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Homozygosity disequilibrium associated with treatment response and its methylation regulation

机译:与治疗反应相关的纯合不平衡及其甲基化调控

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Homozygosity disequilibrium (HD), indicating a nonrandom pattern of sizable runs of homozygosity that deviates from a random allocation of homozygous and heterozygous genotypes in the genome, is an important phenomenon in population genomics and medical genomics. We performed the first genome-wide study investigating the roles of HD in pharmacogenomics and pharmacoepigenomics by analyzing GAW20 data. We inferred whole-genome profiles of homozygosity intensities and performed genome-wide homozygosity association analyses to identify regions of HD associated with triglyceride (TG) response to fenofibrate by using LOHAS (Loss-of-Heterozygosity Analysis Suite) software. The analysis identified a region of HD contained in MACROD2 at 20p12 to be significantly associated with TG response to fenofibrate. We also examined the common genetic component in TG and methylation responses to fenofibrate. The methylation response to fenofibrate was regarded as a methylation quantitative trait, and our methylation quantitative trait locus analysis identified a cis -acting regulation association with marginal significance between the homozygosity intensity of MACROD2 and the methylation response to fenofibrate. These findings may help delineate the genetic basis of pharmacogenomic and pharmacoepigenomic responses to fenofibrate intervention.
机译:纯合子不平衡(HD),表明与基因组中纯合子和杂合子基因型的随机分配不同的纯合子相当大的运行的非随机模式,是种群基因组学和医学基因组学中的重要现象。我们进行了第一项全基因组研究,通过分析GAW20数据,研究了HD在药物基因组学和药物表观基因组学中的作用。我们推断出纯合强度的全基因组图谱,并进行了全基因组纯合性关联分析,以通过使用LOHAS(杂合性丢失分析套件)软件来识别与甘油三酸酯(TG)对非诺贝特反应的HD相关区域。该分析确定了在20p12时MACROD2中包含的HD区域与TG对非诺贝特的反应显着相关。我们还检查了TG和非诺贝特甲基化反应中常见的遗传成分。对非诺贝特的甲基化反应被视为甲基化定量性状,我们的甲基化定量性状基因座分析确定了顺式作用的调控关联,在MACROD2的纯合强度与对非诺贝特的甲基化反应之间具有边际意义。这些发现可能有助于描述非诺贝特干预药物基因组学和药物表观遗传学反应的遗传基础。

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