髓源性抑制细胞作为新生物制剂治疗轴性脊柱炎有效性的生物标志物

T. Tyrinova, A. Morenkova, A. V. Fedorova, M. Tikhonova, N. Ilina, O. Chumasova, A. Sizikov
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引用次数: 0

摘要

先天免疫细胞,包括髓细胞-髓源性抑制细胞(MDSCs),被认为在轴性脊柱性关节炎(AxSp)的发病机制中起重要作用。髓系来源的抑制细胞代表了一种异质的未成熟细胞群,能够抑制先天和适应性免疫反应,对T细胞具有最明显的抑制活性。生物疾病调节抗风湿药物(bDMARDs)可以降低临床和实验室疾病活动,但其效果在不同的AxSp患者中差异很大。本研究旨在研究MDSCs亚群及其在AxSp中对bDMARD治疗反应的抑制功能。该研究纳入病程为16.5年(中位数)的AxSp患者;在79%的病例中检测到HLA-B27(+)状态。所有患者至少在过去12周内接受了bdmard治疗,包括TNF抑制剂(依那西普、certolizumab pegol、阿达木单抗或golimumab)或IL-17抑制剂(secukinumab、ixekizumab或netakimab)。流式细胞术检测粒细胞MDSCs (G-MDSCs, Lin-HLA-DR-CD33+CD66b+)、单核细胞MDSCs (M-MDSCs, HLA-DRlow/- cd14 +)、早期分化MDSCs (E-MDSCs, Lin-HLA-DR-CD33+CD66b -)的百分比以及细胞内精氨酸酶-1的表达。与健康供者相比,对bdmard有稳定反应的患者(应答者)循环MDSC亚群的频率没有显著差异。与健康供体(pU = 0.01和pU = 0.02)和应答者(pU = 0.03和pU = 0.07)相比,bDMARDs治疗无应答的患者E-MDSCs的相对和绝对数量均有所增加。E-MDSCs百分比增加与疾病活动性- ESR呈正相关(Rs = 0.821;p = 0.023), CRP (Rs = 0.714;p = 0.07)和ASDASCRP (Rs = 0.829;P = 0.042)。有反应的患者没有表现出疾病活动性和循环MDSCs之间的相关性。通过细胞内参与抑制T细胞反应的精氨酸酶-1分子的表达分析MDSCs的抑制潜能。与供体相比,反应稳定的患者E-MDSCs中精氨酸酶-1的表达增加(pU = 0.02)。无应答者Arg-1表达无显著变化,但表达精氨酸酶-1的G-MDSCs百分比与ASDASESR指标呈正相关(Rs = 0.857;p = 0.014)和BASDAI (Rs = 0.785;P = 0.036)。因此,E-MDSCs以及MDSCs中的精氨酸酶-1表达可能作为bDMARD治疗有效性的生物标志物,并作为AxSp治疗反应的潜在候选预测因子。
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Myeloid-derived suppressor cells as biomarkers of the effectiveness of therapy with new biological agents in axial spondyloarthritis
Innate immune cells, including myeloid cells — myeloid derived suppressor cells (MDSCs) — are supposed to play an important role in the pathogenesis of axial spondyloarthritis (AxSp). Myeloid derived suppressor cells represent a heterogeneous population of immature cells capable of suppressing innate and adaptive immune responses with the most pronounced suppressor activity against T cells. Biological disease-modifying antirheumatic drugs (bDMARDs) can reduce the clinical and laboratory disease activity, but their effectiveness varies widely in different patients with AxSp. The present study is aimed at studying MDSCs subpopulations and their suppressive function depending on the response to bDMARD therapy in AxSp. The study included AxSp patients with a disease duration of 16.5 years (median); HLA-B27 (+) status was detected in 79% of cases. All patients received bDMARDs at least the past 12 weeks, including TNF inhibitors (etanercept, certolizumab pegol, adalimumab, or golimumab) or IL-17 inhibitors (secukinumab, ixekizumab, or netakimab). Percentage of granulocytic MDSCs (G-MDSCs, Lin-HLA-DR-CD33+CD66b+), monocytic MDSCs (M-MDSCs, HLA-DRlow/-CD14+), MDSCs of early stage differentiation (E-MDSCs, Lin-HLA-DR- CD33+CD66b-), as well as intracellular expression of arginase-1 was assessed by flow cytometry. Frequency of circulating MDSC subpopulations of patients with a stable response to bDMARDs (responders) did not differ significantly compared to healthy donors. Patients not responding to bDMARDs therapy showed increased relative and absolute number of E-MDSCs compared to healthy donors (pU = 0.01 and pU = 0.02, respectively) and the responders (pU = 0.03 and pU = 0.07, respectively). Increased percentage of E-MDSCs was positively correlated to disease activity — ESR (Rs = 0.821; p = 0.023), CRP (Rs = 0.714; p = 0.07) and ASDASCRP (Rs = 0.829; p = 0.042) in the non-responder group. Responder patients exhibited no correlation between disease activity and circulating MDSCs. The suppressor potential of MDSCs was analyzed by the intracellular expression of arginase-1 molecule which is involved in the inhibition of T cell response. Patients with the stable response were characterized by increased expression of arginase-1 in E-MDSCs compared to donors (pU = 0.02). Non-responders did not demonstrate significant changes in Arg-1 expression, however, the percentage of arginase-1-expressing G-MDSCs was positively correlated to indexes ASDASESR (Rs = 0.857; p = 0.014) and BASDAI (Rs = 0.785; p = 0.036). Thus, E-MDSCs as well as arginase-1 expression in MDSCs may serve as biomarkers of effectiveness bDMARD therapy, and act as potential candidate predictors of response to therapy in AxSp.
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来源期刊
Medical Immunology (Russia)
Medical Immunology (Russia) Medicine-Immunology and Allergy
CiteScore
0.70
自引率
0.00%
发文量
88
审稿时长
12 weeks
期刊介绍: The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.
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