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基于生物反应器模型,质子泵抑制剂通过改变pH值而非影响肠道微生物群来增加感染风险。

Proton-pump inhibitors increase infection risk by altering pH rather than by affecting the gut microbiome based on a bioreactor model.

作者信息

Schumacher Julia, Müller Patrick, Sulzer Johannes, Faber Franziska, Molitor Bastian, Maier Lisa

机构信息

Cluster of Excellence EXC 2124 Controlling Microbes to Fight Infections, University of Tübingen, Tübingen, Germany.

Environmental Biotechnology Group, Department of Geosciences, University of Tübingen, Tübingen, Germany.

出版信息

Gut Microbes. 2025 Dec;17(1):2519697. doi: 10.1080/19490976.2025.2519697. Epub 2025 Jun 16.

Abstract

infections often occur after antibiotic use, but they have also been linked to proton-pump inhibitor (PPI) therapy. The underlying mechanism - whether infection risk is due to a direct effect of PPIs on the gut microbiome or changes in gastrointestinal pH - has remained unclear. To disentangle both possibilities, we studied the impact of the proton-pump inhibitor omeprazole and pH changes on key members of the human gut microbiome and stool-derived microbial communities from different donors . We then developed a custom multiple-bioreactor system to grow a model human microbiome community and a stool-derived community in chemostat mode and tested the effects of omeprazole exposure, pH changes, and their combination on growth within these communities. Our findings show that changes in pH significantly affect the gut microbial community's biomass and the abundances of different bacterial taxa, leading to increased growth within the community. However, omeprazole treatment alone did not result in such effects. These findings imply that the higher risk of infection following proton-pump inhibitor therapy is probably because of alterations in gastrointestinal pH rather than a direct interaction between the drug and the microbiome. This understanding offers a new perspective on infection risks in proton-pump inhibitor therapy.

摘要

感染常在使用抗生素后发生,但也与质子泵抑制剂(PPI)治疗有关。其潜在机制——感染风险是由于PPI对肠道微生物群的直接作用还是胃肠道pH值的变化——仍不清楚。为了厘清这两种可能性,我们研究了质子泵抑制剂奥美拉唑和pH值变化对来自不同捐赠者的人类肠道微生物群关键成员和粪便衍生微生物群落的影响。然后,我们开发了一种定制的多生物反应器系统,以恒化器模式培养模型人类微生物群落和粪便衍生群落,并测试了奥美拉唑暴露、pH值变化及其组合对这些群落内生长的影响。我们的研究结果表明,pH值变化显著影响肠道微生物群落的生物量和不同细菌类群的丰度,导致群落内生长增加。然而,单独使用奥美拉唑治疗并未产生此类效果。这些发现表明,质子泵抑制剂治疗后感染风险较高可能是由于胃肠道pH值的改变,而非药物与微生物群之间的直接相互作用。这一认识为质子泵抑制剂治疗中的感染风险提供了新的视角。

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