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人 Vδ3 γδ T 细胞诱导 B 细胞成熟和 IgM 分泌。

Human Vδ3 γδ T cells induce maturation and IgM secretion by B cells.

机构信息

Discipline of Immunology, Trinity Translational Medicine Institute, School of Medicine, Trinity College Dublin, Ireland.

Discipline of Clinical Medicine, Trinity Translational Medicine Institute, School of Medicine, Trinity College Dublin, Ireland.

出版信息

Immunol Lett. 2018 Apr;196:126-134. doi: 10.1016/j.imlet.2018.02.002. Epub 2018 Feb 10.

DOI:10.1016/j.imlet.2018.02.002
PMID:29438730
Abstract

This study tested the hypothesis that the Vδ3 subset of human γδ T cells, like their Vδ2 counterparts, can influence differentiation, antibody secretion and cytokine production by B cells. Vδ3 T cells constitute a minor subset of peripheral blood lymphocytes but are enriched in the liver and gut and are expanded in patients with cytomegalovirus activation and B cell chronic lymphocytic leukemia. They have been reported to include MHC class I and CD1d restricted cells. Like Vδ2 T cells, they are capable of maturing dendritic cells into cytokine-producing antigen presenting cells, making them potential targets for dendritic cell-based immunotherapies. Since it is unknown if Vδ3 T cells can also provide B cell help, we investigated if Vδ3 T cells can promote B cell differentiation, antibody secretion and cytokine production in vitro. Vδ3 T cells were sorted from healthy human blood and expanded using phytohemagglutinin and cultured with freshly isolated human B cells. We found that Vδ3 T cells and B cells reciprocally induced expression of maturation markers CD40, CD86 and HLA-DR but not T1, T2 or T17 cytokines. Furthermore, Vδ3 T cells promoted the release of IgM, but not IgG, IgA or IgE by B cells. These data demonstrate, for the first time, a reciprocal activating relationship between Vδ3 T cells and B cells, which could prove a useful target for cellular immunotherapy.

摘要

本研究旨在验证以下假设

与 Vδ2 型 γδ T 细胞类似,人 Vδ3 型 γδ T 细胞亚群能够影响 B 细胞的分化、抗体分泌和细胞因子产生。Vδ3 T 细胞是外周血淋巴细胞中的一个小亚群,但在肝脏和肠道中丰富,在巨细胞病毒激活和 B 细胞慢性淋巴细胞白血病患者中扩增。已有报道称其包括 MHC Ⅰ类和 CD1d 限制细胞。与 Vδ2 T 细胞一样,它们能够将树突状细胞成熟为产生细胞因子的抗原提呈细胞,使其成为基于树突状细胞的免疫疗法的潜在靶点。由于尚不清楚 Vδ3 T 细胞是否也能提供 B 细胞辅助,我们研究了 Vδ3 T 细胞是否能在体外促进 B 细胞分化、抗体分泌和细胞因子产生。我们从健康人的血液中分离出 Vδ3 T 细胞,并用植物血凝素进行扩增,并与新分离的人 B 细胞共培养。结果发现,Vδ3 T 细胞和 B 细胞相互诱导表达成熟标志物 CD40、CD86 和 HLA-DR,但不表达 T1、T2 或 T17 细胞因子。此外,Vδ3 T 细胞促进 B 细胞释放 IgM,但不促进 IgG、IgA 或 IgE 的释放。这些数据首次证明了 Vδ3 T 细胞与 B 细胞之间存在相互激活的关系,这可能成为细胞免疫治疗的一个有用靶点。

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