Genetic variation in severe cystic fibrosis liver disease is associated with novel mechanisms for disease pathogenesis.

IF 12.9 1区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Hepatology Pub Date : 2024-11-01 Epub Date: 2024-03-27 DOI:10.1097/HEP.0000000000000863

Jaclyn R Stonebraker, Rhonda G Pace, Paul J Gallins, Hong Dang, Melis A Aksit, Anna V Faino, William W Gordon, Sonya MacParland, Michael J Bamshad, Ronald L Gibson, Garry R Cutting, Peter R Durie, Fred A Wright, Yi-Hui Zhou, Scott M Blackman, Wanda K O'Neal, Simon C Ling, Michael R Knowles

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Abstract

Background and aims: It is not known why severe cystic fibrosis (CF) liver disease (CFLD) with portal hypertension occurs in only ~7% of people with CF. We aimed to identify genetic modifiers for severe CFLD to improve understanding of disease mechanisms.

Approach and results: Whole-genome sequencing was available in 4082 people with CF with pancreatic insufficiency (n = 516 with severe CFLD; n = 3566 without CFLD). We tested ~15.9 million single nucleotide polymorphisms (SNPs) for association with severe CFLD versus no-CFLD, using pre-modulator clinical phenotypes including (1) genetic variant ( SERPINA1 ; Z allele) previously associated with severe CFLD; (2) candidate SNPs (n = 205) associated with non-CF liver diseases; (3) genome-wide association study of common/rare SNPs; (4) transcriptome-wide association; and (5) gene-level and pathway analyses. The Z allele was significantly associated with severe CFLD ( p = 1.1 × 10 -4 ). No significant candidate SNPs were identified. A genome-wide association study identified genome-wide significant SNPs in 2 loci and 2 suggestive loci. These 4 loci contained genes [significant, PKD1 ( p = 8.05 × 10 -10 ) and FNBP1 ( p = 4.74 × 10 -9 ); suggestive, DUSP6 ( p = 1.51 × 10 -7 ) and ANKUB1 ( p = 4.69 × 10 -7 )] relevant to severe CFLD pathophysiology. The transcriptome-wide association identified 3 genes [ CXCR1 ( p = 1.01 × 10 -6 ) , AAMP ( p = 1.07 × 10 -6 ), and TRBV24 ( p = 1.23 × 10 -5 )] involved in hepatic inflammation and innate immunity. Gene-ranked analyses identified pathways enriched in genes linked to multiple liver pathologies.

Conclusion: These results identify loci/genes associated with severe CFLD that point to disease mechanisms involving hepatic fibrosis, inflammation, innate immune function, vascular pathology, intracellular signaling, actin cytoskeleton and tight junction integrity and mechanisms of hepatic steatosis and insulin resistance. These discoveries will facilitate mechanistic studies and the development of therapeutics for severe CFLD.

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严重囊性纤维化肝病的基因变异与疾病发病的新机制有关。

背景和目的：目前尚不清楚为什么只有约 7% 的囊性纤维化肝病（CF）患者会出现严重的囊性纤维化肝病（CFLD）并伴有门脉高压。我们的目标是确定严重囊性纤维化肝病的遗传修饰因子，以加深对疾病机制的了解：我们对 4082 名胰腺功能不全的 CF 患者进行了全基因组测序（516 人患有重度 CFLD；3566 人未患有 CFLD）。我们测试了约 1590 万个 SNPs 与重度 CFLD 和无 CFLD 的相关性，使用的前调节器临床表型包括1）以前与严重 CFLD 相关的基因变异（SERPINA1；Z-等位基因）；2）与非 CFLD 肝病相关的候选 SNPs（n=205）；3）常见/罕见 SNPs 的全基因组关联研究（GWAS）；4）全转录组关联研究（TWAS）；5）基因水平和通路分析。Z-等位基因与严重 CFLD 显著相关（p=1.1×10-4）。没有发现重要的候选 SNP。GWAS 在 2 个基因位点和 2 个提示性基因位点中发现了全基因组范围的重要 SNPs。这4个位点包含与严重CFLD病理生理学相关的基因[显性基因，PKD1（p=8.05×10-10）和FNBP1（p=4.74×10-9）；提示性基因，DUSP6（p=1.51×10-7）和ANKUB1（p=4.69×10-7）]。TWAS发现了3个参与肝脏炎症和先天免疫的基因[CXCR1（p=1.01×10-6）、AAMP（p=1.07×10-6）和TRBV24（p=1.23×10-5）]。基因排序分析确定了与多种肝脏病变相关的基因所富集的通路：这些结果确定了与重度 CFLD 相关的基因位点/基因，它们指向涉及肝纤维化、炎症和先天性免疫功能、血管病理学、细胞内信号传导、肌动蛋白细胞骨架和紧密连接完整性以及肝脂肪变性和胰岛素抵抗机制的疾病机制。这些发现将促进机理研究和严重 CFLD 治疗药物的开发。

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

Hepatology 医学-胃肠肝病学

CiteScore

27.50

自引率

3.70%

发文量

609

审稿时长

1 months

期刊介绍： HEPATOLOGY is recognized as the leading publication in the field of liver disease. It features original, peer-reviewed articles covering various aspects of liver structure, function, and disease. The journal's distinguished Editorial Board carefully selects the best articles each month, focusing on topics including immunology, chronic hepatitis, viral hepatitis, cirrhosis, genetic and metabolic liver diseases, liver cancer, and drug metabolism.