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白细胞介素 23 受体多态性与类风湿关节炎易感性的关联:一项更新的荟萃分析和试验序贯分析。

Association of Interleukin 23 Receptor Polymorphisms with Predisposition to Rheumatoid Arthritis: An Updated Meta and Trial Sequential Analysis.

机构信息

ImmGen EvSys Lab, Department of Biotechnology, Berhampur University, Bhanja Bihar, Berhampur, Odisha, 760007, India.

Centre of Excellence on Bioprospecting of "Ethnopharmaceuticals of Southern Odisha" (CoE-BESO), Berhampur University, Bhanja Bihar, Berhampur, Odisha, 760007, India.

出版信息

Biochem Genet. 2024 Oct;62(5):4067-4086. doi: 10.1007/s10528-023-10644-x. Epub 2024 Jan 25.

Abstract

The etiology of Rheumatoid Arthritis (RA) development remained unclear, and several factors, such as environmental, genetic, and immune system dysfunction, have been attributed to the susceptibility. Interleukin 23 (IL23) induces expansion of the Th17 cells through the IL-23 receptor (IL-23R) and believes in playing a major role in RA pathogenesis. Various genetic mutants in the IL23R gene (rs10489629, rs1343151, rs2201841, rs7517847, rs1004819, rs10889677, rs11209026, rs7530511) have been associated with the susceptibility RA, but results are contradictories. We performed a meta-analysis to establish the association of IL23R polymorphisms with susceptibility RA. For the meta-analysis, a detailed search of databases like Google Scholar, PubMed, Scopus, Web of Science, and Science Direct was conducted, and data were extracted from the included reports. The meta-analysis was performed by the Comprehensive Meta-Analysis v3 software. A significant association of IL-23R rs11209026 (AA vs. GG: Odds ratio = 2.250, p-value = 0.01; AA vs. GG+GA: Odds ratio = 2.271, p-value = 0.01), rs1343151 (A vs. G: Odds ratio = 1.091, p-value = 0.001; AA vs. GG: Odds ratio = 1.209, p-value = 0.001; GA vs. GG: Odds ratio = 1.116, p-value = 0.004; AA+GA vs. GG: Odds ratio = 1.135, p-value = 0.000; AA vs. GG+GA: Odds ratio = 1.144, p-value = 0.012) and rs10889677 (CA vs. CC: Odds ratio = 1.375, p-value = 0.041) polymorphisms were observed with increased susceptibility for the development of RA. In contrast, IL-23R rs10489629 (G vs. A: odds ratio = 0.901, p-value = 0.047, GG vs. AA: Odds ratio = 0.763, p-value = 0.022, GG vs. AA+AG: Odds ratio = 0.852, p-value = 0.00) and IL23R rs2201841 (CC vs. TT+TC: Odds ratio = 0.826, p-value = 0.026) variants were linked with protection against the development of RA. In addition, the trial sequential analysis revealed the inclusion of a sufficient number of studies in the present meta-analysis, and no further additional studies are required. IL-23R variants are associated with genetic susceptibility or resistance against the development of RA.

摘要

类风湿关节炎(RA)发病的病因学仍不清楚,许多因素,如环境、遗传和免疫系统功能障碍,都与易感性有关。白细胞介素 23(IL23)通过白细胞介素 23 受体(IL-23R)诱导 Th17 细胞的扩增,并被认为在 RA 发病机制中起主要作用。IL23R 基因中的各种遗传突变体(rs10489629、rs1343151、rs2201841、rs7517847、rs1004819、rs10889677、rs11209026、rs7530511)与 RA 的易感性有关,但结果存在矛盾。我们进行了一项荟萃分析,以确定 IL23R 多态性与 RA 易感性的关系。为了进行荟萃分析,我们详细搜索了 Google Scholar、PubMed、Scopus、Web of Science 和 Science Direct 等数据库,并从纳入的报告中提取数据。荟萃分析由 Comprehensive Meta-Analysis v3 软件进行。IL-23R rs11209026(AA 与 GG:优势比=2.250,p 值=0.01;AA 与 GG+GA:优势比=2.271,p 值=0.01)、rs1343151(A 与 G:优势比=1.091,p 值=0.001;AA 与 GG:优势比=1.209,p 值=0.001;GA 与 GG:优势比=1.116,p 值=0.004;AA+GA 与 GG:优势比=1.135,p 值=0.000;AA 与 GG+GA:优势比=1.144,p 值=0.012)和 rs10889677(CA 与 CC:优势比=1.375,p 值=0.041)多态性与 RA 发病的易感性增加有关。相比之下,IL-23R rs10489629(G 与 A:优势比=0.901,p 值=0.047,GG 与 AA:优势比=0.763,p 值=0.022,GG 与 AA+AG:优势比=0.852,p 值=0.00)和 IL23R rs2201841(CC 与 TT+TC:优势比=0.826,p 值=0.026)变体与 RA 发病的保护有关。此外,试验序贯分析表明,目前的荟萃分析中包含了足够数量的研究,不需要进一步的额外研究。IL-23R 变体与 RA 发病的遗传易感性或抗性有关。

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