Franks Paul W, Barroso Inês, Luan Jian'an, Ekelund Ulf, Crowley Vivion E F, Brage Søren, Sandhu Manjinder S, Jakes Rupert W, Middelberg Rita P S, Harding Anne-Helen, Schafer Alan J, O'Rahilly Stephen, Wareham Nicholas J
Institute of Public Health, University of Cambridge, United Kingdom.
Med Sci Sports Exerc. 2003 Dec;35(12):1998-2004. doi: 10.1249/01.MSS.0000099109.73351.81.
Sedentary lifestyles are increasingly common and result in low cardiorespiratory fitness ([OV0312]O2max), a well-established predictor of early mortality and coronary heart disease (CHD). Adaptation in [OV0312]O2max after exercise training varies considerably between people. Because there are hereditary components to fitness, it is likely that genetic factors explain some of this variability. PPARGC1 (PGC-1alpha) coactivates genes involved in energy transduction and mitochondrial biogenesis. Transgenic mouse data demonstrate that overexpression of PGC-1alpha mRNA increases endurance capacity by transformation of nonoxidative to oxidative skeletal muscle tissue. Other murine studies demonstrate that exercise increases PGC-1alpha mRNA expression.
To explore whether a candidate polymorphism in the PGC-1alpha gene modifies the association between physical activity energy expenditure (PAEE) and predicted [OV0312]O2max ([OV0312]O2max.pred).
We examined whether the Gly482Ser polymorphism of PGC-1alpha modified the relationship between objectively measured PAEE and [OV0312]O2max.pred in a population-based sample of 599 healthy middle-aged people. PAEE was assessed using individual calibration with 4 d of heart rate monitoring. [OV0312]O2max.pred was measured during a submaximal exercise stress test on a bicycle ergometer.
Homozygosity at the Ser482 allele was found in 12.7% of the cohort, whereas 38.9% and 48.4% carried the Gly482Gly and Gly482Ser genotypes, respectively. The association between PAEE and [OV0312]O2max.pred (mL x kg(-1) x min(-1)) was strongest in people homozygous for the Ser482 allele (beta = 12.03; P < 0.00001) compared with carriers of the Gly allele (beta = 5.61; P < 0.00001). In a recessive model for the Ser482 allele, the interaction between PAEE and genotype on [OV0312]O2max.pred (L x min(-1)) was highly significant (P = 0.009).
Our results indicate that Ser482 homozygotes may be most capable of improving cardiorespiratory fitness when physically active, and that Gly482Ser may explain some of the between-person variance previously reported in cardiorespiratory adaptation after exercise training.
久坐的生活方式越来越普遍,会导致心肺适能([OV0312]O2max)降低,而心肺适能是已明确的早期死亡率和冠心病(CHD)的预测指标。运动训练后,人们的[OV0312]O2max适应情况差异很大。由于健康状况存在遗传因素,很可能是基因因素导致了部分这种变异性。PPARGC1(PGC-1α)可共激活参与能量转导和线粒体生物合成的基因。转基因小鼠数据表明,PGC-1α mRNA的过表达通过将非氧化型骨骼肌组织转变为氧化型,从而提高耐力。其他小鼠研究表明,运动可增加PGC-1α mRNA的表达。
探讨PGC-1α基因中的一个候选多态性是否会改变体力活动能量消耗(PAEE)与预测的[OV0312]O2max([OV0312]O2max.pred)之间的关联。
我们在599名健康中年人的人群样本中,研究了PGC-1α的Gly482Ser多态性是否改变了客观测量的PAEE与[OV0312]O2max.pred之间的关系。使用4天心率监测的个体校准来评估PAEE。在自行车测力计上进行次极量运动应激测试时测量[OV0312]O2max.pred。
该队列中12.7%的人在Ser482等位基因处为纯合子,而分别有38.9%和48.4%的人携带Gly482Gly和Gly482Ser基因型。与Gly等位基因携带者相比(β = 5.61;P < 0.00001),在Ser482等位基因纯合的人群中,PAEE与[OV0312]O2max.pred(mL×kg-1×min-1)之间的关联最强(β = 12.03;P < 0.00001)。在Ser482等位基因的隐性模型中,PAEE与基因型对[OV0312]O2max.pred(L×min-1)的相互作用非常显著(P = 0.009)。
我们的结果表明,Ser482纯合子在进行体育活动时可能最有能力改善心肺适能,并且Gly482Ser可能解释了先前报道的运动训练后心肺适应中个体间差异的部分原因。
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