[Causal association between immune cells and sepsis: a based on Mendelian randomization method study].

Q3 Medicine

Zhonghua wei zhong bing ji jiu yi xue Pub Date : 2024-08-01 DOI:10.3760/cma.j.cn121430-20240527-00462

Qiushuang Yu, Lingxu Li, Yina Tao, Longqiang Zhang, Junfeng Hu, Huaxue Wang

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引用次数: 0

Abstract

Objective: To investigate the causal association between immune cell and different types of sepsis by using Mendelian randomization (MR) method, and to find the immune cell phenotypes causally associated with sepsis.

Methods: Summary data for various circulating immune cell phenotypes were obtained from the GWAS catalog (GCST90001391-GCST90002121). Sepsis data were sourced from the UK Biobank database. Single nucleotide polymorphisms (SNP) were used as instrumental variables. The correlation threshold of P < 5×10^-6 was used to identify the strongly correlated instrumental variables, and the code was used to remove the linkage disequilibrium and the instrumental variables with F-value < 10. Inverse variance weighting (IVW) was used as the main research method to evaluate the stability and reliability of the results, including Cochran's Q test, MR-Egger regression and Leave one out. Reverse MR analysis was performed based on the immunophenotypic results of the removal of horizontal pleiotropy, and the immune cell phenotype with one-way causal association was obtained. Odds ratio (OR) and 95% confidence interval (95%CI) were used to represent the effect value of the results.

Results: CD16 on CD14^-CD16⁺; monocyte had horizontal pleiotropy in sepsis (OR = 0.965 4, 95%CI was 0.933 5-0.998 3, P = 0.039 6). There were five immunophenotypes that had reverse causal associations with the types associated with sepsis. After excluding immune cell phenotypes with horizontal pleiotropy and reverse causation, a total of 42 immune cell phenotypes with sepsis, 36 immune cell phenotypes with sepsis (28-day death in critical care), 32 immune cell phenotypes with sepsis (critical care), 44 immune cell phenotypes with sepsis (28-day death), and 30 immune cell phenotypes had potential causal associations with sepsis (under 75 years old). After false discovery rate (FDR) correction, the correlations between BAFF-R on IgD^- CD38br and sepsis (28-day death) were negative and strong (OR = 0.737 8, 95%CI was 0.635 9-0.856 0, P = 6.05×10^-5, P_FDR = 0.044 2).

Conclusions: A variety of immune cell phenotypes may have a protective effect on sepsis, especially BAFF-R on IgD^- CD38br expression is negatively correlated with sepsis (28-day death), which provides a new idea for immune modulation therapy in sepsis.

查看原文本刊更多论文

[免疫细胞与败血症之间的因果关系：基于孟德尔随机法的研究]。

目的利用孟德尔随机化（MR）方法研究免疫细胞与不同类型败血症之间的因果关系，并找出与败血症有因果关系的免疫细胞表型：各种循环免疫细胞表型的汇总数据来自 GWAS 目录（GCST90001391-GCST90002121）。败血症数据来自英国生物库数据库。单核苷酸多态性（SNP）被用作工具变量。用 P < 5×10-6 的相关性阈值来识别强相关的工具变量，并用代码剔除联系不平衡和 F 值 < 10 的工具变量。以反向方差加权法（IVW）为主要研究方法，评价结果的稳定性和可靠性，包括 Cochran's Q 检验、MR-Egger 回归和留一法。根据剔除横向褶积的免疫表型结果进行反向 MR 分析，得到具有单向因果关联的免疫细胞表型。用比值比（OR）和95%置信区间（95%CI）表示结果的效应值：结果：CD14上的CD16-CD16+；单核细胞在脓毒症中具有水平多向性（OR=0.965 4，95%CI为0.933 5-0.998 3，P=0.039 6）。有五种免疫表型与败血症相关类型存在反向因果关系。在排除了具有水平褶积性和反向因果关系的免疫细胞表型后，共有42种免疫细胞表型与败血症有关，36种免疫细胞表型与败血症（重症监护中28天死亡）有关，32种免疫细胞表型与败血症（重症监护）有关，44种免疫细胞表型与败血症（28天死亡）有关，30种免疫细胞表型与败血症（75岁以下）有潜在的因果关系。经错误发现率（FDR）校正后，IgD- CD38br上的BAFF-R与脓毒症（28天死亡）呈负强相关（OR=0.737 8，95%CI为0.635 9-0.856 0，P=6.05×10-5，PFDR=0.044 2）：多种免疫细胞表型可能对脓毒症有保护作用，尤其是IgD- CD38br表达的BAFF-R与脓毒症（28天死亡）呈负相关，这为脓毒症的免疫调节治疗提供了新思路。

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

Zhonghua wei zhong bing ji jiu yi xue Medicine-Critical Care and Intensive Care Medicine

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1.00

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0.00%

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