微小RNA结合位点的基因变异影响微小RNA介导的与心脏代谢表型相关的多个基因的调控。

Genetic Variations in MicroRNA-Binding Sites Affect MicroRNA-Mediated Regulation of Several Genes Associated With Cardio-metabolic Phenotypes.

作者信息

Ghanbari Mohsen, Franco Oscar H, de Looper Hans W J, Hofman Albert, Erkeland Stefan J, Dehghan Abbas

机构信息

From the Department of Epidemiology (M.G., O.H.F., A.H., A.D.) and Department of Hematology, Cancer Institute (H.d.L., S.E.), Erasmus University Medical Center, Rotterdam, The Netherlands; and Department of Genetics, School of Medicine, Mashhad University of Medical Sciences, Mashhad, Iran (M.G.).

出版信息

Circ Cardiovasc Genet. 2015 Jun;8(3):473-86. doi: 10.1161/CIRCGENETICS.114.000968. Epub 2015 Mar 26.

DOI:10.1161/CIRCGENETICS.114.000968

PMID:25814643

Abstract

BACKGROUND

Genome-wide association studies enabled us to discover a large number of variants and genomic loci contributing to cardiovascular and metabolic disorders. However, because the vast majority of the identified variants are thought to merely be proxies for other functional variants, the causal mechanisms remain to be elucidated. We hypothesized that the part of the functional variants involved in deregulating cardiometabolic genes is located in microRNA (miRNA)-binding sites.

METHODS AND RESULTS

Using the largest genome-wide association studies available on glycemic indices, lipid traits, anthropometric measures, blood pressure, coronary artery diseases, and type 2 diabetes mellitus, we identified 11,067 variants that are associated with cardiometabolic phenotypes. Of these, 230 variants are located within miRNA-binding sites in the 3'-untranslated region of 155 cardiometabolic genes. Thirty-seven of 230 variants were found to fulfill our predefined criteria for being functional in their genomic loci. Ten variants were subsequently selected for experimental validation based on genome-wide association studies results, expression quantitative trait loci (eQTL) analyses, and coexpression of their host genes and regulatory miRNAs in relevant tissues. Luciferase reporter assays revealed an allele-specific regulation of genes hosting the variants by miRNAs. These cotransfection experiments showed that rs174545 (FADS1:miR-181a-2), rs1059611 (LPL:miR-136), rs13702 (LPL:miR-410), rs1046875 (FN3KRP:miR-34a), rs7956 (MKRN2:miR-154), rs3217992 (CDKN2B:miR-138-2-3p), and rs11735092 (HSD17B13:miR-375) decrease or abrogate miRNA-dependent regulation of the genes. Conversely, 2 variants, rs6857 (PVRL2:miR-320e) and rs907091 (IKZF3:miR-326), were shown to enhance the activity of miRNAs on their host genes.

CONCLUSIONS

We provide evidence for a model in which polymorphisms in miRNA-binding sites can both positively and negatively affect miRNA-mediated regulation of cardiometabolic genes.

摘要

背景

全基因组关联研究使我们能够发现大量与心血管和代谢紊乱相关的变异体和基因组位点。然而，由于绝大多数已鉴定的变异体被认为仅仅是其他功能变异体的替代物，其因果机制仍有待阐明。我们推测，参与调节心脏代谢基因的部分功能变异体位于微小RNA（miRNA）结合位点。

方法与结果

利用现有的关于血糖指数、脂质性状、人体测量指标、血压、冠状动脉疾病和2型糖尿病的最大规模全基因组关联研究，我们鉴定出11,067个与心脏代谢表型相关的变异体。其中，230个变异体位于155个心脏代谢基因3'非翻译区的miRNA结合位点内。在230个变异体中，有37个被发现符合我们预先定义的在其基因组位点具有功能的标准。随后，根据全基因组关联研究结果、表达定量性状位点（eQTL）分析以及它们的宿主基因和调控miRNA在相关组织中的共表达情况，选择了10个变异体进行实验验证。荧光素酶报告基因检测揭示了miRNA对携带变异体的基因的等位基因特异性调控。这些共转染实验表明，rs174545（FADS1:miR-181a-2）、rs1059611（LPL:miR-136）、rs13702（LPL:miR-410）、rs1046875（FN3KRP:miR-34a）、rs7956（MKRN2:miR-154）、rs3217992（CDKN2B:miR-138-2-3p）和rs11735092（HSD17B13:miR-375）降低或消除了miRNA对这些基因的依赖性调控。相反，2个变异体rs6857（PVRL2:miR-320e）和rs907091（IKZF3:miR-326）被证明增强了miRNA对其宿主基因的活性。