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Genetic regulation of adipose tissue transcript expression is involved in modulating serum triglyceride and HDL-cholesterol

机译:脂肪组织转录本表达的遗传调控参与调节血清甘油三酸酯和HDL-胆固醇

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摘要

Dyslipidemia is a major contributor to the increased cardiovascular disease and mortality associated with obesity and type 2 diabetes. We hypothesized that variation in expression of adipose tissue transcripts is associated with serum lipid concentrations in African Americans (AAs), and common genetic variants regulate expression levels of these transcripts. Fasting serum lipid levels, genome-wide transcript expression profiles of subcutaneous adipose tissue, and genome-wide SNP genotypes were analyzed in a cohort of non-diabetic AAs (N=250). Serum triglyceride (TRIG) and high density lipoprotein-cholesterol (HDL-C) levels were associated (FDR<0.01) with expression level of 1021 and 1875 adipose tissue transcripts, respectively, but none associated with total cholesterol or LDL-C levels. Serum HDL-C-associated transcripts were enriched for salient biological pathways, including branched-chain amino acid degradation, and oxidative phosphorylation. Genes in immuno-inflammatory pathways were activated among individuals with higher serum TRIG levels. We identified significant cis-regulatory SNPs (cis-eSNPs) for 449 serum lipid-associated transcripts in adipose tissue. The cis-eSNPs of 12 genes were nominally associated (p<0.001) with serum lipid level in genome wide association studies in Global Lipids Genetics Consortium (GLGC) cohorts. Allelic effect direction of cis-eSNPs on expression of MARCH2, BEST1 and TMEM258 matched with effect direction of these SNP alleles on serum TRIG or HDL-C levels in GLGC cohorts. These data suggest that expressions of serum lipid-associated transcripts in adipose tissue are dependent on common cis-eSNPs in African Americans. Thus, genetically-mediated transcriptional regulation in adipose tissue may play a role in reducing HDL-C and increasing TRIG in serum.
机译:血脂异常是与肥胖症和2型糖尿病相关的心血管疾病和死亡率增加的主要原因。我们假设脂肪组织转录本表达的变化与非裔美国人(AAs)中的血清脂质浓度有关,并且常见的遗传变异调节这些转录本的表达水平。在一组非糖尿病AA(N = 250)中分析了空腹血清脂质水平,皮下脂肪组织的全基因组转录本表达谱和全基因组SNP基因型。血清甘油三酸酯(TRIG)和高密度脂蛋白胆固醇(HDL-C)水平分别与1021和1875脂肪组织转录本的表达水平相关(FDR <0.01),但与总胆固醇或LDL-C水平无关。血清HDL-C相关的转录本丰富了显着的生物途径,包括分支链氨基酸降解和氧化磷酸化。血清TRIG水平较高的个体中,免疫炎症途径的基因被激活。我们为脂肪组织中的449种与脂质相关的转录本确定了重要的顺式SNPs(cis-eSNPs)。在全球脂质遗传学联盟(GLGC)队列的全基因组关联研究中,12个基因的cis-eSNPs与血清脂质水平名义上相关(p <0.001)。顺式-eSNPs等位基因对MARCH2,BEST1和TMEM258表达的影响方向与这些SNP等位基因对GLGC人群血清TRIG或HDL-C水平的影响方向匹配。这些数据表明,脂肪组织中血清脂质相关转录物的表达依赖于非洲裔美国人常见的顺式eSNPs。因此,脂肪组织中遗传介导的转录调控可能在降低HDL-C和增加血清TRIG方面发挥作用。

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