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Gut microbiotas and immune checkpoint inhibitor therapy response: a causal or coincidental relationship?

机译:Gut microbiotas和免疫检查点抑制剂治疗反应:因果或巧合吗?

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摘要

As the largest immune organ, human gut microbiome could influence the efficacy of immune checkpoint inhibitor therapy (ICI). However, identifying contributory microbes from over 35,000 species is virtually impossible and the identified microbes are not consistent among studies. The reason for the disparity may be that the microbes found in feces are markers of other factors that link immune response and microbiotas. Notably, gut microbiome is influenced by stool consistency, diet and other lifestyle factors. Therefore, the ICI and microbiotas relationship must be adjusted for potential confounders and analyzed longitudinally. Moreover, a recent study where 11 low-abundance commensal bacteria induced interferon-gamma-producing CD8 T cells, challenges the validity of the abundance-oriented microbiotas investigations. This study also confirmed the hierarchy in immunogenic roles among microbiotas. Fecal transplantation trials in germ-free mice provided "the proof of principle" that germ-free mice reproduce the donor's microbiome and corresponding ICI efficacy. However, species-specific biological differences prevent direct extrapolation between the results in murine and human models. Fecal transplantation or supplementation with microbes found in ICI responders requires caution due to potential adverse events.
机译:作为最大的免疫器官,人体肠道微生物组可以影响免疫检查点抑制剂治疗(ICI)的疗效。然而,鉴定来自35,000种物种的贡献微生物几乎是不可能的,所鉴定的微生物在研究中不一致。差距的原因可能是粪便中发现的微生物是链接免疫应答和微生物瘤的其他因素的标记。值得注意的是,肠道微生物组受到粪便一致性,饮食和其他生活方式因素的影响。因此,必须对ICI和微生物解答关系进行调整以进行潜在的混乱,并纵向分析。此外,最近的一项研究,其中11种低丰富的共谋细菌诱导干扰素 - γ-产生CD8 T细胞,挑战丰富导向的微生物溶胀的有效性。本研究还证实了微生物溶胀中免疫原性作用的等级。无菌小鼠中的粪便移植试验提供“原则上的证据”,毒药小鼠再现供体的微生物组和相应的ICI疗效。然而,物种特异性生物差异可防止鼠和人类模型的结果之间的直接外推。粪便移植或补充在ICI响应者中发现的微生物需要注意潜在的不良事件。

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