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转化生长因子-β增强Vδ2 T细胞的细胞毒性活性。

TGF-β enhances the cytotoxic activity of Vδ2 T cells.

作者信息

Peters Christian, Meyer Annika, Kouakanou Léonce, Feder Julia, Schricker Tim, Lettau Marcus, Janssen Ottmar, Wesch Daniela, Kabelitz Dieter

机构信息

Institute of Immunology, Christian-Albrechts University of Kiel, Kiel, Germany.

出版信息

Oncoimmunology. 2018 Sep 26;8(1):e1522471. doi: 10.1080/2162402X.2018.1522471. eCollection 2019.

Abstract

TGF-β is a pleiotropic cytokine with multiple roles in immunity. Apart from its suppressive activity, TGF-β is a driving cytokine in the differentiation of induced regulatory T cells (iTreg) but also in the polarization of interleukin-9 (IL-9) producing T helper 9 (Th9) T cells. Human Vδ2 expressing γδ T cells exert potent cytotoxicity towards a variety of solid tumor and leukemia/lymphoma target cells and thus are in the focus of current strategies to develop cell-based immunotherapies. Here we report that TGF-β unexpectedly augments the cytotoxic effector activity of short-term expanded Vδ2 T cells when purified γδ T cells are activated with specific pyrophosphate antigens and IL-2 or IL-15 in the presence of TGF-β. TGF-β up-regulates the expression of CD54, CD103, interferon-γ, IL-9 and granzyme B in γδ T cells while CD56 and CD11a/CD18 are down-regulated. Moreover, we show that CD103 (αE/β7 integrin) is recruited to the immunological synapse in γδ T cells. Increased cytotoxic activity of TGF-β-exposed γδ T cells is reduced by anti-CD103 and further diminished upon additional anti-CD11a antibody treatment, pointing to a role of cellular adhesion in the enhanced cytolytic activity. Furthermore, magnetically sorted CD103-positive Vδ2 T cells exhibit superior cytolytic activity. In view of the importance of CD103 for tissue homing of lymphocytes, our results suggest that adoptive transfer of CD103-expressing Vδ2 T cells might favor their homing to solid tumors.

摘要

转化生长因子-β(TGF-β)是一种多效性细胞因子,在免疫中发挥多种作用。除了其抑制活性外,TGF-β还是诱导调节性T细胞(iTreg)分化以及产生白细胞介素-9(IL-9)的辅助性T细胞9(Th9)极化过程中的驱动性细胞因子。表达人Vδ2的γδT细胞对多种实体瘤和白血病/淋巴瘤靶细胞具有强大的细胞毒性,因此是当前基于细胞的免疫治疗策略的重点。在此我们报告,当在TGF-β存在的情况下,用特定焦磷酸抗原以及IL-2或IL-15激活纯化的γδT细胞时,TGF-β出人意料地增强了短期扩增的Vδ2T细胞的细胞毒性效应活性。TGF-β上调γδT细胞中CD54、CD103、干扰素-γ、IL-9和颗粒酶B的表达,而CD56和CD11a/CD18表达下调。此外,我们表明CD103(αE/β7整合素)被招募到γδT细胞的免疫突触中。抗CD103可降低TGF-β处理的γδT细胞增强的细胞毒性活性,而额外的抗CD11a抗体处理后细胞毒性进一步减弱,这表明细胞黏附在增强的细胞溶解活性中起作用。此外,磁性分选的CD103阳性Vδ2T细胞表现出更强的细胞溶解活性。鉴于CD103对淋巴细胞组织归巢的重要性,我们的结果表明,过继转移表达CD103的Vδ2T细胞可能有利于它们归巢到实体瘤。

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