Biogenetic Markers for Predicting Response to Immunotherapy in Rheumatoid Arthritis

Sara H. Jabbar, K. Mohammed, N. Ali
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Abstract

Background: TNF-α plays a critical role in the pathogenesis of RA. Gene polymorphisms occurring in this pro-inflammatory cytokine or their receptors may influence responses to biological therapy. Objectives: This study aimed to evaluate the impact of -238G/A(rs361525), -308G/A(rs1800629), -376G/A(rs1800750), +489G/A(rs80267059) SNPs in TNF-α and +587T/G(rs1061622), +884A/G(rs5746032) SNPs in TNFRII genes on responsiveness to TNF inhibitors as well as their effect on serum levels of TNF-α and TNFRII. Subjects and methods: Sixty patients with RA treated with anti-TNF therapy (30 responders and 30 non-responders) were allocated to this study. SNPs in the TNF-α and TNFRII genes were studied by three different techniques: PCR-sequencing, PCR-RFLP, and q-PCR-TaqMan assay. TNF-α and TNFRII serum levels were determined using the ELISA technique. Results: TNF-α -308 (GA), +489 (GA), and TNFRII +587 (TG) genotypes were found to be more associated with non-responsiveness to TNF than homozygous genotypes (OR: 1.3, 2.5, and 2.0, respectively). On other hand, TNF-α -238 and -376 (GA) genotypes, were found to be more associated with TNFi responsiveness than homozygous genotypes (OR: 0.172 and 0.22, respectively). However, none of them reached a significant level. Furthermore, the studied SNPs were found to be unrelated to serum levels of TNF-α and TNFRII. Conclusion: According to our findings, the TNF-α -238G/A, -308G/A, -376G/A, +489G/A, and TNFRII +587T/G, +884A/G SNPs were not significantly associated with the responsiveness of RA patients to biological therapy and had no effect on the serum levels of TNF-α and TNFR.
预测类风湿关节炎免疫治疗反应的生物遗传学标志物
背景:TNF-α在RA的发病过程中起关键作用。在这种促炎细胞因子或其受体中发生的基因多态性可能影响对生物治疗的反应。目的:本研究旨在评估TNF-α基因中-238G/A(rs361525)、-308G/A(rs1800629)、-376G/A(rs1800750)、+489G/A(rs80267059) snp和TNFRII基因中+587T/G(rs1061622)、+884A/G(rss5746032) snp对TNF抑制剂反应性的影响及其对血清TNF-α和TNFRII水平的影响。对象和方法:60例接受抗tnf治疗的RA患者(30例有反应者和30例无反应者)被分配到本研究中。通过pcr -测序、PCR-RFLP和q-PCR-TaqMan三种不同的技术研究TNF-α和TNFRII基因的snp。采用ELISA技术检测血清TNF-α和TNFRII水平。结果:TNF-α -308 (GA)、+489 (GA)和TNFRII +587 (TG)基因型与TNF无应答性的相关性高于纯合子基因型(OR分别为1.3、2.5和2.0)。另一方面,TNF-α -238和-376 (GA)基因型与TNF- fi反应性的相关性高于纯合子基因型(OR分别为0.172和0.22)。然而,它们都没有达到显著水平。此外,研究发现snp与血清TNF-α和TNFRII水平无关。结论:根据我们的研究结果,TNF-α -238G/A、-308G/A、-376G/A、+489G/A和TNFRII +587T/G、+884A/G snp与RA患者对生物治疗的反应性无显著相关性,对血清TNF-α和TNFR水平无影响。
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