A new evaluation system for drug–microbiota interactions

IF 23.7 Q1 MICROBIOLOGY

iMeta Pub Date : 2024-05-07 DOI:10.1002/imt2.199

Tian-Hao Liu, Chen-Yang Zhang, Hang Zhang, Jing Jin, Xue Li, Shi-Qiang Liang, Yu-Zheng Xue, Feng-Lai Yuan, Ya-Hong Zhou, Xiu-Wu Bian, Hong Wei

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Abstract

The drug response phenotype is determined by a combination of genetic and environmental factors. The high clinical conversion failure rate of gene-targeted drugs might be attributed to the lack of emphasis on environmental factors and the inherent individual variability in drug response (IVDR). Current evidence suggests that environmental variables, rather than the disease itself, are the primary determinants of both gut microbiota composition and drug metabolism. Additionally, individual differences in gut microbiota create a unique metabolic environment that influences the in vivo processes underlying drug absorption, distribution, metabolism, and excretion (ADME). Here, we discuss how gut microbiota, shaped by both genetic and environmental factors, affects the host's ADME microenvironment within a new evaluation system for drug–microbiota interactions. Furthermore, we propose a new top-down research approach to investigate the intricate nature of drug–microbiota interactions in vivo. This approach utilizes germ-free animal models, providing foundation for the development of a new evaluation system for drug–microbiota interactions.

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药物与微生物群相互作用的新评估系统

药物反应表型由遗传和环境因素共同决定。基因靶向药物的临床转化失败率较高，这可能是由于缺乏对环境因素的重视以及药物反应固有的个体差异性（IVDR）造成的。目前的证据表明，环境变量而非疾病本身是肠道微生物群组成和药物代谢的主要决定因素。此外，肠道微生物群的个体差异会形成独特的代谢环境，影响药物吸收、分布、代谢和排泄（ADME）的体内过程。在此，我们将讨论肠道微生物群是如何在药物与微生物群相互作用的新评价体系中，通过遗传和环境因素影响宿主的 ADME 微环境的。此外，我们还提出了一种新的自上而下的研究方法，用于研究药物与微生物群在体内相互作用的复杂性质。这种方法利用无菌动物模型，为开发药物与微生物群相互作用的新评估系统奠定了基础。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

iMeta

CiteScore

10.80

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0.00%

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