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首页> 外文期刊>American Journal of Physiology >Regulation of androgen receptor expression at the onset of functional overload in rat plantaris muscle.
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Regulation of androgen receptor expression at the onset of functional overload in rat plantaris muscle.

机译:大鼠足底肌肉功能超负荷发作时雄激素受体表达的调节。

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Skeletal muscle androgen receptor (AR) expression at the onset of functional overload (OV) has not been well described. It is also not known if overload and/or anabolic steroid differentially regulate AR expression. The purpose of this study was to examine AR gene expression at the onset of functional OV in rat plantaris muscle with and without nandrolone decanoate (ND) administration. The functional significance of AR protein induction was examined using skeletal alpha-actin promoter activity in transiently transfected CV-1 fibroblast cells. Male Sprague-Dawley rats ( approximately 125 g) were functionally overloaded for 1, 3, 7, or 21 days. A subset of animals was given an ND (6 mg/kg) injection at day 0 and then overloaded for 3 days. Control animals underwent sham surgeries. AR protein concentration increased 106 and 279% after 7 and 21 days of OV, respectively. AR mRNA increased 430% after 7 days of OV. AR protein expression in C2C12 murine myotubes subjected to 1% chronic radial stretch for 18 h was elevated 101% compared with control. ND treatment increased AR protein concentration 1,300% compared with controls, and there was no additional effect when ND and OV were combined. ND with 3 days of OV treatment increased AR mRNA expression 50% compared with control. AR overexpression in transiently transfected CV-1 fibroblast cells increased -424 bp skeletal alpha-actin promoter activity 80 to 1,800% in a dose-dependent fashion. Co-overexpression of either serum response factor (SRF) or active RhoA with AR overexpression induced a synergistic 36- and 28-fold induction of skeletal alpha-actin promoter. Cotransfection of AR, SRF, and active RhoA induced 180-fold increase in skeletal alpha-actin promoter activity. In conclusion, AR protein expression is increased after 7 days of functional OV, and this induction is regulated pretranslationally. AR induction in conjunction with SRF and RhoA signaling may be an important regulator of gene expression during overload-induced muscle growth.
机译:功能超负荷(OV)发作时骨骼肌雄激素受体(AR)的表达尚未得到很好的描述。还不清楚超负荷和/或合成代谢类固醇是否差异调节AR表达。这项研究的目的是检查大鼠plant肌在服用和不服用癸酸诺龙(ND)时功能性OV发病时AR基因的表达。在瞬时转染的CV-1成纤维细胞中,使用骨骼肌α-肌动蛋白启动子活性检测AR蛋白诱导的功能意义。雄性Sprague-Dawley大鼠(约125 g)在功能上超负荷1、3、7或21天。在第0天给一部分动物进行ND(6 mg / kg)注射,然后超负荷3天。对照动物进行假手术。 OV 7天和21天后,AR蛋白浓度分别增加106%和279%。 OV 7天后,AR mRNA增加了430%。与对照组相比,经过1%慢性放射状拉伸18 h的C2C12鼠肌管中的AR蛋白表达提高了101%。与对照组相比,ND处理使AR蛋白浓度增加了1300%,并且将ND和OV合并使用时没有其他作用。 OV处理3天的ND与对照组相比,AR mRNA表达增加了50%。在瞬时转染的CV-1成纤维细胞中,AR的过度表达以剂量依赖的方式使-424 bp的骨骼肌α-肌动蛋白启动子活性增加80至1800%。血清反应因子(SRF)或活性RhoA与AR过表达的共过表达诱导骨骼肌α-肌动蛋白启动子的36倍和28倍协同诱导。 AR,SRF和活性RhoA的共转染诱导骨骼肌α-肌动蛋白启动子活性增加180倍。总之,功能性OV 7天后AR蛋白表达增加,并且该诱导在翻译前受到调节。 AR诱导与SRF和RhoA信号结合可能是超负荷诱导的肌肉生长过程中基因表达的重要调节剂。

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