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Brain-derived neurotrophic factor, epigenetics in stroke skeletal muscle, and exercise training

机译:脑衍生的神经营养因子,中风骨骼肌表观症,以及运动训练

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Objective (1) To compare paretic (P) vs nonparetic (NP) skeletal muscle brain-derived neurotrophic factor (BDNF) and the effects of resistive training (RT) on systemic and skeletal muscle BDNF mRNA expression in stroke; and (2) to compare the DNA methylation profile for BDNF and BDNFAS (BDNF antisense RNA) between P and NP muscle and the effects of aerobic exercise training (AEX) on DNA methylation in stroke. Methods In this longitudinal investigation, participants (50–76 years) with chronic stroke underwent a fasting blood draw, a 12-week (3×/week) RT intervention (n = 16), and repeated bilateral vastus lateralis muscle tissue biopsies (n = 10) with BDNF expression determined by RT-PCR. Five stroke survivors completed 6 months of AEX (3×/week) and had bilateral muscle biopsies. DNA methylation status in gene BDNF and BDNFAS was assessed by Illumina 450k methylation array. Results P muscle had ~45% lower BDNF mRNA expression than NP muscle (6.79 ± 1.30 vs 10.52 ± 2.06 arbitrary units [AU], p 0.05), and P muscle exhibited differential methylation status in the DNA sequences of BDNF (3 CpG [5′-C-phosphate-G-3′] sites, p = 0.016–0.044) and BDNFAS (1 CpG site, p = 0.016) compared to NP. Plasma BDNF and muscle BDNF messenger RNA (mRNA) expression did not significantly change after RT. BDNFAS DNA methylation increased after AEX in P relative to NP muscle ( p = 0.017). Conclusions This is the first evidence that stroke hemiparesis reduces BDNF skeletal muscle expression, with our findings identifying methylation alterations on the DNA sequence of BDNF and BDNFAS gene. Preliminary results further indicate that AEX increases methylation in BDNFAS gene, which presumably could regulate the expression of BDNF.
机译:目的(1)比较瘫痪(p)腹肌脑源脑衍生的神经营养因子(bdnf)以及电阻训练(RT)对卒中中骨骼肌BDNF mRNA表达的影响; (2)将PDNF和BDNFAS(BDNF反义RNA)的DNA甲基化谱与P和NP肌肉之间的DNA甲基化分布和有氧运动运动训练(AEX)的影响进行比较,对中风中的DNA甲基化。该方法在这种纵向调查中,参与者(50-76岁)与慢性中风进行禁食血液绘制,为12周(3×/周)RT干预(n = 16),并重复双侧覆盖侧肌组织活组织检查(n = 10)通过RT-PCR测定BDNF表达。五次中风幸存者完成了6个月的AEX(3×/周),并且具有双侧肌肉活组织检查。 Illumina 450K甲基化阵列评估基因BDNF和BDNFA中的DNA甲基化状态。结果P肌肉比NP肌肉(6.79±1.30 Vs 10.52±1.30 vs10.52±1.30)和P肌肉在BDNF的DNA序列中表现出差分甲基化状态(3.79±1.30 vs 10.52±1.30)和P肌肉(3 cpg [与NP相比,5'-C-磷酸磷-13']位点,P = 0.016-0.044)和BDNFA(1个CPG位点,P = 0.016)。血浆BDNF和肌肉BDNF信使RNA(mRNA)表达在RT后没有显着变化。 BDNFAS DNA甲基化相对于NP肌肉(P = 0.017)在P中的AEX后增加。结论这是卒中偏瘫的第一种证据减少了BDNF骨骼肌表达,同时我们的研究结果确定了BDNF和BDNFA基因的DNA序列上的甲基化改变。初步结果进一步表明AEX在BDNFA基因中增加了甲基化,这可能是可以调节BDNF的表达。

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