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Gut microbiome and anticancer immune response: really hot Sh(star)t!

机译:肠道微生物组和抗癌免疫应答:真的很热(星)t!

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摘要

The impact of gut microbiota in eliciting innate and adaptive immune responses beneficial for the host in the context of effective therapies against cancer has been highlighted recently. Chemotherapeutic agents, by compromising, to some extent, the intestinal integrity, increase the gut permeability and selective translocation of Gram-positive bacteria in secondary lymphoid organs. There, anticommensal pathogenic Th17 T-cell responses are primed, facilitating the accumulation of Th1 helper T cells in tumor beds after chemotherapy as well as tumor regression. Importantly, the redox equilibrium of myeloid cells contained in the tumor microenvironment is also influenced by the intestinal microbiota. Hence, the anticancer efficacy of alkylating agents (such as cyclophosphamide) and platinum salts (oxaliplatin, cis-platin) is compromised in germ-free mice or animals treated with antibiotics. These findings represent a paradigm shift in our understanding of the mode of action of many compounds having an impact on the host-microbe mutualism.
机译:最近强调了肠道微生物肠肠道微生物症对癌症的有效治疗背景下有利于主持人的自生先生和适应性免疫反应。通过损害在一定程度上,化学治疗剂在一定程度上,增加次级淋巴器官中革肠阳性细菌的肠道渗透性和选择性易位。在那里,孕源致病致胞细胞反应促进了化疗后肿瘤床中TH1辅助T细胞的积累以及肿瘤回归。重要的是,肿瘤微环境中含有的骨髓细胞的氧化还原平衡也受到肠道微生物的影响。因此,烷基化试剂(例如环磷酰胺)和铂盐(Oxaliplatin,Cis-铂)的抗癌疗效在无菌小鼠或用抗生素处理的动物中受到损害。这些发现代表了我们对许多化合物的作用方式对宿主微生物共同主义的作用方式进行了范式转变。

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