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激活并扩增对恶性肿瘤具有广泛特异性的多克隆γδ T细胞。

Activating and propagating polyclonal gamma delta T cells with broad specificity for malignancies.

作者信息

Deniger Drew C, Maiti Sourindra N, Mi Tiejuan, Switzer Kirsten C, Ramachandran Vijaya, Hurton Lenka V, Ang Sonny, Olivares Simon, Rabinovich Brian A, Huls M Helen, Lee Dean A, Bast Robert C, Champlin Richard E, Cooper Laurence J N

机构信息

Departments of Pediatrics, University of Texas Graduate School of Biomedical Sciences at Houston, Houston, Texas.

Departments of Pediatrics.

出版信息

Clin Cancer Res. 2014 Nov 15;20(22):5708-19. doi: 10.1158/1078-0432.CCR-13-3451. Epub 2014 May 15.

Abstract

PURPOSE

To activate and propagate populations of γδ T cells expressing polyclonal repertoire of γ and δ T-cell receptor (TCR) chains for adoptive immunotherapy of cancer, which has yet to be achieved.

EXPERIMENTAL DESIGN

Clinical-grade artificial antigen-presenting cells (aAPC) derived from K562 tumor cells were used as irradiated feeders to activate and expand human γδ T cells to clinical scale. These cells were tested for proliferation, TCR expression, memory phenotype, cytokine secretion, and tumor killing.

RESULTS

γδ T-cell proliferation was dependent upon CD137L expression on aAPC and addition of exogenous IL2 and IL21. Propagated γδ T cells were polyclonal as they expressed TRDV1, TRDV2-2, TRDV3, TRDV5, TRDV7, and TRDV8 with TRGV2, TRGV3F, TRGV7, TRGV8, TRGV9A1, TRGV10A1, and TRGV11 TCR chains. IFNγ production by Vδ1, Vδ2, and Vδ1(neg)Vδ2(neg) subsets was inhibited by pan-TCRγδ antibody when added to cocultures of polyclonal γδ T cells and tumor cell lines. Polyclonal γδ T cells killed acute and chronic leukemia, colon, pancreatic, and ovarian cancer cell lines, but not healthy autologous or allogeneic normal B cells. Blocking antibodies demonstrated that polyclonal γδ T cells mediated tumor cell lysis through combination of DNAM1, NKG2D, and TCRγδ. The adoptive transfer of activated and propagated γδ T cells expressing polyclonal versus defined Vδ TCR chains imparted a hierarchy (polyclonal>Vδ1>Vδ1(neg)Vδ2(neg)>Vδ2) of survival of mice with ovarian cancer xenografts.

CONCLUSIONS

Polyclonal γδ T cells can be activated and propagated with clinical-grade aAPCs and demonstrate broad antitumor activities, which will facilitate the implementation of γδ T-cell cancer immunotherapies in humans.

摘要

目的

激活并扩增表达γ和δ T细胞受体(TCR)链多克隆库的γδ T细胞群体,用于癌症的过继性免疫治疗,目前这一目标尚未实现。

实验设计

源自K562肿瘤细胞的临床级人工抗原呈递细胞(aAPC)用作经辐照的饲养细胞,将人γδ T细胞激活并扩增至临床规模。对这些细胞进行增殖、TCR表达、记忆表型、细胞因子分泌及肿瘤杀伤检测。

结果

γδ T细胞增殖依赖于aAPC上CD137L的表达以及外源性IL2和IL21的添加。扩增的γδ T细胞是多克隆的,因为它们表达TRDV1、TRDV2-2、TRDV3、TRDV5、TRDV7和TRDV8以及TRGV2、TRGV3F、TRGV7、TRGV8、TRGV9A1、TRGV10A1和TRGV11 TCR链。当将泛TCRγδ抗体添加到多克隆γδ T细胞与肿瘤细胞系的共培养物中时,Vδ1、Vδ2和Vδ1(neg)Vδ2(neg)亚群的IFNγ产生受到抑制。多克隆γδ T细胞可杀伤急性和慢性白血病、结肠、胰腺及卵巢癌细胞系,但不杀伤健康的自体或异体正常B细胞。阻断抗体表明,多克隆γδ T细胞通过DNAM1、NKG2D和TCRγδ的组合介导肿瘤细胞裂解。表达多克隆与特定Vδ TCR链的激活并扩增的γδ T细胞的过继性转移赋予了携带卵巢癌异种移植物的小鼠生存等级(多克隆>Vδ

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