHB (Src homology 2 protein in beta-cells) is an adapter protein previously found to be involved in ES cell differentiation to mesoderm. To further study the role of SHB in this context, we have established ES cell lines deficient for one (SHB+/-) or both SHB alleles (SHB-/-). Differentiating embryoid bodies (EBs) derived from these ES cell lines were used for gene expression analysis. Alternatively, EBs were stained for the blood vessel marker CD31. For hematopoietic differentiation, EBs were differentiated in methylcellulose. SHB-/- EBs exhibited delayed down-regulation of the early mesodermal marker Brachyury. Later mesodermal markers relatively specific for the hematopoietic, vascular, and cardiac lineages were expressed at lower levels on day 6 or 8 of differentiation in EBs lacking SHB. The expression of vascular endothelial growth factor receptor-2 and fibroblast growth factor receptor-1 was also reduced in SHB-/- EBs. SHB-/- EBs demonstrated impaired blood vessel formation after vascular endothelial growth factor stimulation. In addition, the SHB-/- ES cells formed fewer blood cell colonies than SHB+/+ ES cells. It is concluded that SHB is required for appropriate hematopoietic and vascular differentiation and that delayed down-regulation of Brachyury expression may play a role in this context.

摘要

确定中胚层起源于双能性的中内胚层群体,为了研究在此阶段控制其发育的过程,可以利用胚胎干细胞(ES细胞)。SHB(β细胞中的Src同源2蛋白)是一种衔接蛋白,先前发现它参与ES细胞向中胚层的分化。为了进一步研究SHB在此过程中的作用,我们建立了缺失一个(SHB+/-)或两个SHB等位基因(SHB-/-)的ES细胞系。源自这些ES细胞系的分化胚状体(EBs)用于基因表达分析。或者,对EBs进行血管标志物CD31染色。对于造血分化,EBs在甲基纤维素中进行分化。SHB-/- EBs表现出早期中胚层标志物Brachyury的下调延迟。在缺乏SHB的EBs分化的第6天或第8天,相对特异于造血、血管和心脏谱系的后期中胚层标志物表达水平较低。血管内皮生长因子受体-2和成纤维细胞生长因子受体-1的表达在SHB-/- EBs中也降低。SHB-/- EBs在血管内皮生长因子刺激后显示出血管形成受损。此外,SHB-/- ES细胞形成的血细胞集落比SHB+/+ ES细胞少。得出的结论是,SHB是适当的造血和血管分化所必需的,并且Brachyury表达的延迟下调可能在此过程中起作用。

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