首页> 外文OA文献 >E-box- and MEF-2-independent muscle-specific expression, positive autoregulation, and cross-activation of the chicken MyoD (CMD1) promoter reveal an indirect regulatory pathway.
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E-box- and MEF-2-independent muscle-specific expression, positive autoregulation, and cross-activation of the chicken MyoD (CMD1) promoter reveal an indirect regulatory pathway.

机译:E-box和MEF-2独立的肌肉特异性表达,阳性自我调节和鸡MyoD(CMD1)启动子的交叉激活揭示了间接调节途径。

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摘要

Members of the MyoD family of gene-regulatory proteins (MyoD, myogenin, myf5, and MRF4) have all been shown not only to regulate the transcription of numerous muscle-specific genes but also to positively autoregulate and cross activate each other's transcription. In the case of muscle-specific genes, this transcriptional regulation can often be correlated with the presence of a DNA consensus in the regulatory region CANNTG, known as an E box. Little is known about the regulatory interactions of the myogenic factors themselves; however, these interactions are thought to be important for the activation and maintenance of the muscle phenotype. We have identified the minimal region in the chicken MyoD (CMD1) promoter necessary for muscle-specific transcription in primary cultures of embryonic chicken skeletal muscle. The CMD1 promoter is silent in primary chick fibroblast cultures and in muscle cell cultures treated with the thymidine analog bromodeoxyuridine. However, CMD1 and chicken myogenin, as well as, to a lesser degree, chicken Myf5 and MRF4, expressed in trans can activate transcription from the minimal CMD1 promoter in these primary fibroblast cultures. Here we show that the CMD1 promoter contains numerous E-box binding sites for CMD1 and the other myogenic factors, as well as a MEF-2 binding site. Surprisingly, neither muscle-specific and the other myogenic factors, as well as a MEF-2 binding site. Surprisingly, neither muscle-specific expression, autoregulation, or cross activation depends upon the presence of of these E-box or MEF-2 binding sites in the CMD1 promoter. These results demonstrate that the autoregulation and cross activation of the chicken MyoD promoter through the putative direct binding of the myogenic basic helix-loop-helix regulatory factors is mediated through an indirect pathway that involves unidentified regulatory elements and/or ancillary factors.
机译:MyoD基因调节蛋白家族的成员(MyoD,myogenin,myf5和MRF4)不仅被证明可以调节许多肌肉特异性基因的转录,而且还可以积极地自动调节并交叉激活彼此的转录。在肌肉特异性基因的情况下,这种转录调节通常可以与调节区域CANNTG(称为E盒)中DNA共有序列的存在相关。关于肌源性因子本身的调节相互作用知之甚少。然而,这些相互作用被认为对于激活和维持肌肉表型很重要。我们已经确定了鸡MyoD(CMD1)启动子中的最小区域,该区域是胚胎鸡骨骼肌原代培养中肌肉特异性转录所必需的。在原代雏鸡成纤维细胞培养物中和用胸苷类似物溴脱氧尿苷处理的肌肉细胞培养物中,CMD1启动子沉默。但是,在这些初级成纤维细胞培养物中,反式表达的CMD1和鸡肌生成素,以及在较小程度上,鸡Myf5和MRF4可以激活这些初级成纤维细胞培养物中最小CMD1启动子的转录。在这里,我们显示CMD1启动子包含CMD1和其他肌原性因子的许多E-box结合位点以及MEF-2结合位点。出人意料的是,既没有肌肉特异性因子也没有其他肌原性因子,也没有MEF-2结合位点。出人意料的是,肌肉特异性表达,自动调节或交叉激活都不依赖于CMD1启动子中这些E-box或MEF-2结合位点的存在。这些结果表明,通过肌原性基本螺旋-环-螺旋调节因子的推定直接结合,鸡MyoD启动子的自动调节和交叉激活是通过涉及未知的调节因子和/或辅助因子的间接途径介导的。

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