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Genetic Polymorphisms of IL-17F and TRAF3IP2 Could Be Predictive Factors of the Long-Term Effect of Infliximab against Crohn’s Disease

机译:IL-17F和TRaF3Ip2的遗传多态性可能是英夫利昔单抗对克罗恩病长期影响的预测因素

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摘要

Background. We aimed to identify certain genes related to response to infliximab (IFX) and biomarkers to predict the IFX effect for Japanese Crohn's disease (CD) patients by performing an association study of single nucleotide polymorphisms (SNPs) in candidate genes in the interleukin-(IL-) 17 signaling pathway with response to IFX after 1 year of treatment. Methods. A total of 103 patients were divided into two groups, responders and nonresponders. Twenty-eight tag SNPs in 5 genes were genotyped. The frequencies of alleles and genotypes of each SNP were compared between responders and nonresponders in three different inheritance models. A genetic test was performed using a combination of the associated SNPs as biomarkers. Results. Multivariate logistic regression analysis indicated that the four variable factors, concomitant use of immunomodulators, penetrating disease, a G/G genotype of rs766748 in IL-17F, and a C/C or C/A genotype of rs1883136 in TRAF3IP2, independently contributed to response to IFX after 1 year of treatment. Genetic test using the polymorphisms of these genes perfectly predicted the responder and nonresponder CD patients with both concomitant use of immunomodulators and penetrating disease. Conclusion. IL17F and TRAF3IP2 are one of IFX-related genes, useful as biomarkers of IFX response, and may be target molecules for new therapeutic drugs.
机译:背景。我们旨在通过对白介素-(IL)候选基因中的单核苷酸多态性(SNP)进行关联研究,确定与英夫利昔单抗(IFX)和生物标记物相关的某些基因,从而预测日本克罗恩病(CD)患者的IFX效果。 -)治疗1年后对IFX有反应的17条信号通路。方法。总共103例患者分为响应者和不响应者两组。对5个基因中的28个标签SNP进行基因分型。在三种不同的遗传模型中,比较了应答者和非应答者之间每个SNP的等位基因频率和基因型。使用相关SNP的组合作为生物标记物进行了基因测试。结果。多元逻辑回归分析表明,四个变量因素,免疫调节剂的同时使用,穿透性疾病,IL-17F中rs766748的G / G基因型和TRAF3IP2中rs1883136的C / C或C / A基因型独立影响应答治疗1年后改用IFX。使用这些基因的多态性进行的遗传测试完美地预测了反应性和非反应性CD患者同时使用免疫调节剂和穿透性疾病。结论。 IL17F和TRAF3IP2是IFX相关基因之一,可用作IFX反应的生物标志物,并且可能是新治疗药物的靶分子。

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