Abstract
BackgroundUSA300 methicillin-resistant Staphylococcus aureus (MRSA) is a community- and hospital-acquired pathogen that frequently causes infections but also can survive on the human body asymptomatically as a part of the normal microbiota. We devised a comparative genomic strategy to track colonizing USA300 at different body sites after an initial infection. We sampled ST8 S. aureus from subjects at the site of a first known MRSA infection. Within 60 days of this infection and again 12 months later, each subject was tested for asymptomatic colonization in the nose, throat and perirectal region. 93 S. aureus strains underwent whole genome shotgun sequencing.ResultsAmong 28 subjects at the initial sampling time, we isolated S. aureus from the nose, throat and perirectal sites from 15, 11 and 15 of them, respectively. Twelve months later we isolated S. aureus from 9 subjects, with 6, 3 and 3 strains from the nose, throat and perirectal area, respectively. Genome sequencing revealed that 23 patients (ages 0–66 years) carried USA300 intra-subject lineages (ISLs), defined as having an index infection isolate and closely related colonizing strains. Pairwise distance between strains in different ISLs was 48 to 162 single nucleotide polymorphisms (SNPs) across the core regions of the chromosome, whereas within the same ISL it was 0 to 26 SNPs. Strains in ISLs from the same subject differed in plasmid and prophage content, and contained deletions that removed the mecA-containing SCCmec and ACME regions. Five strains contained frameshift mutations in agr toxin-regulating genes. Persistence of an ISL was not associated with clinical or demographic subject characteristics. We inferred that colonization with the ISL occurred about 18 weeks before the first assessment of asymptomatic colonization.ConclusionsClonal lineages of USA300 may continue to colonize people at one or more anatomic sites up to a year after an initial infection and experience loss of the SCCmec, loss and gain of other mobile genetic elements, and mutations in the agr operon.
Highlights
USA300 methicillin-resistant Staphylococcus aureus (MRSA) is a community- and hospital-acquired pathogen that frequently causes infections and can survive on the human body asymptomatically as a part of the normal microbiota
Colonizing ST8 S. aureus strains can be isolated 12 months following initial infection We isolated and sequenced 89 novel USA300 strains from 29 subjects who presented with a ST8 MRSA infection and were subsequently found to have at least a single ST8 S. aureus isolate obtained from a colonization culture at ≥1 of the 3 tested body sites at time 1 or time 2 (12 months) (Additional file 3)
In this study we showed that S. aureus USA300 intra-subject lineage (ISL), defined as having < 30 single nucleotide polymorphisms (SNPs) over 86% of the chromosome from the common ancestor, asymptomatically colonized a patient for more than a year after a confirmed or suspected infection
Summary
USA300 methicillin-resistant Staphylococcus aureus (MRSA) is a community- and hospital-acquired pathogen that frequently causes infections and can survive on the human body asymptomatically as a part of the normal microbiota. Staphylococcus aureus is one of the most common human bacterial pathogens, causing skin and soft tissue infections (SSTI), bacteremia, osteomyelitis and other disseminated infections [1]. While it can be deadly, S. aureus is more commonly a commensal species, living on the skin, the mucous membranes, and in the gut [2] of 25–50% of the human population [3]. USA300, which has spread to many other parts of the world [13, 14], is MLST ST8 and usually
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