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TFH1 细胞失衡在系统性硬化症中异常 B 细胞分化中起作用。

Imbalance toward TFH 1 cells playing a role in aberrant B cell differentiation in systemic sclerosis.

机构信息

Department of Dermatology, Kansai Medical University, Hirakata, Japan.

Department of Dermatology and Venereology, University of Medicine and Pharmacy at Ho Chi Minh City, Ho Chi Minh, Vietnam, Japan.

出版信息

Rheumatology (Oxford). 2021 Mar 2;60(3):1553-1562. doi: 10.1093/rheumatology/keaa669.

DOI:10.1093/rheumatology/keaa669
PMID:33175976
Abstract

OBJECTIVE

SSc is a connective tissue disease with multisystem disorder induced by the inflammation and fibrosis following T and B cell abnormalities. Follicular helper CD4+ T (TFH) cells play a crucial role in the formation of germinal centres and specialize in interacting to aid B cell differentiation. We aimed to investigate TFH cells and their subsets to evaluate their involvement with B cell alteration in SSc.

METHOD

Circulating TFH cells (cTFH), B cells and their subsets were assessed by flow cytometry. The concentration of serum cytokines was measured by cytokine array assay. Immunohistochemistry and IF were performed to evaluate the migration of TFH cells in SSc skin lesions.

RESULTS

The proportion of cTFH cells did not differ from controls, but their subsets were imbalanced in SSc patients. The frequency of TFH 1 was increased and correlated with ACA titre, serum IgM or CRP levels of patients, and cytokine concentrations of IL-21 and IL-6 that induce B cell differentiation in SSc. cTFH cells from SSc showed activated phenotype with expressing higher cytokine levels compared with controls. The frequency of TFH 17 was also increased, but was not correlated with a high level of Th17 cytokines in patients' sera. Furthermore, infiltration of TFH cells was found in skin lesion of SSc patients.

CONCLUSION

We here describe an imbalance of cTFH toward TFH 1 that may induce B cell alteration through IL-21 and IL-6 pathways and promote inflammation, contributing to the pathogenesis of SSc disease.

摘要

目的

SSc 是一种结缔组织疾病,由 T 和 B 细胞异常引起的炎症和纤维化导致多系统紊乱。滤泡辅助性 CD4+T(TFH)细胞在生发中心的形成中起着至关重要的作用,专门与 B 细胞分化相互作用。我们旨在研究 TFH 细胞及其亚群,以评估它们在 SSc 中与 B 细胞改变的关系。

方法

通过流式细胞术评估循环 TFH 细胞(cTFH)、B 细胞及其亚群。通过细胞因子阵列测定法测量血清细胞因子的浓度。进行免疫组织化学和 IF 以评估 TFH 细胞在 SSc 皮肤病变中的迁移。

结果

cTFH 细胞的比例与对照组无差异,但 SSc 患者的亚群失衡。TFH1 的频率增加,并与 ACA 滴度、患者的血清 IgM 或 CRP 水平以及诱导 SSc 中 B 细胞分化的细胞因子 IL-21 和 IL-6 的浓度相关。与对照组相比,来自 SSc 的 cTFH 细胞表现出激活表型,表达更高水平的细胞因子。TFH17 的频率也增加,但与患者血清中高水平的 Th17 细胞因子无关。此外,还发现 TFH 细胞浸润在 SSc 患者的皮肤病变中。

结论

我们在这里描述了 cTFH 向 TFH1 的不平衡,这可能通过 IL-21 和 IL-6 途径诱导 B 细胞改变,并促进炎症,导致 SSc 疾病的发病机制。

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