S1PR4 基因敲除通过 CD8+T 细胞扩增来抑制肿瘤生长并提高化疗效果。
S1PR4 ablation reduces tumor growth and improves chemotherapy via CD8+ T cell expansion.
机构信息
Institute of Biochemistry I, Faculty of Medicine, Goethe University Frankfurt, Frankfurt, Germany.
Institute for Tumor Biology and Experimental Therapy, Georg-Speyer-Haus, Frankfurt, Germany.
出版信息
J Clin Invest. 2020 Oct 1;130(10):5461-5476. doi: 10.1172/JCI136928.
Abstract
Tumor immunosuppression is a limiting factor for successful cancer therapy. The lipid sphingosine-1-phosphate (S1P), which signals through 5 distinct G protein-coupled receptors (S1PR1-5), has emerged as an important regulator of carcinogenesis. However, the utility of targeting S1P in tumors is hindered by S1P's impact on immune cell trafficking. Here, we report that ablation of the immune cell-specific receptor S1PR4, which plays a minor role in immune cell trafficking, delayed tumor development and improved therapy success in murine models of mammary and colitis-associated colorectal cancer through increased CD8+ T cell abundance. Transcriptome analysis revealed that S1PR4 affected proliferation and survival of CD8+ T cells in a cell-intrinsic manner via the expression of Pik3ap1 and Lta4h. Accordingly, PIK3AP1 expression was connected to increased CD8+ T cell proliferation and clinical parameters in human breast and colon cancer. Our data indicate a so-far-unappreciated tumor-promoting role of S1P by restricting CD8+ T cell expansion via S1PR4.
摘要
肿瘤免疫抑制是癌症治疗成功的一个限制因素。脂质鞘氨醇-1-磷酸(S1P)通过 5 种不同的 G 蛋白偶联受体(S1PR1-5)发出信号,已成为癌症发生的重要调节剂。然而,由于 S1P 对免疫细胞迁移的影响,靶向 S1P 在肿瘤中的应用受到阻碍。在这里,我们报告说,通过增加 CD8+T 细胞的丰度,靶向免疫细胞特异性受体 S1PR4(在免疫细胞迁移中作用较小)的缺失会延迟乳腺和结肠炎相关结直肠癌的小鼠模型中的肿瘤发展并提高治疗成功率。转录组分析表明,S1PR4 通过表达 Pik3ap1 和 Lta4h 以细胞内固有方式影响 CD8+T 细胞的增殖和存活。因此,PIK3AP1 的表达与人类乳腺癌和结肠癌中 CD8+T 细胞增殖和临床参数的增加有关。我们的数据表明,S1P 通过 S1PR4 限制 CD8+T 细胞的扩增,从而发挥了迄今为止尚未被认识到的肿瘤促进作用。
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