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The Beta-adrenergic agonist, Ractopamine, increases skeletal muscle expression of Asparagine Synthetase as part of an integrated stress response gene program

机译:β-肾上腺素能激动剂莱克多巴胺可增加天冬酰胺合成酶的骨骼肌表达,这是整合应激反应基因程序的一部分

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Synthetic beta-adrenergic agonists (BA) have broad biomedical and agricultural application for increasing lean body mass, yet a poor understanding of the biology underpinning these agents is limiting further drug discovery potential. Growing female pigs (77?±?7?kg) were administered the BA, Ractopamine (20?ppm in feed), or the recombinant growth hormone (GH), Reporcin (10?mg/48?hrs injected) for 1, 3, 7, 13 (n?=?10 per treatment, per time point) or 27 days (n?=?15 per treatment). Using RNA-sequencing and inferred pathway analysis, we examined temporal changes to the Longissimus Dorsi skeletal muscle transcriptome (n?=?3 per treatment, per time point) relative to a feed-only control cohort. Gene expression changes were affirmed by quantitative-PCR on all samples (n?=?164). RNA-sequencing analysis revealed that BA treatment had greater effects than GH, and that asparagine synthetase (Asns) was the 5th most significantly increased gene by BA at day 3. ASNS protein expression was dramatically increased by BA treatment at day 7 (p??0.05). The most significantly increased gene at day 3 was activating transcription factor 5 (Atf5), a transcription factor known to regulate ASNS gene expression. Gene and protein expression of Atf4, another known regulator of Asns expression, was not changed by BA treatment. Expression of more than 20 known Atf4 target genes were increased by BA treatment, suggesting that BA treatment induces an integrated stress response (ISR) in skeletal muscle of pigs. In support of this, mRNA expression of sestrin-2 (Sesn2) and cyclin-dependant kinase 1 alpha (Cdkn1a), two key stress-responsive genes and negative regulators of cellular growth, were also strongly increased from day 3 of BA treatment. Finally, tRNA charging was the most significantly enriched pathway induced by BA treatment, suggesting alterations to the translational capacity/efficiency of the muscle. BA-mediated changes to the skeletal muscle transcriptome are highly indicative of an integrated stress response (ISR), particularly genes relating to amino acid biosynthesis and protein translational capacity.
机译:合成的β-肾上腺素能激动剂(BA)具有广泛的生物医学和农业应用,可增加瘦体重,但是对这些因子基础的生物学认识不足,限制了进一步的药物发现潜力。在生长中的雌猪(77?±?7?kg)中,给予BA,莱克多巴胺(饲料中20?ppm)或重组生长激素(GH),Reporcin(注射10?mg / 48?hrs)1、3 ,7、13(每个时间点每个治疗n = 10)或27天(每个治疗n = 15)。使用RNA测序和推断的通路分析,我们检查了Longissimus Dorsi骨骼肌转录组相对于仅进食对照组的时间变化(n = 3,每次治疗,每个时间点)。通过定量PCR在所有样品上证实了基因表达的变化(n≥164)。 RNA测序分析显示,BA处理比GH效果更好,并且天冬酰胺合成酶(Asns)是第3天BA显着增加的基因第五高的基因。第7天,BA处理显着增加了ASNS蛋白表达(p?< 0.05)。在第3天,最明显增加的基因是激活转录因子5(Atf5),这是一种已知可调节ASNS基因表达的转录因子。 Atf4的基因和蛋白质表达(另一种已知的Asns表达调节剂)不会因BA处理而改变。 BA处理可增加20多种已知Atf4靶基因的表达,这表明BA处理可诱导猪骨骼肌中的综合应激反应(ISR)。支持这一点的是,从BA处理的第3天起,两个关键的应激反应基因和细胞生长的负调节剂——sestrin-2(Sesn2)和细胞周期蛋白依赖性激酶1 alpha(Cdkn1a)的mRNA表达也大大增加。最后,tRNA充电是BA处理诱导的最丰富的途径,表明肌肉的翻译能力/效率发生了改变。 BA介导的骨骼肌转录组的变化高度指示了整合的应激反应(ISR),特别是与氨基酸生物合成和蛋白质翻译能力有关的基因。

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