AUTHOR=Liu Hongbo , Zhu Binghua , Liang Beibei , Xu Xuebin , Qiu Shaofu , Jia Leili , Li Peng , Yang Lang , Li Yongrui , Xiang Ying , Xie Jing , Wang Ligui , Yang Chaojie , Sun Yansong , Song Hongbin 

TITLE=A Novel mcr-1 Variant Carried by an IncI2-Type Plasmid Identified From a Multidrug Resistant Enterotoxigenic Escherichia coli

JOURNAL=Frontiers in Microbiology

VOLUME=9

YEAR=2018

URL=https://www.frontiersin.org/journals/microbiology/articles/10.3389/fmicb.2018.00815

DOI=10.3389/fmicb.2018.00815

ISSN=1664-302X

ABSTRACT=<p>In this study, we discovered a novel mobilized colistin resistance (<italic>mcr-1</italic>) gene variant, named <italic>mcr-1.9</italic>, which was identified in a colistin-resistant enterotoxigenic <italic>Escherichia coli</italic> (ETEC) strain from a clinical diarrhea case. The <italic>mcr-1.9</italic> gene differs from <italic>mcr-1</italic> at position 1036 due to a single nucleotide polymorphism (G→A), which results in an aspartic acid residue being replaced by an asparagine residue (Asp346→Asn) in the MCR-1 protein sequence. Antimicrobial susceptibility testing showed that the <italic>mcr-1.9</italic>-harboring ETEC strain is resistant to colistin at a minimum inhibitory concentration of 4 μg/ml. Plasmid profiling and conjugation experiments also suggest that the <italic>mcr-1.9</italic> variant can be successfully transferred into the <italic>E. coli</italic> strain J53, indicating that the gene is located on a transferable plasmid. Bioinformatics analysis of data obtained from genome sequencing indicates that the <italic>mcr-1.9</italic> gene is located on a 64,005 bp plasmid which has been named pEC26. This plasmid was found to have high similarity to the <italic>mcr-1</italic>-bearing IncI2-type plasmids pWF-5-19C (99% identity and 99% coverage) and pmcr1-IncI2 (99% identity and 98% coverage). The <italic>mcr-1.9-</italic>harboring ETEC also shows multidrug resistance to nine classes of antibiotics, and contains several virulence and antimicrobial-resistance genes suggested by the genome sequence analysis. Our report is the first to identify a new <italic>mcr-1</italic> variant in an ETEC isolated from a human fecal sample, raising concerns about the existence of more such variants in human intestinal flora. Therefore, we believe that an undertaking to identify new <italic>mcr-1</italic> variants in the bacterial communities of human intestines is of utmost importance, and that measures need to be taken to control the spread of <italic>mcr-1</italic> and its variants in human intestinal microflora.</p>