[Inflammatory factors and prostate cancer: Two-sample Mendelian randomization analysis].

Q4 Medicine 中华男科学杂志 Pub Date : 2024-07-01

Yin Zeng, Gan-Lin Zhang, Jun Guo, Meng-Ping Yang, Qiang Han, Guo-Wang Yang

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引用次数: 0

Abstract

Objective: To evaluate the potential causal relationship between inflammatory factors and PCa using the two-sample Mendelian randomization (MR) method.

Methods: We selected summary statistics of genome-wide association studies (GWAS) (n = 14 824) on 91 inflammatory factors, with PCa as the outcome in the latest 9th edition of FinnGen database for MR analysis. We evaluated the causal relationship between inflammatory factors and PCa using the odds ratio (OR) and 95% confidence interval (CI) of such regression models as inverse variance weighting (IVW), MR-Egger regression, simple mode (SM), weighted mode (WM) and weighted median estimator (WME), with IVW as the main statistical method for this study. We further verified the results of MR by Bayesian analysis, and evaluated the heterogeneity of genetic instrumental variables, pleiotropic effects and sensitivity of single nucleotide polymorphisms (SNP) as instrumental variables to the exposure-outcome relationship by Cochran's Q test, MR-Egger intercept test and leave-one-out cross validation.

Results: IVW showed that among the 91 inflammatory factors, interleukin-22 receptor A1 (IL-22RA1) and sulfotransferase 1A1 (ST1A1) were correlated positively with the risk of PCa； IL-22RA1：IVW（OR ［95% CI］: 1.12 ［1.00－1.25］, P = 0.04）；ST1A1：IVW（OR ［95% CI］: 1.08 (1.00－1.16), P = 0. 03）, while Chemokine ligand 11 (CXCL11) and interleukin 17 A (IL-17 A) negatively with the risk of PCa； CXCL11：IVW（OR ［95% CI］: 0.88 ［0.81－0.95］, P = 0.00）；IL-17A：IVW（OR ［95% CI］: 0.91 ［0.84－0.98］, P = 0.02）. No potential horizontal pleiotropy was detected by MR-Egger intercept analysis (P > 0.05, IL-22RA1 = 0.885, ST1A1 = 0.949, CXCL11 = 0.391, IL-17A = 0.884), nor biased SNPs in the MR pleiotropy residual sum and outlier (MR-PRESSO) test (P > 0.05, IL-22RA1 = 0.479, ST1A1 = 0.629, CXCL11 = 0.326, IL-17A = 0.444), or heterogeneity P > 0.05, IL-22RA1 = 0.543, ST1A1 = 0.677, CXCL11 = 0.336, IL-17A = 0.494). Leave-one-out sensitivity analysis indicated no significant impact of individual SNP sites on the overall causal relationship prediction, suggesting the reliable results of analysis.

Conclusion: Among the 91 inflammatory factors, IL-22RA1 and ST1A1 have a positive causal relationship, while CXCL11 and IL-17A have a negative causal relationship with PCa.

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[炎症因素与前列腺癌：双样本孟德尔随机分析]。

目的：采用双样本孟德尔随机法评估炎症因素与 PCa 之间的潜在因果关系：采用双样本孟德尔随机化（MR）方法评估炎症因素与PCa之间的潜在因果关系：我们选取了FinnGen数据库最新第9版中以PCa为结局的91个炎症因子的全基因组关联研究（GWAS）（n = 14 824）的汇总统计数据进行MR分析。我们使用反方差加权（IVW）、MR-Egger 回归、简单模式（SM）、加权模式（WM）和加权中值估计器（WME）等回归模型的比值比（OR）和 95% 置信区间（CI）评估了炎症因子与 PCa 之间的因果关系，其中 IVW 是本研究的主要统计方法。我们通过贝叶斯分析进一步验证了MR的结果，并通过Cochran's Q检验、MR-Egger截距检验和leave-one-out交叉验证评估了遗传工具变量的异质性、多向效应以及单核苷酸多态性（SNP）作为工具变量对暴露-结果关系的敏感性：IVW显示，在91个炎症因子中，白细胞介素-22受体A1（IL-22RA1）和磺基转移酶1A1（ST1A1）与PCa风险呈正相关；IL-22RA1：IVW（OR ［95% CI］：1.12 ［1.00-1.25］，P = 0.04）；ST1A1：IVW（OR ［95% CI］：03），而趋化因子配体11（CXCL11）和白细胞介素17 A（IL-17 A）与PCa的发病风险呈负相关；CXCL11：IVW（OR ［95% CI］：0.88 ［0.81-0.95］，P = 0.00）；IL-17A：IVW（OR ［95% CI］：0.91 ［0.84-0.98］, P = 0.02）.MR-Egger截距分析（P＞0.05，IL-22RA1＝0.885，ST1A1＝0.949，CXCL11＝0.391，IL-17A＝0.884）和MR-PRESSO（MR pleiotropy residual sum and outlier）检验（P＞0.05，IL-22RA1 = 0.479，ST1A1 = 0.629，CXCL11 = 0.326，IL-17A = 0.444），或异质性 P > 0.05，IL-22RA1 = 0.543，ST1A1 = 0.677，CXCL11 = 0.336，IL-17A = 0.494）。留空敏感性分析表明，单个 SNP 位点对整体因果关系预测无显著影响，表明分析结果可靠：结论：在91个炎症因子中，IL-22RA1和ST1A1与PCa存在正向因果关系，而CXCL11和IL-17A与PCa存在负向因果关系。

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

中华男科学杂志 Medicine-Medicine (all)

CiteScore

0.40

自引率

0.00%

发文量

5367

期刊介绍： National journal of andrology was founded in June 1995. It is a core journal of andrology and reproductive medicine, published monthly, and is publicly distributed at home and abroad. The main columns include expert talks, monographs (basic research, clinical research, evidence-based medicine, traditional Chinese medicine), reviews, clinical experience exchanges, case reports, etc. Priority is given to various fund-funded projects, especially the 12th Five-Year National Support Plan and the National Natural Science Foundation funded projects. This journal is included in about 20 domestic databases, including the National Science and Technology Paper Statistical Source Journal (China Science and Technology Core Journal), the Source Journal of the China Science Citation Database, the Statistical Source Journal of the China Academic Journal Comprehensive Evaluation Database (CAJCED), the Full-text Collection Journal of the China Journal Full-text Database (CJFD), the Overview of the Chinese Core Journals (2017 Edition), and the Source Journal of the Top Academic Papers of China's Fine Science and Technology Journals (F5000). It has been included in the full text of the American Chemical Abstracts, the American MEDLINE, the American EBSCO, and the database.