肠道微生物组与免疫调节在恶性肿瘤治疗中的作用

Babu Hs, N. West, A. Cripps, J. Sanmugarajah, R. Mason
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引用次数: 0

摘要

肠道微生物组在晚期恶性肿瘤免疫检查点抑制剂治疗(ICIs)的反应和毒性中的潜在作用已成为医学肿瘤学领域日益关注的领域。许多临床前和临床试验已经确定了对ICI结果有有益影响的不同微生物组因素,包括特定微生物和多样性,并表明肠道微生物组的改变可以影响治疗结果,例如通过抗生素给药。有共存的证据表明,微生物组也可能影响ICIs的毒性特征。目前,现有文献描述了微生物组与ICI结果之间的关联,但因果关系尚未确定。此外,迄今为止的研究在受试者和各自微生物组组成之间存在固有异质性方面提出了问题。虽然有希望,但小鼠人源化模型或无菌小鼠不一定表现出与人类相当的免疫能力或宏基因组功能。粪便微生物群可能在更大的抗肿瘤免疫反应和影响这一反应的患者因素中发挥作用,这必须在临床背景下整体看待。最终,这是一个充满希望的领域,正在快速发展。研究同样也在进行中,以优化治疗方法来改变这些微生物群,无论是通过粪便移植,还是直接向肠道补充短链脂肪酸。更多地了解微生物组的组成部分如何发挥局部和全身免疫反应,可能预示着用免疫疗法治疗实体肿瘤的重大飞跃。
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The Gut Microbiome and Immune Modulation in The Treatment of Malignancy
The potential role of the gut microbiomes in the response and toxicity to immune checkpoint inhibitor therapies (ICIs) in advanced malignancies has been a growing area of interest within the field of medical oncology. A number of pre-clinical and clinical trials have identified different microbiome factors that beneficially impact upon ICI outcomes, including specific microorganisms and diversity and suggested that treatment outcomes can be influenced by modification of the gut microbiome, such as through antibiotic administration. There is coexisting evidence the microbiome may also impact on the toxicity profile of ICIs. Currently, the available literature describes associations between the microbiome and ICI outcomes, but the causal link is yet to be established. Additionally, the studies to date pose problems in the inherent heterogeneity that exists between subjects and respective microbiome composition. While promising, murine-humanised models or germ-free mice do not necessarily exhibit comparable immunocompetency or metagenomic function to humans. The faecal microbiome is likely to play a part of the much larger anti-tumour immune response and patient factors that influence this, which must be viewed holistically in the clinical context. Ultimately, this is a promising area, hurtling forward rapidly. Research is equally underway for optimizing methods to administer treatments to alter these microbiomes, whether it be via faecal transplantation, or supplementation with short chain fatty acids directly to the bowel. Learning more about how the constituent parts of the microbiome exert local and systemic immune responses could herald a significant leap forward in how solid tumours are treated with immunotherapy.
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