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全表型组关联分析揭示了基因决定的肝酶水平与疾病表型之间的新联系。

Phenome-Wide Association Analysis Reveals Novel Links Between Genetically Determined Levels of Liver Enzymes and Disease Phenotypes.

作者信息

Liu Zhenqiu, Suo Chen, Jiang Yanfeng, Zhao Renjia, Zhang Tiejun, Jin Li, Chen Xingdong

机构信息

State Key Laboratory of Genetic Engineering, Human Phenome Institute, School of Life Sciences, Fudan University, Shanghai, 200438 China.

Fudan University Taizhou Institute of Health Sciences, Taizhou, 225316 China.

出版信息

Phenomics. 2022 Jan 11;2(5):295-311. doi: 10.1007/s43657-021-00033-y. eCollection 2022 Oct.

DOI:10.1007/s43657-021-00033-y
PMID:36939802
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9590558/
Abstract

UNLABELLED

Serum liver enzymes (alanine aminotransferase [ALT], aspartate aminotransferase [AST], λ-glutamyl transferase [GGT] and alkaline phosphatase [ALP]) are the leading biomarkers to measure liver injury, and they have been reported to be associated with several intrahepatic and extrahepatic diseases in observational studies. We conducted a phenome-wide association study (PheWAS) to identify disease phenotypes associated with genetically predicted liver enzymes based on the UK Biobank cohort. Univariable and multivariable Mendelian randomization (MR) analyses were performed to obtain the causal estimates of associations that detected in PheWAS. Our PheWAS identified 40 out of 1,376 pairs (16, 17, three and four pairs for ALT, AST, GGT and ALP, respectively) of genotype-phenotype associations reaching statistical significance at the 5% threshold. A total of 34 links were further validated in Mendelian randomization analyses. Most of the disease phenotypes that associated with genetically determined ALT level were liver-related, including primary liver cancer and alcoholic liver damage. The disease outcomes associated with genetically determined AST involved a wide range of phenotypic categories including endocrine/metabolic diseases, digestive diseases, and neurological disorder. Genetically predicted GGT level was associated with the risk of other chronic non-alcoholic liver disease, abnormal results of function study of liver, and cholelithiasis. Genetically determined ALP level was associated with pulmonary heart disease, phlebitis and thrombophlebitis of lower extremities, and hypercholesterolemia. Our findings reveal novel links between liver enzymes and disease phenotypes providing insights into the full understanding of the biological roles of liver enzymes.

SUPPLEMENTARY INFORMATION

The online version contains supplementary material available at 10.1007/s43657-021-00033-y.

摘要

未标注

血清肝酶(丙氨酸氨基转移酶[ALT]、天冬氨酸氨基转移酶[AST]、γ-谷氨酰转移酶[GGT]和碱性磷酸酶[ALP])是衡量肝损伤的主要生物标志物,在观察性研究中,据报道它们与多种肝内和肝外疾病有关。我们基于英国生物银行队列进行了一项全表型关联研究(PheWAS),以确定与基因预测的肝酶相关的疾病表型。进行了单变量和多变量孟德尔随机化(MR)分析,以获得在PheWAS中检测到的关联的因果估计。我们的PheWAS在1376对基因型-表型关联中确定了40对(ALT、AST、GGT和ALP分别为16、17、3和4对)在5%阈值下达到统计学显著性。在孟德尔随机化分析中进一步验证了总共34个关联。与基因决定的ALT水平相关的大多数疾病表型与肝脏相关,包括原发性肝癌和酒精性肝损伤。与基因决定的AST相关的疾病结局涉及广泛的表型类别,包括内分泌/代谢疾病、消化系统疾病和神经系统疾病。基因预测的GGT水平与其他慢性非酒精性肝病的风险、肝功能研究异常结果和胆结石有关。基因决定的ALP水平与肺心病、下肢静脉炎和血栓性静脉炎以及高胆固醇血症有关。我们的研究结果揭示了肝酶与疾病表型之间的新关联,为全面理解肝酶的生物学作用提供了见解。

补充信息

在线版本包含可在10.1007/s43657-021-00033-y获取的补充材料。

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