Human γδ T cells induce CD8+ T cell antitumor responses via antigen-presenting effect through HSP90-MyD88-mediated activation of JNK

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作者
Shengdong Wang
Hengyuan Li
Tao Chen
Hao Zhou
Wenkan Zhang
Nong Lin
Xiaohua Yu
Yu Lou
Binghao Li
Eloy Yinwang
Zenan Wang
Keyi Wang
Yucheng Xue
Hao Qu
Peng Lin
Hangxiang Sun
Wangsiyuan Teng
Haochen Mou
Xupeng Chai
Zhijian Cai
Zhaoming Ye
机构
[1] The Second Affiliated Hospital of Zhejiang University School of Medicine,Department of Orthopedics, Musculoskeletal Tumor Center
[2] Zhejiang University,Institute of Orthopedic Research
[3] Key Laboratory of Motor System Disease Research and Precision Therapy of Zhejiang Province,Department of Hepatobiliary and Pancreatic Surgery, The First Affiliated Hospital
[4] Zhejiang University School of Medicine,Institute of Immunology and Department of Orthopaedics of the Second Affiliated Hospital
[5] Zhejiang University School of Medicine,undefined
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关键词
γδ T cells; Antigen presentation; Tumor immunotherapy; Osteosarcoma;
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摘要
Human Vγ9Vδ2 T cells have attracted considerable attention as novel alternative antigen-presenting cells (APCs) with the potential to replace dendritic cells in antitumor immunotherapy owing to their high proliferative capacity and low cost. However, the utility of γδ T cells as APCs to induce CD8+ T cell-mediated antitumor immune response, as well as the mechanism by which they perform APC functions, remains unexplored. In this study, we found that activated Vγ9Vδ2 T cells were capable of inducing robust CD8+ T cell responses in osteosarcoma cells. Activated γδ T cells also effectively suppressed osteosarcoma growth by priming CD8+ T cells in xenograft animal models. Mechanistically, we further revealed that activated γδ T cells exhibited increased HSP90 production, which fed back to upregulate MyD88, followed by JNK activation and a subsequent improvement in CCL5 secretion, leading to enhanced CD8+ T cell cross-priming. Thus, our study suggests that Vγ9Vδ2 T cells represent a promising alternative APC for the development of γδ T cell-based tumor immunotherapy.
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页码:1803 / 1821
页数:18
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