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首页> 外文期刊>Journal of applied physiology >Exploring the underlying biology of intrinsic cardiorespiratory fitness through integrative analysis of genomic variants and muscle gene expression profiling
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Exploring the underlying biology of intrinsic cardiorespiratory fitness through integrative analysis of genomic variants and muscle gene expression profiling

机译:通过基因组变体和肌肉基因表达分析的整合分析探索固有内在心肺健康的潜在生物学

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摘要

Intrinsic cardiorespiratory fitness (CRF) is defined as the level of CRF in the sedentary state. There are large individual differences in intrinsic CRF among sedentary adults. The physiology of variability in CRF has received much attention, but little is known about the genetic and molecular mechanisms that impact intrinsic CRF. These issues were explored in the present study by interrogating intrinsic CRF-associated DNA sequence variation and skeletal muscle gene expression data from the HERITAGE Family Study through an integrative bioinformatics guided approach. A combined analytic strategy involving genetic association, pathway enrichment, tissue-specific network structure, cis-regulatory genome effects, and expression quantitative trait loci was used to select and rank genes through a variation-adjusted weighted ranking scheme. Prioritized genes were further interrogated for corroborative evidence from knockout mouse phenotypes and relevant physiological traits from the HERITAGE cohort. The mean intrinsic (V)over dotO(2max) was 33.1 ml O-2.kg(-1).min(-1) (SD = 8.8) for the sample of 493 sedentary adults. Suggestive evidence was found for gene loci related to cardiovascular physiology (ATE1, CASQ2, NOTO, and SGCG), hematopoiesis (PICALM, SSB, CA9, and CASQ2), skeletal muscle phenotypes (SGCG, DMRT2, ADARB1, and CASQ2), and metabolism (ATE1, PICALM, RAB11FIP5, GBA2, SGCG, PRADC1, ARL6IP5, and CASQ2). Supportive evidence for a role of several of these loci was uncovered via association between DNA variants and muscle gene expression levels with exercise cardiovascular and muscle physiological traits. This initial effort to define the underlying molecular substrates of intrinsic CRF warrants further studies based on appropriate cohorts and study designs. complemented by functional investigations.
机译:固有内在的心肺刺激健身(CRF)定义为久坐状态下的CRF水平。久坐成年人中的内在CRF存在大的个体差异。 CRF在CRF中变异性的生理学受到了很大的关注,但对于影响内在CRF的遗传和分子机制很少。通过通过综合生物信息学的引导方法询问来自遗产家庭研究的内在CRF相关的DNA序列变异和骨骼肌基因表达数据,在本研究中探讨了这些问题。涉及遗传结合,途径富集,组织特异性网络结构,顺式调节基因组效应和表达定量性状基因座的组合分析策略用于通过变化调整的加权排名方案来选择和排列基因。进一步询问优先的基因,用于来自淘汰鼠标表型和来自遗产队队的相关生理性状的证据。在493个久坐体成人的样品中,Doto(2max)上的平均内在(v)为33.1ml O 2。kg(-1).min(-1)(sd = 8.8)。发现有关心血管生理学(ATE1,CASQ2,NOTO和SGCG)的基因基因座的提示证据,血液缺陷(PICALM,SSB,CA9和CASQ2),骨骼肌表型(SGCG,DMRT2,ADARB1和CASQ2)和代谢(ATE1,PICALM,RAB11FIP5,GBA2,SGCG,PRADC1,ARL6IP5和CASQ2)。通过锻炼心血管和肌肉生理特性,通过DNA变体和肌肉基因表达水平之间的关联发现了几个这些基因座的作用的支持证据。这种初步努力定义内在CRF的底层分子底物权证根据适当的队列和研究设计进一步研究。通过功能调查补充。

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