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293碱基对β-肌球蛋白重链启动子在转基因小鼠中的肌肉特异性和诱导性表达。

Muscle-specific and inducible expression of 293-base pair beta-myosin heavy chain promoter in transgenic mice.

作者信息

Wiedenman J L, Tsika G L, Gao L, McCarthy J J, Rivera-Rivera I D, Vyas D, Sheriff-Carter K, Tsika R W

机构信息

University of Illinois, Urbana-Champaign 6180, USA.

出版信息

Am J Physiol. 1996 Sep;271(3 Pt 2):R688-95. doi: 10.1152/ajpregu.1996.271.3.R688.

Abstract

The DNA regulatory element(s) involved in beta-myosin heavy chain (beta-MHC) induction by the physiological stimulus of mechanical overload have not been identified as yet. To delineate regulatory sequences that are required for mechanical overload induction of the beta-MHC gene, transgenic mouse lines were generated that harbor transgenes containing serial deletions of the human beta-MHC promoter to nucleotides -293 (beta 293), -201 (beta 201), and -141 (beta 141) from the transcription start site (+1). Mechanically overloaded adult plantaris and soleus muscles contained 11- and 1.9-fold increases, respectively, in endogenous beta-MHC-specific mRNA transcripts (Northern blot) compared with sham-operated controls. Expression assays (chloramphenicol acetyltransferase specific activity) revealed that only transgene beta 293 expression was muscle specific in both fetal and adult mice and was induced in the plantaris (10- to 27-fold) and soleus (2- to 2.5-fold) muscles by mechanical overload. Histochemical staining for myosin adenosinetriphosphatase activity revealed a fiber-type transition of type II to type I in the overloaded plantaris and soleus muscles. These transgenic data suggest that sequences located between nucleotides -293 and +120 may be sufficient to regulate the endogenous beta-MHC gene in response to developmental signals and to the physiological signals generated by mechanical overload in fast- and slow-twitch muscles.

摘要

由机械过载的生理刺激所介导的β-肌球蛋白重链(β-MHC)诱导过程中涉及的DNA调控元件,至今尚未明确。为了描绘β-MHC基因机械过载诱导所需的调控序列,构建了转基因小鼠品系,这些品系携带的转基因包含从转录起始位点(+1)起对人β-MHC启动子进行连续缺失直至核苷酸-293(β293)、-201(β201)和-141(β141)的片段。与假手术对照组相比,机械过载的成年比目鱼肌和趾长屈肌中内源性β-MHC特异性mRNA转录本(Northern印迹法)分别增加了11倍和1.9倍。表达分析(氯霉素乙酰转移酶特异性活性)显示,只有转基因β293的表达在胎儿和成年小鼠中均具有肌肉特异性,并且在趾长屈肌(10至27倍)和比目鱼肌(2至2.5倍)中因机械过载而被诱导。肌球蛋白三磷酸腺苷酶活性的组织化学染色显示,过载的趾长屈肌和比目鱼肌中出现了从II型到I型的纤维类型转变。这些转基因数据表明,位于核苷酸-293和+120之间的序列可能足以响应发育信号以及快速和慢速收缩肌肉中机械过载产生的生理信号来调控内源性β-MHC基因。

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