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开发一种新的抗生素诱导的犬结肠微生物群失调模型。

Development of a new antibiotic-induced dysbiosis model of the canine colonic microbiota.

机构信息

Université Clermont Auvergne, UMR 454 MEDIS UCA-INRAE, Clermont-Ferrand, France; Lallemand Animal Nutrition, Blagnac Cedex, France.

Lallemand Animal Nutrition, Blagnac Cedex, France.

出版信息

Int J Antimicrob Agents. 2024 Apr;63(4):107102. doi: 10.1016/j.ijantimicag.2024.107102. Epub 2024 Feb 5.

Abstract

As in humans, antibiotics are widely used in dogs to treat gastrointestinal infections, contributing to the global burden of antimicrobial resistance on both human and animal health. Close contact between pets and their owners can lead to horizontal transfer of gut microbes, including transmission of antibiotic resistance. Nevertheless, until now, the impact of antibiotics on the canine gut microbiota has been poorly described. The aim of this study was to adapt the canine mucosal artificial colon (CANIM-ARCOL) model, reproducing the main nutritional, physicochemical and microbial parameters found in the large intestine of the dog to simulate an antibiotic-induced perturbation. Following initial investigation of five antibiotic cocktails at in-field doses, a 5-day regimen of metronidazole/enrofloxacin (ME) was selected for further model development. Two CANIM-ARCOL bioreactors were inoculated with a faecal sample (n=2 donors) and run in parallel for 26 days under control or antibiotic conditions. ME reduced microbial diversity and induced major shifts in bacterial populations, leading to a state of dysbiosis characterized by an increase in the relative abundance of Streptococcaceae, Lactobacillaceae and Enterobacteriaceae, and a decrease in the relative abundance of Bacteroidaceae, Fusobacteriota and Clostridiaceae. Overall, mucus-associated microbiota were less impacted by antibiotics than luminal microbes. Microbial alterations were associated with drastic decreases in gas production and short-chain fatty acid concentrations. Finally, the model was well validated through in-vitro-in-vivo comparisons in a study in dogs. The CANIM-ARCOL model provides a relevant platform as an alternative to in-vivo assays for an in-depth understanding of antibiotic-microbiota interactions and further testing of restoration strategies at individual level.

摘要

与人类一样,抗生素在狗中被广泛用于治疗胃肠道感染,这导致了人类和动物健康的抗微生物药物耐药性的全球负担。宠物与它们的主人之间的密切接触会导致肠道微生物的水平转移,包括抗生素耐药性的传播。然而,直到现在,抗生素对犬肠道微生物群的影响还描述得很差。本研究的目的是适应犬黏膜人工结肠(CANIM-ARCOL)模型,该模型再现了狗大肠中发现的主要营养、物理化学和微生物参数,以模拟抗生素诱导的扰动。在现场剂量下对五种抗生素鸡尾酒进行初步研究后,选择了 5 天的甲硝唑/恩诺沙星(ME)方案用于进一步的模型开发。两个 CANIM-ARCOL 生物反应器用粪便样本(n=2 个供体)接种,并在对照或抗生素条件下平行运行 26 天。ME 降低了微生物多样性,并引起了细菌种群的重大变化,导致了一种失调状态,其特征是链球菌科、乳杆菌科和肠杆菌科的相对丰度增加,拟杆菌科、梭菌科和梭菌科的相对丰度减少。总的来说,抗生素对粘液相关微生物群的影响小于对腔微生物的影响。微生物的改变与气体产生和短链脂肪酸浓度的急剧下降有关。最后,该模型在犬体内-体外研究中得到了很好的验证。CANIM-ARCOL 模型为深入了解抗生素-微生物群相互作用和进一步在个体水平上测试恢复策略提供了一个替代体内试验的相关平台。

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