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缺氧诱导因子 1 将快速模式化肌肉活动与大鼠的快肌表型联系起来。

Hypoxia inducible factor 1 links fast-patterned muscle activity and fast muscle phenotype in rats.

机构信息

Department of Molecular Biosciences, University of Oslo, PO Box 1041, Blindern, N-0316 Oslo, Norway.

出版信息

J Physiol. 2011 Mar 15;589(Pt 6):1443-54. doi: 10.1113/jphysiol.2010.202762. Epub 2011 Jan 24.

Abstract

Exercise influences muscle phenotype by the specific pattern of action potentials delivered to the muscle, triggering intracellular signalling pathways. PO2 can be reduced by an order of magnitude in working muscle. In humans, carriers of a hyperactive polymorphism of the transcription factor hypoxia inducible factor 1α (HIF-1α) have 50% more fast fibres, and this polymorphism is prevalent among strength athletes. We have investigated the putative role of HIF-1α in mediating activity changes in muscle.When rat muscles were stimulated with short high frequency bursts of action potentials known to induce a fast muscle phenotype, HIF-1α increased by about 80%. In contrast, a pattern consisting of long low frequency trains known to make fast muscles slow reduced the HIF-1α level of the fast extensor digitorum longus (EDL) muscle by 44%. Nuclear protein extracts from normal EDL contained 2.3-fold more HIF-1α and 4-fold more HIF-1β than the slow soleus muscle, while von-Hippel-Lindau protein was 4.8-fold higher in slow muscles. mRNA displayed a reciprocal pattern; thus FIH-1 mRNA was almost 2-fold higher in fast muscle, while the HIF-1α level was half, and consequently protein/mRNA ratio for HIF-1α was more than 4-fold higher in the fast muscle, suggesting that HIF-1α is strongly suppressed post-transcriptionally in slow muscles.When HIF-1α was overexpressed for 14 days after somatic gene transfer in adult rats, a slow-to-fast transformation was observed, encompassing an increase in fibre cross sectional area, oxidative enzyme activity and myosin heavy chain. The latter was shown to be regulated at the mRNA level in C2C12 myotubes.

摘要

运动通过传递给肌肉的动作电位的特定模式来影响肌肉表型,从而触发细胞内信号通路。在工作肌肉中,PO2 可以降低一个数量级。在人类中,转录因子缺氧诱导因子 1α(HIF-1α)的超活性多态性的携带者具有 50%更多的快肌纤维,并且这种多态性在力量运动员中很普遍。我们研究了 HIF-1α 在介导肌肉活动变化中的潜在作用。当大鼠肌肉受到已知诱导快肌表型的短高频动作电位脉冲刺激时,HIF-1α 增加了约 80%。相比之下,由长低频列车组成的模式(已知使快肌变慢)使快伸趾长肌(EDL)的 HIF-1α 水平降低了 44%。正常 EDL 的核蛋白提取物中 HIF-1α 的含量比慢肌比目鱼肌高 2.3 倍,而 HIF-1β 的含量比慢肌比目鱼肌高 4 倍,而 von-Hippel-Lindau 蛋白在慢肌中的含量高 4.8 倍。mRNA 显示出相反的模式;因此,快肌中的 FIH-1 mRNA 几乎高 2 倍,而 HIF-1α 水平减半,因此 HIF-1α 的蛋白/mRNA 比值在快肌中高 4 倍以上,表明 HIF-1α 在慢肌中受到强烈的转录后抑制。当在成年大鼠中通过体基因转移过度表达 HIF-1α 14 天后,观察到从慢到快的转变,包括纤维横截面积、氧化酶活性和肌球蛋白重链增加。在 C2C12 肌管中,发现后者在 mRNA 水平受到调节。

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