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MHC IIB基因内的一个E框与肌分化因子结合,是快肌中基因表达所必需的。

An E-box within the MHC IIB gene is bound by MyoD and is required for gene expression in fast muscle.

作者信息

Wheeler M T, Snyder E C, Patterson M N, Swoap S J

机构信息

Department of Biology, Williams College, Williamstown, Massachusetts 01267, USA.

出版信息

Am J Physiol. 1999 May;276(5):C1069-78. doi: 10.1152/ajpcell.1999.276.5.C1069.

Abstract

The myosin heavy chain (MHC) IIB gene is selectively expressed in skeletal muscles, imparting fast contractile kinetics. Why the MHC IIB gene product is expressed in muscles like the tibialis anterior (TA) and not expressed in muscles like the soleus is currently unclear. It is shown here that the mutation of an E-box within the MHC IIB promoter decreased reporter gene activity in the fast-twitch TA muscle 90-fold as compared with the wild-type promoter. Reporter gene expression within the TA required this E-box for activation of a heterologous construct containing upstream regulatory regions of the MHC IIB promoter linked to the basal 70-kDa heat shock protein TATA promoter. Electrophoretic mobility shift assays demonstrated that mutation of the E-box prevented the binding of both MyoD and myogenin to this element. In cotransfected C2C12 myotubes and Hep G2 cells, MyoD preferentially activated the MHC IIB promoter in an E-box-dependent manner, whereas myogenin activated the MHC IIB promoter to a lesser extent, and in an E-box-independent manner. A time course analysis of hindlimb suspension demonstrated that the unweighted soleus muscle activated expression of MyoD mRNA before the de novo expression of MHC IIB mRNA. These data suggest a possible causative role for MyoD in the observed upregulation of MHC IIB in the unweighted soleus muscle.

摘要

肌球蛋白重链(MHC)IIB基因在骨骼肌中选择性表达,赋予快速收缩动力学特性。目前尚不清楚为什么MHC IIB基因产物在诸如胫前肌(TA)这样的肌肉中表达,而在比目鱼肌等肌肉中不表达。本文表明,与野生型启动子相比,MHC IIB启动子内一个E盒的突变使快速收缩的TA肌中报告基因活性降低了90倍。TA肌内的报告基因表达需要这个E盒来激活一个异源构建体,该构建体包含与基础70 kDa热休克蛋白TATA启动子相连的MHC IIB启动子上游调控区。电泳迁移率变动分析表明,E盒的突变阻止了MyoD和肌细胞生成素与该元件的结合。在共转染的C2C12肌管和Hep G2细胞中,MyoD以E盒依赖的方式优先激活MHC IIB启动子,而肌细胞生成素激活MHC IIB启动子的程度较小,且以E盒非依赖的方式激活。后肢悬吊的时间进程分析表明,未负重的比目鱼肌在MHC IIB mRNA从头表达之前就激活了MyoD mRNA的表达。这些数据表明MyoD在未负重比目鱼肌中观察到的MHC IIB上调中可能起因果作用。

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