Aspirin prevents metastasis by limiting platelet TXA(2) suppression of T cell immunity.

阿司匹林通过限制血小板 TXA(2) 对 T 细胞免疫的抑制作用来预防转移

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作者:Yang Jie, Yamashita-Kanemaru Yumi, Morris Benjamin I, Contursi Annalisa, Trajkovski Daniel, Xu Jingru, Patrascan Ilinca, Benson Jayme, Evans Alexander C, Conti Alberto G, Al-Deka Aws, Dahmani Layla, Avdic-Belltheus Adnan, Zhang Baojie, Okkenhaug Hanneke, Whiteside Sarah K, Imianowski Charlotte J, Wesolowski Alexander J, Webb Louise V, Puccio Simone, Tacconelli Stefania, Bruno Annalisa, Di Berardino Sara, De Michele Alessandra, Welch Heidi C E, Yu I-Shing, Lin Shu-Wha, Mitra Suman, Lugli Enrico, van der Weyden Louise, Okkenhaug Klaus, Saeb-Parsy Kourosh, Patrignani Paola, Adams David J, Roychoudhuri Rahul
Metastasis is the spread of cancer cells from primary tumours to distant organs and is the cause of 90% of cancer deaths globally(1,2). Metastasizing cancer cells are uniquely vulnerable to immune attack, as they are initially deprived of the immunosuppressive microenvironment found within established tumours(3). There is interest in therapeutically exploiting this immune vulnerability to prevent recurrence in patients with early cancer at risk of metastasis. Here we show that inhibitors of cyclooxygenase 1 (COX-1), including aspirin, enhance immunity to cancer metastasis by releasing T cells from suppression by platelet-derived thromboxane A(2) (TXA(2)). TXA(2) acts on T cells to trigger an immunosuppressive pathway that is dependent on the guanine exchange factor ARHGEF1, suppressing T cell receptor-driven kinase signalling, proliferation and effector functions. T cell-specific conditional deletion of Arhgef1 in mice increases T cell activation at the metastatic site, provoking immune-mediated rejection of lung and liver metastases. Consequently, restricting the availability of TXA(2) using aspirin, selective COX-1 inhibitors or platelet-specific deletion of COX-1 reduces the rate of metastasis in a manner that is dependent on T cell-intrinsic expression of ARHGEF1 and signalling by TXA(2) in vivo. These findings reveal a novel immunosuppressive pathway that limits T cell immunity to cancer metastasis, providing mechanistic insights into the anti-metastatic activity of aspirin and paving the way for more effective anti-metastatic immunotherapies.

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