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首页> 外文期刊>STEM CELLS >Reduction of Shp-2 Expression by Small Interfering RNA Reduces Murine Embryonic Stem Cell-Derived In Vitro Hematopoietic Differentiation
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Reduction of Shp-2 Expression by Small Interfering RNA Reduces Murine Embryonic Stem Cell-Derived In Vitro Hematopoietic Differentiation

机译:小干扰RNA减少Shp-2表达减少小鼠胚胎干细胞衍生的体外造血分化。

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摘要

Shp-2 is a member of a small family of cytoplasmic Src homology 2 (SH2) domain-containing protein tyrosine phosphatases. Although Shp-2 has been shown to be necessary for hematopoiesis using a mouse model expressing a mutant residual protein (Shp-2/), we used small interfering RNA (siRNA) to reduce Shp-2 expression and examined the consequences on embryonic stem cell (ESC)-derived hemangioblast, primitive, and definitive hematopoietic development. We found that at a concentration of 50 nM, Shp-2 siRNA effectively diminished Shp-2 expression in differentiating embryoid bodies. Hemangioblast, primitive, and definitive hematopoietic progenitor formation was decreased significantly after transfection with Shp-2 siRNA but not with scrambled siRNA. Because Shp-2 is involved in signals emanating from the basic fibroblast growth factor (bFGF) receptor, we asked whether Shp-2 functions in bFGF-mediated hemangioblast development. Reduction of Shp-2 expression using siRNA, but not scrambled siRNA, blocked the bFGF-induced increase in hemangioblast development. Using siRNA as an independent method of reducing Shp-2 function, in contrast to the mutant mouse model (Shp-2/) previously used, we demonstrate that Shp-2 is required in hemangioblast, primitive, and definitive progenitor hematopoietic development and that Shp-2 is integrally necessary for bFGF-mediated hemangioblast production.
机译:Shp-2是一小部分细胞质Src同源2(SH2)域包含蛋白酪氨酸磷酸酶。尽管使用表达突变残留蛋白(Shp-2 /)的小鼠模型显示Shp-2对于造血是必需的,但我们使用小干扰RNA(siRNA)来减少Shp-2的表达,并研究了其对胚胎干细胞的影响(ESC)衍生的成血管细胞,原始和确定的造血发育。我们发现,在50 nM的浓度下,Shp-2 siRNA可有效减少分化胚状体中Shp-2的表达。用Shp-2 siRNA转染后,成血成血管细胞,原始和确定的造血祖细胞形成显着减少,但未加扰的siRNA则没有。由于Shp-2参与了从基本成纤维细胞生长因子(bFGF)受体发出的信号,因此我们询问Shp-2是否在bFGF介导的成血管细胞发育中起作用。使用siRNA而不是加扰的siRNA减少Shp-2表达,可阻止bFGF诱导的成血管细胞发育增加。与以前使用的突变小鼠模型(Shp-2 /)相比,使用siRNA作为降低Shp-2功能的独立方法,我们证明了成血成血管细胞,原始和确定的祖细胞造血发育中需要Shp-2,并且Shp -2对于bFGF介导的成血成血管细胞生产必不可少。

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