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人二级淋巴组织中CD20阳性和CD20阴性浆细胞的T细胞依赖性存活

T cell-dependent survival of CD20+ and CD20- plasma cells in human secondary lymphoid tissue.

作者信息

Withers David R, Fiorini Claudia, Fischer Randy T, Ettinger Rachel, Lipsky Peter E, Grammer Amrie C

机构信息

B Cell Biology Group, National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, 9000 Rockville Pike, Bethesda, MD 20892, USA

出版信息

Blood. 2007 Jun 1;109(11):4856-64. doi: 10.1182/blood-2006-08-043414. Epub 2007 Feb 13.

Abstract

The signals mediating human plasma cell survival in vivo, particularly within secondary lymphoid tissue, are unclear. Human tonsils grafted into immunodeficient mice were therefore used to delineate the mechanisms promoting the survival of plasma cells. Tonsillar plasma cells were maintained within the grafts and the majority were nonproliferating, indicating a long-lived phenotype. A significant depletion of graft plasma cells was observed after anti-CD20 treatment, consistent with the expression of CD20 by most of the cells. Moreover, anti-CD52 treatment caused the complete loss of all graft lymphocytes, including plasma cells. Unexpectedly, anti-CD3, but not anti-CD154, treatment caused the complete loss of plasma cells, indicating an essential role for T cells, but not CD40-CD154 interactions in plasma cell survival. The in vitro coculture of purified tonsillar plasma cells and T cells revealed a T-cell survival signal requiring cell contact. Furthermore, immunofluorescence studies detected a close association between human plasma cells and T cells in vivo. These data reveal that human tonsil contains long-lived plasma cells, the majority of which express CD20 and can be deleted with anti-CD20 therapy. In addition, an important role for contact-dependent interactions with T cells in human plasma cell survival within secondary lymphoid tissue was identified.

摘要

介导人类浆细胞在体内(尤其是在二级淋巴组织内)存活的信号尚不清楚。因此,将人类扁桃体移植到免疫缺陷小鼠体内,以阐明促进浆细胞存活的机制。扁桃体浆细胞在移植组织中得以维持,且大多数细胞不增殖,表明其具有长寿表型。抗CD20治疗后观察到移植组织中的浆细胞显著减少,这与大多数细胞表达CD20一致。此外,抗CD52治疗导致所有移植淋巴细胞(包括浆细胞)完全消失。出乎意料的是,抗CD3治疗而非抗CD154治疗导致浆细胞完全消失,这表明T细胞在浆细胞存活中起关键作用,而CD40 - CD154相互作用并非如此。纯化的扁桃体浆细胞与T细胞的体外共培养揭示了一种需要细胞接触的T细胞存活信号。此外,免疫荧光研究在体内检测到人类浆细胞与T细胞之间存在密切关联。这些数据表明,人类扁桃体含有长寿浆细胞,其中大多数表达CD20,可通过抗CD20疗法清除。此外,还确定了与T细胞的接触依赖性相互作用在二级淋巴组织中人类浆细胞存活中的重要作用。

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