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Gut microbiome interactions with drug metabolism, efficacy, and toxicity

机译:肠道微生物组合与药物代谢,疗效和毒性相互作用

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摘要

The gut microbiota has both direct and indirect effects on drug and xenobiotic metabolisms, and this can have consequences for both efficacy and toxicity. Indeed, microbiome-driven drug metabolism is essential for the activation of certain pro drugs, for example, azo drugs such as prontosil and neoprontosil resulting in the release of sulfanilamide. In addition to providing a major source of reductive metabolizing capability, the gut microbiota provides a suite of additional reactions including acetylation, deacylation, decarboxylation, dehydroxylation, demethylation, dehalogenation, and importantly, in the context of certain types of drug related toxicity, conjugates hydrolysis reactions. In addition to direct effects, the gut microbiota can affect drug metabolism and toxicity indirectly via, for example, the modulation of host drug metabolism and disposition and competition of bacterial-derived metabolites for xenobiotic metabolism pathways. Also, of course, the therapeutic drugs themselves can have effects, both intended and unwanted, which can impact the health and composition of the gut microbiota with unforeseen consequences.
机译:肠道微生物会对药物和异种症代谢具有直接和间接影响,这可能对疗效和毒性产生后果。实际上,微生物组驱动的药物代谢对于激活某些专业药物,例如偶氮药物,例如Prontosil和Neoprontosil,导致磺胺胺的释放。除了提供还原性代谢能力的主要来源之外,肠道微生物群还提供了一套额外的反应,包括乙酰化,脱酰化,脱羧,脱羟基化,去偏析,脱卤,重要的是,在某些类型的药物相关毒性的背景下,缀合物水解反应。除了直接效果之外,肠道微生物会可以间接地通过例如对宿主药物代谢和性格调节和异种衍生的代谢物的调节来影响药物代谢和毒性。此外,当然,治疗药物本身可以具有意图和不需要的效果,这可能会影响肠道微生物的健康和组成与无法预见的后果。

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