Sex hormone pathway gene polymorphisms are associated with risk of advanced hepatitis C-related liver disease in males.

International journal of molecular epidemiology and genetics Pub Date : 2014-10-22 eCollection Date: 2014-01-01
Donna L White, Yanhong Liu, Jose Garcia, Hashem B El-Serag, Li Jiao, Spiridon Tsavachidis, Luis M Franco, Ju-Seog Lee, Shahriar Tavakoli-Tabasi, David Moore, Radoslav Goldman, Jill Kuzniarek, David J Ramsey, Fasiha Kanwal, Marco Marcelli
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Abstract

Background: Males have excess advanced liver disease and cirrhosis risk including from chronic hepatitis C virus (HCV) infection though the reasons are unclear.

Goal: To examine the role variants in genes involved in androgen and estrogen biosynthesis and metabolism play in HCV-related liver disease risk in males.

Methods: We performed a cross-sectional study evaluating single nucleotide polymorphisms (SNPs) in 16 candidate genes involved in androgen and estrogen ligand and receptor synthesis and risk of advanced hepatic fibrosis (F3/F4-F4) and inflammation (A2/A3-A3). We calculated adjusted odds ratios (ORs) using logistic regression and used multifactor dimensionality reduction (MDR) analysis to assess for gene-environment interaction.

Results: Among 466 chronically HCV-infected males, 59% (n = 274) had advanced fibrosis and 54% (n = 252) had advanced inflammation. Nine of 472 SNPs were significantly associated with fibrosis risk; 4 in AKR1C3 (e.g., AKR1C3 rs2186174: ORadj = 2.04, 95% CI 1.38-3.02), 1 each in AKR1C2 and ESR1, and 1 in HSD17B6. Four SNPs were associated with inflammation risk, 2 in SRD5A1 (e.g., SRD5A1 rs248800: ORadj = 1.86, 95% CI 1.20-2.88) and 1 each in AKR1C2 and AKR1C3. MDR analysis identified a single AKR1C3 locus (rs2186174) as the best model for advanced fibrosis; while a 4-locus model with diabetes, AKR1C2 rs12414884, SRD5A1 rs6555406, and SRD5A1 rs248800 was best for inflammation.

Conclusions: The consistency of our findings suggests AKR1C isoenzymes 2 and 3, and potentially SRD5A1, may play a role in progression of HCV-related liver disease in males. Future studies are needed to validate these findings and to assess if similar associations exist in females.

性激素通路基因多态性与男性罹患晚期丙型肝炎相关肝病的风险有关。
背景:目标:研究参与雄激素和雌激素生物合成和代谢的基因变异在男性HCV相关肝病风险中的作用:我们进行了一项横断面研究,评估了参与雄激素和雌激素配体及受体合成的16个候选基因中的单核苷酸多态性(SNPs)与晚期肝纤维化(F3/F4-F4)和炎症(A2/A3-A3)风险的关系。我们使用逻辑回归计算了调整后的几率比(ORs),并使用多因素降维(MDR)分析评估了基因与环境的交互作用:在466名长期感染HCV的男性中,59%(n = 274)为晚期纤维化,54%(n = 252)为晚期炎症。472 个 SNPs 中有 9 个与纤维化风险显著相关;其中 4 个在 AKR1C3 中(如 AKR1C3 rs2186174:ORadj = 2.04,95% CI 1.38-3.02),AKR1C2 和 ESR1 中各有 1 个,HSD17B6 中有 1 个。4 个 SNP 与炎症风险相关,其中 2 个在 SRD5A1 中(如 SRD5A1 rs248800:ORadj = 1.86,95% CI 1.20-2.88),AKR1C2 和 AKR1C3 中各有 1 个。MDR分析发现,单个AKR1C3位点(rs2186174)是晚期纤维化的最佳模型;而包含糖尿病、AKR1C2 rs12414884、SRD5A1 rs6555406和SRD5A1 rs248800的4位点模型是炎症的最佳模型:我们研究结果的一致性表明,AKR1C同工酶2和3以及SRD5A1可能在男性HCV相关肝病的进展中发挥作用。未来的研究需要验证这些发现,并评估女性是否也存在类似的关联。
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