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人类不变自然杀伤 T 细胞亚群体外差异促进 B 细胞的分化、抗体产生和 T 细胞刺激。

Human invariant NKT cell subsets differentially promote differentiation, antibody production, and T cell stimulation by B cells in vitro.

机构信息

Department of Immunology, School of Medicine, Trinity College Dublin, Dublin 8, Ireland.

出版信息

J Immunol. 2013 Aug 15;191(4):1666-76. doi: 10.4049/jimmunol.1202223. Epub 2013 Jul 12.

DOI:10.4049/jimmunol.1202223
PMID:23851681
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4201948/
Abstract

Invariant NK T (iNKT) cells can provide help for B cell activation and Ab production. Because B cells are also capable of cytokine production, Ag presentation, and T cell activation, we hypothesized that iNKT cells will also influence these activities. Furthermore, subsets of iNKT cells based on CD4 and CD8 expression that have distinct functional activities may differentially affect B cell functions. We investigated the effects of coculturing expanded human CD4(+), CD8α(+), and CD4(-)CD8α(-) double-negative (DN) iNKT cells with autologous peripheral B cells in vitro. All iNKT cell subsets induced IgM, IgA, and IgG release by B cells without needing the iNKT cell agonist ligand α-galactosylceramide. Additionally, CD4(+) iNKT cells induced expansions of cells with phenotypes of regulatory B cells. When cocultured with α-galactosylceramide-pulsed B cells, CD4(+) and DN iNKT cells secreted Th1 and Th2 cytokines but at 10-1000-fold lower levels than when cultured with dendritic cells. CD4(+) iNKT cells reciprocally induced IL-4 and IL-10 production by B cells. DN iNKT cells expressed the cytotoxic degranulation marker CD107a upon exposure to B cells. Remarkably, whereas iNKT cell subsets could induce CD40 and CD86 expression by B cells, iNKT cell-matured B cells were unable to drive proliferation of autologous and alloreactive conventional T cells, as seen with B cells cultured in the absence of iNKT cells. Therefore, human CD4(+), CD8α(+), and DN iNKT cells can differentially promote and regulate the induction of Ab and T cell responses by B cells.

摘要

不变自然杀伤 T(iNKT)细胞可以为 B 细胞激活和 Ab 产生提供帮助。由于 B 细胞也能够产生细胞因子、抗原呈递和 T 细胞激活,我们假设 iNKT 细胞也会影响这些活动。此外,基于 CD4 和 CD8 表达的 iNKT 细胞亚群具有不同的功能活性,可能会对 B 细胞功能产生不同的影响。我们研究了体外共培养扩增的人 CD4(+)、CD8α(+)和 CD4(-)CD8α(-)双阴性(DN)iNKT 细胞与自体外周 B 细胞的影响。所有 iNKT 细胞亚群在不需要 iNKT 细胞激动剂配体 α-半乳糖神经酰胺的情况下诱导 B 细胞释放 IgM、IgA 和 IgG。此外,CD4(+)iNKT 细胞诱导具有调节性 B 细胞表型的细胞扩增。当与 α-半乳糖神经酰胺脉冲 B 细胞共培养时,CD4(+)和 DN iNKT 细胞分泌 Th1 和 Th2 细胞因子,但水平比与树突状细胞共培养时低 10-1000 倍。CD4(+)iNKT 细胞通过 B 细胞反式诱导 IL-4 和 IL-10 产生。DN iNKT 细胞在暴露于 B 细胞时表达细胞毒性脱颗粒标记物 CD107a。值得注意的是,尽管 iNKT 细胞亚群可以诱导 B 细胞表达 CD40 和 CD86,但 iNKT 细胞成熟的 B 细胞无法驱动自体和同种异体反应性常规 T 细胞的增殖,就像在没有 iNKT 细胞的情况下培养 B 细胞一样。因此,人 CD4(+)、CD8α(+)和 DN iNKT 细胞可以差异化地促进和调节 B 细胞诱导的 Ab 和 T 细胞反应。

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