肠道微生物群与硬皮病:双样本双向孟德尔随机研究

Jun Hu, Jiayan Chen, Peiyan Wang, Changji Xiao, Kalibinuer Kelaimu, Xianshu Gao, Xiaomei Li
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摘要

(1) 背景:最近的研究表明,肠道微生物组(GMs)与炎症性疾病之间存在潜在联系,但GMs在扁平苔藓(LS)中的作用仍不清楚。本研究旨在调查肠道微生物组与扁平苔藓之间的因果关系,重点研究主要的肠道微生物类群。(2)方法:我们利用孟德尔随机化(MR)方法,对 211 个 GM 分类群及其与 2,445 名 LS 患者和 353,088 名健康对照的关系进行了 GWAS 统计汇总。GM 分类群的 GWAS 数据来自 MiBioGen 联盟,LS 的 GWAS 数据来自 FinnGen 联盟。主要分析工具包括反方差加权(IVW)法、加权 MR、简单模式、加权中位数和 MR-Egger 法。敏感性分析包括留一分析、MR-Egger 截距检验、MR-PRESSO 全局检验和 Cochrane Q 检验。对正向 MR 研究中发现的细菌进行了反向 MR 分析。(3)结果:我们确定了一个强因果关系:伯克霍尔德氏菌目[几率比(OR)= 0.420,95% 置信区间(CI):0.230 - 0.765,P = 0.005],以及三个名义上的显著关系:蓝藻门(OR = 0.585,95% CI:0.373 - 0.919,p = 0.020)、倍增菌类(OR = 0.403,95% CI:0.189 - 0.857,p = 0.018)和丁弧菌属(OR = 0.678,95% CI:0.507 - 0.907,p = 0.009)。此外,根据 MR-Egger 截距检验和 MR-PRESSO 全局检验(p > 0.05),该 MR 分析未受水平多效性的影响。值得注意的是,我们的结果的可靠性得到了撇除分析的证实。反向 MR 分析表明 LS 与 GM 之间没有明显的因果关系。(4) 结论:这项磁共振研究确定了与降低 LS 风险相关的特定肠道菌群,为疾病的治疗和预防提供了新的见解。未来的研究应结合元基因组学对广泛的微生物组 GWAS 数据集进行测序。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Gut microbiome and lichen sclerosus: a two-sample bi-directional Mendelian randomization study
(1) Background: Recent studies suggest a potential link between gut microbiomes (GMs) and inflammatory diseases, but the role of GMs in lichen sclerosus (LS) remains unclear. This study aims to investigate the causal relationship between GMs and LS, focusing on key GM taxa. (2) Methods: We utilized GWAS summary statistics for 211 GM taxa and their association with 2,445 LS patients and 353,088 healthy controls, employing Mendelian randomization (MR). GWAS data for GM taxa came from the MiBioGen consortium, and for LS from the FinnGen consortium. The primary analytical tools included the inverse-variance weighted (IVW) method, weighted MR, simple mode, weighted median, and MR-Egger methods. Sensitivity analyses included leave-one-out analysis, MR-Egger intercept test, MR-PRESSO global test, and Cochrane's Q-test. A reverse MR analysis was conducted on bacteria identified in the forward MR study. (3) Results: We identified one strong causal relationship: order Burkholderiales [odds ratio (OR) = 0.420, 95% confidence interval (CI): 0.230 - 0.765, p = 0.005], and three nominally significant relationships: phylum Cyanobacteria (OR = 0.585, 95% CI: 0.373 - 0.919, p = 0.020), class Betaproteobacteria (OR = 0.403, 95% CI: 0.189 - 0.857, p = 0.018), and genus Butyrivibrio (OR = 0.678, 95% CI: 0.507 - 0.907, p = 0.009). Moreover, this MR analysis was not impacted by horizontal pleiotropy, according to the MR-Egger intercept test and MR-PRESSO global test (p > 0.05). Remarkably, the reliability of our results was confirmed by leave-one-out analysis. Reverse MR analysis showed no significant causal relationship between LS and GM. (4) Conclusions: This MR study identifies specific gut flora linked to a lower risk of LS, offering new insights for disease treatment and prevention. Future research should incorporate metagenomics sequencing of extensive microbiome GWAS datasets.
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