检查点抑制剂治疗中微生物组与结肠免疫系统的相互作用

Jacob Dehinsilu, Chrysi Sergaki, G. Amos, V. Fontana, M. Pirmohamed
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引用次数: 0

摘要

免疫检查点抑制剂疗法的出现是癌症治疗发展的重要一步。然而,这是一把双刃剑。免疫相关的不良事件是释放免疫系统刹车的结果,影响许多接受检查点抑制剂治疗的患者,通常使人虚弱,偶尔致命。在小鼠和人类中都显示,某些家族、属和种类的细菌的存在与对检查点抑制剂治疗的反应改善有关,而在没有它们的情况下,对治疗的反应往往很差。最近的研究表明,检查点抑制剂治疗的免疫相关不良事件可能会受到干扰,并可能根据肠道微生物群和部分免疫系统的组成和功能能力进行预测。在与免疫检查点抑制剂治疗相关的结肠炎的情况下,一个有趣的研究途径是基于分泌性免疫球蛋白A (SIgA)的活性。IgA由浆细胞产生,高浓度存在于肠道黏膜,参与微生物群的成熟和维持以及IBD的发展。在这里,我们总结了目前关于肠道微生物群与CPI治疗反应之间相互作用的文献。此外,我们概述了结肠免疫系统,特别关注IgA,作为微生物-免疫系统相互作用的关键组成部分。
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The interplay between the microbiome and colonic immune system in checkpoint inhibitor therapy
The advent of immune checkpoint inhibitor therapy was a significant step in the development of treatments for cancer. It is, however, a double-edged sword. Immune related adverse events are the result of unleashing brakes on the immune system and affect many patients undergoing checkpoint inhibitor therapy, often being debilitating and occasionally lethal. It has been shown both in mice and in humans that the presence of certain families, genera and species of bacteria are associated with improved responses to checkpoint inhibitor therapy, whereas in their absence the response to therapy is often poor. Recent studies have demonstrated that immune related adverse events to checkpoint inhibitor therapy can be perturbed and perhaps predicted based on the composition and functional capacity of the gut microbiota and parts of the immune system. In the case of colitis associated with immune checkpoint inhibitor therapy, one interesting avenue of investigation is based on the activity of secretory immunoglobulin A (SIgA). Produced by plasma cells, IgA is present in high concentrations at the gut mucosa and is involved in both the maturation and maintenance of the microbiota as well as the development of IBD. Here we summarise the current literature surrounding the interplay between the gut microbiota and response to CPI therapy. Additionally, we overview the colonic immune system, paying particular attention to IgA, as a key component of the microbiota-immune system interaction.
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