首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Rapalog combined with CCR4 antagonist improves anticancer vaccines efficacy
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Rapalog combined with CCR4 antagonist improves anticancer vaccines efficacy

机译:Rabalog与CCR4拮抗剂相结合,改善了抗癌疫苗功效

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mTOR pathway inhibitors such as rapalogs represent a promising tool to induce functional memory CD8 T cells. In our study, we investigated the combination of temsirolimus with anticancer vaccines. Using various designs of cancer vaccines (short and long peptides or the B subunit of Shiga toxin as an antigen delivery vector) and tumor models (melanoma, lung and colon cancer), we showed that the administration of temsirolimus efficiently decreased tumor growth and enhanced tumor‐specific CD8 T‐cell responses induced by vaccination. Furthermore, tumor‐specific CD8 T cells induced by the bi‐therapy (vaccine + temsirolimus) exhibit phenotypic characteristics of central memory (CD127 + CD62L + ) CD8 T cells compared to vaccination alone. We demonstrated that regulatory CD4 T cells (T regs ) expansion in vivo limits the efficacy of the bi‐therapy by altering the antitumor CD8 T‐cell responses. Finally, the use of a small molecule CCR4 antagonist to prevent T regs induction considerably improved the efficacy of the bi‐therapy by enhancing CD8 T cells‐mediated antitumor immunity. Taken together, our study highlights the potential interest of combining cancer vaccines with drugs that promote memory CD8 T cells and inhibit T regs .
机译:MTOR途径抑制剂,如RapAlogs代表了诱导功能性记忆CD8 T细胞的有希望的工具。在我们的研究中,我们调查了Temsirolimus与抗癌疫苗的组合。使用各种癌症疫苗设计(Shiga Toxin的短肽或Shiga Toxin的B亚基作为抗原输送载体)和肿瘤模型(黑素瘤,肺和结肠癌),我们表明Temsirolimus的给药有效地降低了肿瘤生长和增强肿瘤疫苗接种诱导的特异性CD8 T细胞应答。此外,由双治疗(疫苗+ Temsirolimus)诱导的肿瘤特异性CD8 T细胞表现出中央记忆(CD127 + CD62L +)CD8 T细胞的表型特性与单独接种疫苗。我们证明,通过改变抗肿瘤CD8 T细胞反应,体内调节CD4 T细胞(T REGS)扩增限制了双治疗的疗效。最后,使用小分子CCR4拮抗剂来预防T Regs诱导通过增强CD8 T细胞介导的抗肿瘤免疫力显着提高了双治疗的功效。我们的研究突出了突出了将癌症疫苗与促进记忆CD8 T细胞的药物组合并抑制T regs的潜在兴趣。

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