Potential causal association between gut microbiota, inflammatory cytokines, and acute pancreatitis: A Mendelian randomization study

Journal of intensive medicine Pub Date : 2024-12-10 DOI:10.1016/j.jointm.2024.10.004

Xiaofeng Wang , Yiwen Qiu , Ying Di , Hou Shaohua , Wei Wu , Weiyi Wang , Huan Liu , Pu Li

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Abstract

Background

Acute pancreatitis (AP) ranks among the most frequently encountered gastrointestinal diseases in the emergency department. Recent studies have increasingly emphasized the substantial connection among gut microbiota, inflammatory cytokines, and AP.

Methods

A two-sample Mendelian randomization (MR) study was conducted using summary statistics of gut microbiota (GM) from the largest available meta-analysis of genome-wide association studies conducted by the MiBioGen consortium (n=18,340). For cytokines, the data were obtained from a study that investigated genome variant associations with 41 inflammatory cytokines and growth factors (n=8293). The summary statistics of AP were obtained from the FinnGen consortium version R5 data (3022 cases and 195,144 controls). The inverse variance weighted (IVW) method was used as the main analysis, with MR–Egger and weighted median as complementary analytical methods. Sensitivity analyses were performed using Cochran's Q-test, MR–Egger intercept test, leave-one-out analyses, and MR–PRESSO. In addition, we employed the reverse MR analysis and MR Steiger method to estimate the orientations of exposure and outcome.

Result

Among the 211 examined GM taxa, the IVW method revealed that Bacteroidales (odds ratio [OR]=1.412, 95% confidence interval [CI]:1.057 to 1.885, P=0.019), Eubacterium fissicatena group (OR=1.240, 95% CI:1.045 to 1.470, P=0.014), and Coprococcus3 (OR=1.481, 95 % CI:1.049 to 2.090, P=0.026) exhibited a positive association with AP. Conversely, Prevotella9 (OR=0.821, 95% CI:0.680 to 0.990, P=0.038), RuminococcaceaeUCG004 (OR=0.757, 95% CI:0.577 to 0.994, P=0.045), and Ruminiclostridium6 (OR=0.696, 95% CI:0.548 to 0.884, P=0.003) displayed a negative correlation with AP. Among the 41 inflammatory cytokines, only macrophage colony-stimulating factor (M_CSF, OR=0.894, 95% CI:0.847 to 0.943, P=0.037) exhibited a negative association with AP. Sensitivity analyses revealed no evidence of pleiotropy or heterogeneity. Nevertheless, the mediation analysis showed that M_CSF did not act as a mediating factor.

Conclusion

This two-sample MR study revealed causal associations between specific GM and inflammatory cytokines with AP, respectively. However, inflammatory cytokines did not appear to act as mediating factors in the pathway from GM to AP.

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肠道菌群、炎症细胞因子和急性胰腺炎之间的潜在因果关系：一项孟德尔随机研究

背景急性胰腺炎（AP）是急诊科最常见的胃肠道疾病之一。最近的研究越来越强调肠道微生物群、炎症细胞因子和ap之间的重要联系。方法采用一项双样本孟德尔随机化（MR）研究，利用MiBioGen联盟进行的全基因组关联研究的最大荟萃分析（n=18,340）中肠道微生物群（GM）的汇总统计数据进行研究。对于细胞因子，数据来自一项研究，该研究调查了基因组变异与41种炎症细胞因子和生长因子（n=8293）的关联。AP的汇总统计数据来自FinnGen consortium version R5数据（3022例，195144例对照）。以方差反加权（IVW）法为主要分析方法，MR-Egger法和加权中位数法为辅助分析方法。采用Cochran’s q检验、MR-Egger截距检验、留一分析和MR-PRESSO进行敏感性分析。此外，我们采用反向磁共振分析和MR Steiger方法来估计暴露方向和结果。结果在211个转基因分类群中，IVW方法显示拟杆菌（优势比[OR]=1.412, 95%可信区间[CI]:1.057 ~ 1.885， P=0.019）、裂裂真杆菌组（OR=1.240, 95% CI:1.045 ~ 1.470， P=0.014）和Coprococcus3组（OR=1.481, 95% CI:1.049 ~ 2.090， P=0.026）与AP呈正相关。相反，Prevotella9组（OR=0.821, 95% CI:0.680 ~ 0.990， P=0.038）、RuminococcaceaeUCG004组（OR=0.757, 95% CI:0.577 ~ 0.994， P=0.045）与AP呈正相关。和Ruminiclostridium6 （OR=0.696, 95% CI:0.548 ~ 0.884， P=0.003）与AP呈负相关。在41种炎症因子中，只有巨噬细胞集落刺激因子（M_CSF， OR=0.894, 95% CI:0.847 ~ 0.943， P=0.037）与AP呈负相关。敏感性分析未发现多效性或异质性的证据。然而，中介分析表明M_CSF不作为中介因素。这项两样本的MR研究分别揭示了特异性GM和炎症细胞因子与AP之间的因果关系。然而，在从GM到AP的过程中，炎症细胞因子似乎并没有作为介导因子。

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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