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Messenger RNA and MicroRNA transcriptomic signatures of cardiometabolic risk factors

机译:代谢风险因素的Messenger RNA和MicroRNA转录组签名

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Background Cardiometabolic (CM) risk factors are heritable and cluster in individuals. We hypothesized that CM risk factors are associated with multiple shared and unique mRNA and microRNA (miRNA) signatures. We examined associations of mRNA and miRNA levels with 6 CM traits: body mass index, HDL-cholesterol and triglycerides, fasting glucose, and systolic and diastolic blood pressures through cross-sectional analysis of 2812 Framingham Heart Study who had whole blood collection for RNA isolation for mRNA and miRNA expression studies and who consented to genetic research. We excluded participants taking medication for hypertension, dyslipidemia, or diabetes. We measured mRNA ( n =?17,318; using the Affymetrix GeneChip Human Exon 1.0 ST Array) and miRNA ( n =?315; using qRT-PCR) expression in whole blood. We used linear regression for mRNA analyses and a combination of linear and logistic regression for miRNA analyses. We conducted miRNA-mRNA coexpression and gene ontology enrichment analyses to explore relations between pleiotropic miRNAs, mRNA expression, and CM trait clustering. Results We identified hundreds of significant associations between mRNAs, miRNAs, and individual CM traits. Four mRNAs ( FAM13A, CSF2RB, HIST1H2AC, WNK1 ) were associated with all 6 CM traits (FDR?Conclusions We identified mRNA and miRNA signatures of individual CM traits and their clustering. Implicated transcripts may play causal roles in CM risk or be downstream consequences of CM risk factors on the transcriptome. Studies are needed to establish whether or not pleiotropic circulating transcripts illuminate causal pathways for CM risk.
机译:背景心脏代谢(CM)危险因素是可遗传的并且在个体中聚集。我们假设CM危险因素与多个共享和独特的mRNA和microRNA(miRNA)签名相关。我们通过2828 Framingham心脏研究的横断面分析检查了mRNA和miRNA水平与6个CM特征的关联:体重指数,HDL-胆固醇和甘油三酸酯,空腹血糖以及收缩压和舒张压用于mRNA和miRNA表达研究以及同意进行基因研究的人员。我们排除了因高血压,血脂异常或糖尿病而服用药物的参与者。我们测量了全血中的mRNA(n =?17,318;使用Affymetrix GeneChip Human Exon 1.0 ST Array)和miRNA(n =?315;使用qRT-PCR)。我们使用线性回归进行mRNA分析,并使用线性回归和逻辑回归进行miRNA分析。我们进行了miRNA-mRNA共表达和基因本体分析,以探索多效性miRNA,mRNA表达和CM性状聚类之间的关系。结果我们鉴定了mRNA,miRNA和单个CM特性之间的数百种重要关联。四个mRNA(FAM13A,CSF2RB,HIST1H2AC,WNK1)与所有6个CM特质(FDR?)相关。转录组中的CM危险因素:需要进行研究以确定多效性循环转录本是否阐明CM危险的因果途径。

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