Interpreting elevated liver blood test results through a genetic lens: A genome-wide association study

IF 6 2区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Liver International Pub Date : 2024-10-19 DOI:10.1111/liv.16114

Hamish Innes, Stephan Buch, Timothy J. Kendall, Jonathan A. Fallowfield, Indra Neil Guha

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Abstract

Background and Aims

Individuals with genetic polymorphisms in UGT1A1 exhibit bilirubin levels that belie their risk of liver disease (Gilbert's syndrome) but it is not known if this phenomenon extends to other common liver blood tests (LBTs).

Methods

A genome-wide association analysis of 10 LBTs was conducted using the UK biobank. Polygenic scores (PGS) were created from discordant loci (e.g. loci associated with the LBT but not associated with cirrhosis morbidity risk). Participants were assigned to a low, intermediate or high PGS for each LBT. A high PGS approximates Gilbert's syndrome (i.e. elevated LBT without an analogous increase in disease risk). The prognostic significance of an ‘elevated’ LBT—and how this differs by PGS—was assessed through competing risk survival analysis.

Results

This study included 157 005 and 166 871 participants for the discovery and validation phases, respectively. Elevated LBTs were more prevalent in the high versus low PGS group, yet the 10-year risk of cirrhosis morbidity was comparable. For example, in the low PGS group, 4.3% had an elevated gamma-glutamyltransferase (GGT) and the 10-year risk of cirrhosis morbidity was .45%. Conversely, in the high PGS group, 21.2% had an elevated GGT and the 10-year risk was .38%. Accordingly, the 10-year risk of cirrhosis morbidity for individuals with an elevated GGT was markedly different in the low vs. high group (4.2% vs. 1.2%; p < .001). Similar results were apparent for Fibrosis-4 index, total bilirubin, and platelet count.

Conclusion

Variability in LBTs is influenced by genetic polymorphisms that have a neutral effect on disease risk. These findings have implications for interpreting elevated LBTs in clinical practice.

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从基因角度解读肝脏血液检测结果升高：全基因组关联研究

背景和目的：具有 UGT1A1 基因多态性的个体表现出的胆红素水平掩盖了他们罹患肝病（吉尔伯特综合征）的风险，但这种现象是否会延伸到其他常见的肝脏血液检测项目（LBTs）中尚不清楚：方法：利用英国生物库对 10 种 LBT 进行了全基因组关联分析。多基因评分（PGS）由不一致的基因位点（如与 LBT 相关但与肝硬化发病风险无关的基因位点）创建。参与者被分配到每个 LBT 的低、中或高 PGS。高 PGS 近似于 Gilbert's 综合征（即 LBT 升高，但疾病风险没有相应增加）。通过竞争风险生存分析评估了LBT "升高 "的预后意义以及PGS的不同：这项研究在发现和验证阶段分别纳入了 157 005 和 166 871 名参与者。高 PGS 组和低 PGS 组的 LBT 升高率更高，但 10 年肝硬化发病风险相当。例如，在低 PGS 组中，4.3% 的人γ-谷氨酰转移酶（GGT）升高，10 年肝硬化发病风险为 0.45%。相反，在高 PGS 组中，21.2% 的人 GGT 升高，10 年风险为 0.38%。因此，GGT 升高者的 10 年肝硬化发病风险在低 PGS 组和高 PGS 组之间存在明显差异（4.2% 对 1.2%；P 结论：低 PGS 组和高 PGS 组的肝硬化发病风险存在明显差异（4.2% 对 1.2%）：LBTs的变异性受遗传多态性的影响，而遗传多态性对疾病风险的影响是中性的。这些发现对在临床实践中解释升高的 LBTs 有一定意义。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Liver International 医学-胃肠肝病学

CiteScore

13.90

自引率

4.50%

发文量

348

审稿时长

2 months

期刊介绍： Liver International promotes all aspects of the science of hepatology from basic research to applied clinical studies. Providing an international forum for the publication of high-quality original research in hepatology, it is an essential resource for everyone working on normal and abnormal structure and function in the liver and its constituent cells, including clinicians and basic scientists involved in the multi-disciplinary field of hepatology. The journal welcomes articles from all fields of hepatology, which may be published as original articles, brief definitive reports, reviews, mini-reviews, images in hepatology and letters to the Editor.