| Literature DB >> 31133751 |
Tao He1, Ran Wang1, Dejun Liu2, Timothy R Walsh2,3, Rong Zhang4, Yuan Lv5, Yuebin Ke6, Quanjiang Ji7, Ruicheng Wei1, Zhihai Liu2, Yingbo Shen2, Gang Wang1, Lichang Sun1, Lei Lei2, Ziquan Lv6, Yun Li5, Maoda Pang1, Liyuan Wang5, Qiaoling Sun4, Yulin Fu2, Huangwei Song2, Yuxin Hao2, Zhangqi Shen2, Shaolin Wang2, Gongxiang Chen4, Congming Wu2, Jianzhong Shen8,9, Yang Wang10,11.
Abstract
Tigecycline is a last-resort antibiotic that is used to treat severe infections caused by extensively drug-resistant bacteria. tet(X) has been shown to encode a flavin-dependent monooxygenase that modifies tigecycline1,2. Here, we report two unique mobile tigecycline-resistance genes, tet(X3) and tet(X4), in numerous Enterobacteriaceae and Acinetobacter that were isolated from animals, meat for consumption and humans. Tet(X3) and Tet(X4) inactivate all tetracyclines, including tigecycline and the newly FDA-approved eravacycline and omadacycline. Both tet(X3) and tet(X4) increase (by 64-128-fold) the tigecycline minimal inhibitory concentration values for Escherichia coli, Klebsiella pneumoniae and Acinetobacter baumannii. In addition, both Tet(X3) (A. baumannii) and Tet(X4) (E. coli) significantly compromise tigecycline in in vivo infection models. Both tet(X3) and tet(X4) are adjacent to insertion sequence ISVsa3 on their respective conjugative plasmids and confer a mild fitness cost (relative fitness of >0.704). Database mining and retrospective screening analyses confirm that tet(X3) and tet(X4) are globally present in clinical bacteria-even in the same bacteria as blaNDM-1, resulting in resistance to both tigecycline and carbapenems. Our findings suggest that both the surveillance of tet(X) variants in clinical and animal sectors and the use of tetracyclines in food production require urgent global attention.Entities:
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Year: 2019 PMID: 31133751 DOI: 10.1038/s41564-019-0445-2
Source DB: PubMed Journal: Nat Microbiol ISSN: 2058-5276 Impact factor: 17.745