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在M-SHIME中抗生素抗性质粒从共生菌向人类肠道微生物群的转移:剂量、个体差异和抗生素使用的影响

Transfer of Antibiotic Resistance Plasmid from Commensal Towards Human Intestinal Microbiota in the M-SHIME: Effect of dosis, Human Individual and Antibiotic Use.

作者信息

Lambrecht Ellen, Coillie Els Van, Boon Nico, Heyndrickx Marc, Wiele Tom Van de

机构信息

CMET, Center for Microbial Ecology and Technology, Ghent University, Coupure links 653, 9000 Gent, Belgium.

ILVO, Flanders Research Institute for Agriculture, Fisheries and Food, Brusselsesteenweg 370, 9090 Melle, Belgium.

出版信息

Life (Basel). 2021 Feb 28;11(3):192. doi: 10.3390/life11030192.

Abstract

Along with (in) direct contact with animals and a contaminated environment, humans are exposed to antibiotic-resistant bacteria by consumption of food. The implications of ingesting antibiotic-resistant commensal bacteria are unknown, as dose-response data on resistance transfer and spreading in our gut is lacking. In this study, transfer of a resistance plasmid (IncF), harbouring several antibiotic resistance genes, from a commensal strain towards human intestinal microbiota was assessed using a Mucosal Simulator of the Human Intestinal Ecosystem (M-SHIME). More specifically, the effect of the initial plasmid donor concentration (10 and 10 CFU/meal), antibiotic treatment (cefotaxime) and human individual (n = 6) on plasmid transfer towards lumen coliforms and anaerobes was determined. Transfer of the resistance plasmid to luminal coliforms and anaerobes was observed shortly after the donor strain arrived in the colon and was independent of the ingested dose. Transfer occurred in all six simulated colons and despite their unique microbial community composition, no differences could be detected in antibiotic resistance transfer rates between the simulated human colons. After 72 h, resistant coliform transconjugants levels ranged from 7.6 × 10 to 7.9 × 10 CFU/Ml colon lumen. Presence of the resistance plasmid was confirmed and quantified by PCR and qPCR. Cefotaxime treatment led to a significant reduction (85%) in resistant coliforms, however no significant effect on the total number of cultivable coliforms and anaerobes was observed.

摘要

除了与动物和受污染环境的(直接)接触外,人类还会通过食用食物接触到抗生素抗性细菌。由于缺乏关于抗性在我们肠道中的转移和传播的剂量反应数据,摄入抗生素抗性共生细菌的影响尚不清楚。在本研究中,使用人类肠道生态系统黏膜模拟器(M-SHIME)评估了携带多个抗生素抗性基因的抗性质粒(IncF)从共生菌株向人类肠道微生物群的转移。更具体地说,确定了初始质粒供体浓度(10和10 CFU/餐)、抗生素治疗(头孢噻肟)和个体(n = 6)对向肠腔大肠菌和厌氧菌的质粒转移的影响。供体菌株到达结肠后不久,就观察到抗性质粒向肠腔大肠菌和厌氧菌的转移,且与摄入剂量无关。在所有六个模拟结肠中均发生了转移,尽管它们的微生物群落组成独特,但在模拟的人类结肠之间的抗生素抗性转移率上未检测到差异。72小时后,抗性大肠菌转接合子水平在7.6×10至7.9×10 CFU/毫升结肠腔之间。通过PCR和qPCR确认并定量了抗性质粒的存在。头孢噻肟治疗导致抗性大肠菌显著减少(85%),然而,未观察到对可培养大肠菌和厌氧菌总数的显著影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6c8/7997361/1b9d3af989ad/life-11-00192-g0A1.jpg

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