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STAT3 和 SMAD1 信号在 Medaka 胚胎干细胞样细胞和囊胚胚胎中的作用。

STAT3 and SMAD1 signaling in Medaka embryonic stem-like cells and blastula embryos.

机构信息

University of Wurzburg, Physiological Chemistry I, Wurzburg, Germany.

出版信息

Stem Cells Dev. 2009 Jan-Feb;18(1):151-60. doi: 10.1089/scd.2007.0262.

Abstract

The activation and transcriptional activity of signal transducer and activator of transcription 3 (STAT3) is essential for maintaining mouse embryonic stem (ES) cell cultures in an undifferentiated state. However, reports from human and monkey ES-cell culture suggest that STAT3 is dispensable for pluripotency in these systems. At the same time, BMP signaling via smad1 was shown to be able to counteract STAT3 signaling in murine ES-cell cultures, while it influences differentiation in multifaceted ways in other cellular contexts. Hence, the question arises whether the signaling situation found in mice or primates and human ES-cells represent the rule or the exception. With this study, we want to contribute an answer to this question from an evolutionary perspective. Therefore, we analyzed the expression and activation status of the Medaka (Oryzias latipes) STAT3 and SMAD1 in Medaka ES-cell-like cultures and their in vivo counterpart, the Medaka blastula embryo. While SMAD signaling is active in the culture system as well as in blastula embryos, our results indicate that STAT3 is inactive and can thus not be involved in pluripotency control of blastula cells or their derived pluripotent in vitro counterparts. These results suggest that the signaling pathways active in the mouse ES-cell culture system represent the exception, while inactivity of STAT3 is apparently the rule in vertebrate ES-cell cultures.

摘要

信号转导子和转录激活子 3(STAT3)的激活和转录活性对于维持小鼠胚胎干细胞(ES 细胞)在未分化状态下的培养至关重要。然而,来自人类和猴 ES 细胞培养的报告表明,在这些系统中,STAT3 对于多能性是可有可无的。与此同时,BMP 信号通过 smad1 被证明能够在鼠 ES 细胞培养物中拮抗 STAT3 信号,而在其他细胞环境中,它以多种方式影响分化。因此,问题出现了,在小鼠、灵长类动物和人类 ES 细胞中发现的信号情况是普遍现象还是例外。通过这项研究,我们希望从进化的角度对这个问题做出回答。因此,我们分析了 Medaka(Oryzias latipes)STAT3 和 SMAD1 在 Medaka ES 细胞样培养物及其体内对应物 Medaka 囊胚中的表达和激活状态。虽然 SMAD 信号在培养系统以及囊胚胚胎中都是活跃的,但我们的结果表明 STAT3 是不活跃的,因此不能参与囊胚细胞或其衍生的体外多能性的多能性控制。这些结果表明,在小鼠 ES 细胞培养系统中活跃的信号通路代表了例外情况,而 STAT3 的不活跃显然是在脊椎动物 ES 细胞培养中是普遍现象。

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