ICEPmu1, an integrative conjugative element (ICE) of Pasteurella multocida: structure and transfer

多杀性巴氏杆菌 生物 基因 遗传学 大肠杆菌 水平基因转移 微生物学 肉汤微量稀释 转移RNA 基因组 细菌 核糖核酸 最小抑制浓度
作者
G. B. Michael,Kristina Kadlec,M.T. Sweeney,E. Brzuszkiewicz,Heiko Liesegang,Rolf Daniel,Robert W. Murray,Jeffrey L. Watts,S. Schwarz
出处
期刊:Journal of Antimicrobial Chemotherapy [Oxford University Press]
卷期号:67 (1): 91-100 被引量:104
标识
DOI:10.1093/jac/dkr411
摘要

Integrative and conjugative elements (ICEs) have not been detected in Pasteurella multocida. In this study the multiresistance ICEPmu1 from bovine P. multocida was analysed for its core genes and its ability to conjugatively transfer into strains of the same and different genera.ICEPmu1 was identified during whole genome sequencing. Coding sequences were predicted by bioinformatic tools and manually curated using the annotation software ERGO. Conjugation into P. multocida, Mannheimia haemolytica and Escherichia coli recipients was performed by mating assays. The presence of ICEPmu1 and its circular intermediate in the recipient strains was confirmed by PCR and sequence analysis. Integration sites were sequenced. Susceptibility testing of the ICEPmu1-carrying recipients was conducted by broth microdilution.The 82 214 bp ICEPmu1 harbours 88 genes. The core genes of ICEPmu1, which are involved in excision/integration and conjugative transfer, resemble those found in a 66 641 bp ICE from Histophilus somni. ICEPmu1 integrates into a tRNA(Leu) and is flanked by 13 bp direct repeats. It is able to conjugatively transfer to P. multocida, M. haemolytica and E. coli, where it also uses a tRNA(Leu) for integration and produces closely related 13 bp direct repeats. PCR assays and susceptibility testing confirmed the presence and the functional activity of the ICEPmu1-associated resistance genes in the recipient strains.The observation that the multiresistance ICEPmu1 is present in a bovine P. multocida and can easily spread across strain and genus boundaries underlines the risk of a rapid dissemination of multiple resistance genes, which will distinctly decrease the therapeutic options.
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