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The Role of SMAD4 in Human Embryonic Stem Cell Self-Renewal and Stem Cell Fate§

机译:SMAD4在人类胚胎干细胞自我更新和干细胞命运中的作用 §

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Transforming growth factor (TGF)- superfamily proteins play a key role in the regulation of human embryonic stem cells (hESCs). Those of the TGF/activinodal branch seem to support self-renewal and pluripotency, whereas those of the bone morphogenic protein (BMP) branch induce differentiation. In contrast to this generalization, we found that hESC remained undifferentiated after knockdown of SMAD4 with inducible short hairpin RNA interference, although the knockdown inhibited TGF signaling and rendered the cells nonresponsive to BMP-induced differentiation. Moreover, the rapid differentiation of hESC after pharmacological inhibition of TGF/activinodal receptor signaling was restricted after SMAD4 knockdown. These results suggest that TGF/activinodal signaling supports the undifferentiated phenotype of hESC by suppressing BMP activity. During long-term culture, SMAD4 knockdown cell populations became less stable and more permissive to neural induction, a situation that was rescued by re-establishment of SMAD4 expression. These results suggest that SMAD4 is not required for maintenance of the undifferentiated state of hESC, but rather to stabilize that state. STEM CELLS 2010;28:863-873
机译:转化生长因子(TGF)-超家族蛋白在调节人类胚胎干细胞(hESCs)中起着关键作用。 TGF /激活素/淋巴结分支的那些似乎支持自我更新和多能性,而骨形态发生蛋白(BMP)分支的那些则诱导分化。与这种概括相反,我们发现敲除SMAD4并诱导可诱导的短发夹RNA干扰后,hESC仍未分化,尽管敲除抑制了TGF信号转导并使细胞对BMP诱导的分化无反应。此外,SMAD4敲低后,抑制TGF /激活素/节点受体信号转导后hESC的快速分化受到限制。这些结果表明,TGF /激活素/节点信号转导通过抑制BMP活性来支持hESC的未分化表型。在长期培养过程中,SMAD4敲低的细胞群变得不稳定,对神经诱导的容许更大,这种情况通过重新建立SMAD4表达得以挽救。这些结果表明SMAD4不需要维持hESC的未分化状态,而是稳定该状态。干细胞2010; 28:863-873

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    《STEM CELLS》 |2010年第5期|863-873|共11页
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    Department of Biomedical Science, Centre for Stem Cell Biology, University of Sheffield, Western Bank, Sheffield, S10 2TN, United Kingdom|Institute of Medical Biology, A*STAR, 8A Biomedical Grove, Immunos 05-40, Singapore 138648, Singapore;

    Department of Biomedical Science, Centre for Stem Cell Biology, University of Sheffield, Western Bank, Sheffield, S10 2TN, United Kingdom|Princess Margaret Hospital (University Health Network) Department of Radiation Oncology, 610 University Ave, Toronto, ON M5G 2M9, Canada;

    Department of Biomedical Science, Centre for Stem Cell Biology, University of Sheffield, Western Bank, Sheffield, S10 2TN, United Kingdom;

    Department of Biomedical Science, Centre for Stem Cell Biology, University of Sheffield, Western Bank, Sheffield, S10 2TN, United Kingdom;

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