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在正常小鼠和狼疮易感小鼠中,一种新型的B-1细胞亚群富含自身反应性。

A novel subpopulation of B-1 cells is enriched with autoreactivity in normal and lupus-prone mice.

作者信息

Zhong Xuemei, Lau Stanley, Bai Chunyan, Degauque Nicolas, Holodick Nichol E, Steven Scott J, Tumang Joseph, Gao Wenda, Rothstein Thomas L

机构信息

Boston University Medical Center, Boston, Massachusetts 02118, USA.

出版信息

Arthritis Rheum. 2009 Dec;60(12):3734-43. doi: 10.1002/art.25015.

Abstract

OBJECTIVE

B-1 cells have long been suggested to play an important role in lupus. However, reports to date have been controversial regarding their pathogenic or protective roles in different animal models. We undertook this study to investigate a novel subpopulation of B-1 cells and its roles in murine lupus.

METHODS

Lymphocyte phenotypes were assessed by flow cytometry. Autoantibody secretion was analyzed by enzyme-linked immunosorbent assay, autoantigen proteome array, and antinuclear antibody assay. Cell proliferation was measured by thymidine incorporation and 5,6-carboxyfluorescein succinimidyl ester dilution. B cell Ig isotype switching was measured by enzyme-linked immunospot assay.

RESULTS

Anti-double-stranded DNA (anti-dsDNA) autoantibodies were preferentially secreted by a subpopulation of CD5+ B-1 cells that expressed programmed death ligand 2 (termed L2pB1 cells). A substantial proportion of hybridoma clones generated from L2pB1 cells reacted to dsDNA. Moreover, these clones were highly cross-reactive with other lupus-related autoantigens. L2pB1 cells were potent antigen-presenting cells and promoted Th17 cell differentiation in vitro. A dramatic increase of circulating L2pB1 cells in lupus-prone BXSB mice was correlated with elevated serum titers of anti-dsDNA antibodies. A significant number of L2pB1 cells preferentially switched to IgG1 and IgG2b when stimulated with interleukin-21.

CONCLUSION

Our findings identify a novel subpopulation of B-1 cells that is enriched for autoreactive specificities, undergoes isotype switch, manifests enhanced antigen presentation, promotes Th17 cell differentiation, and is preferentially associated with the development of lupus in a murine model. Together, these findings suggest that L2pB1 cells have the potential to initiate autoimmunity through serologic and T cell-mediated mechanisms.

摘要

目的

长期以来,人们认为B-1细胞在狼疮中起重要作用。然而,迄今为止,关于它们在不同动物模型中的致病或保护作用的报道一直存在争议。我们进行这项研究以调查B-1细胞的一个新亚群及其在小鼠狼疮中的作用。

方法

通过流式细胞术评估淋巴细胞表型。通过酶联免疫吸附测定、自身抗原蛋白质组芯片和抗核抗体测定分析自身抗体分泌。通过胸苷掺入和5,6-羧基荧光素琥珀酰亚胺酯稀释测量细胞增殖。通过酶联免疫斑点测定测量B细胞Ig同种型转换。

结果

抗双链DNA(抗dsDNA)自身抗体优先由表达程序性死亡配体2的CD5+B-1细胞亚群(称为L2pB1细胞)分泌。从L2pB1细胞产生的大量杂交瘤克隆与dsDNA反应。此外,这些克隆与其他狼疮相关自身抗原有高度交叉反应性。L2pB1细胞是有效的抗原呈递细胞,并在体外促进Th17细胞分化。狼疮易感BXSB小鼠循环L2pB1细胞的显著增加与抗dsDNA抗体的血清滴度升高相关。当用白细胞介素-21刺激时,大量L2pB1细胞优先转换为IgG1和IgG2b。

结论

我们的研究结果确定了一个新的B-1细胞亚群,其富含自身反应性特异性,经历同种型转换,表现出增强的抗原呈递,促进Th17细胞分化,并且在小鼠模型中优先与狼疮的发展相关。总之,这些发现表明L2pB1细胞有可能通过血清学和T细胞介导的机制引发自身免疫。

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