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Transport of daptomycin resistance genes between animals and humans as a possible mechanism for development of de novo daptomycin resistance in enterococci

Published online by Cambridge University Press:  19 December 2012

T. KELESIDIS
T. KELESIDIS*
Affiliation:
Department of Medicine, Division of Infectious Diseases, David Geffen School of Medicine at UCLA, 10833 Le Conte Ave, CHS 37-121 Los Angeles, CA 90095, USA (Email: tkelesidis@mednet.ucla.edu)
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Abstract

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Type
Correspondence
Information
Epidemiology & Infection , Volume 141 , Issue 10 , October 2013 , pp. 2185 - 2186
Copyright
Copyright © Cambridge University Press 2012 

To the Editor

Zoonoses that can be transmitted from livestock to humans have increasingly been reported [Reference Aslam1]. Geenen et al. determined the prevalence of livestock-associated methicillin-resistant Staphylococcus aureus (MRSA) on Dutch broiler farms and in people living and/or working on these farms and concluded that people in contact with live broilers are at risk for MRSA carriage worldwide [Reference Geenen2]. Another emerging infection that may be associated with livestock is daptomycin non-susceptible Enterococcus (DNSE) [Reference Kelesidis3].

Arias et al. described mutations that set the genetic basis for in vivo daptomycin resistance in enterococci that were exposed to daptomycin [Reference Arias4]. These mutations may have originated from recombination between adjacent repetitive nucleotide sequences [Reference Arias4]. However, little is known about the mechanisms of development of daptomycin resistance in patients without prior exposure to daptomycin (de novo DNSE) [Reference Kelesidis5].

The genes encoding antibiotic resistance may derive from commensal bacteria that constitute a reservoir of resistance genes for pathogenic bacteria [Reference O'Brien6]. The level of resistance encountered in commensal bacteria may be a good indicator for selection pressure by antibiotic use and for resistance problems to be expected in pathogens [Reference O'Brien6].

Antibiotic use for animal growth promotion may hasten the appearance of antibiotic-resistant bacteria that, like zoonotic bacteria, might contaminate meat products and reach the intestinal tract of humans [Reference O'Brien6, Reference Johnston and Jaykus7]. Antimicrobial usage in animals has a major role in the selection of bacterial resistance and the transport of resistance genes via the food chain to humans [Reference O'Brien6, Reference Johnston and Jaykus7]. These resistant bacteria can transfer their antibiotic resistance genes, located on mobile genetic elements, to other bacteria, including human enterococci [Reference O'Brien6, Reference Johnston and Jaykus7].

Enterococci are members of the gastrointestinal tract consortium in humans and most other organisms [Reference van den Bogaard and Stobberingh8, Reference Zhang9]. Acquired resistance in Enterococcus spp. is mediated by transferable transposons or plasmids encoding resistance cassettes [Reference van den Bogaard and Stobberingh8, Reference Zhang9]. Multidrug-resistant enterococci can be found in food and animal species [Reference van den Bogaard and Stobberingh8, Reference Zhang9]. Previous studies have shown that food and animal species other than E. faecium and E. faecalis can efficiently transfer antibiotic resistance to human strains in inter-specific matings [Reference van den Bogaard and Stobberingh8, Reference Zhang9]. Of note, vancomycin-resistant enterococci emerged in farm animals in Europe, but became widespread in US hospitals within just a few years [Reference van den Bogaard and Stobberingh8, Reference Zhang9]. The potential development of environmental reservoirs of antibiotic resistance in farmland is a concern [Reference Johnston and Jaykus7, Reference van den Bogaard and Stobberingh8]. Thus, a possible mechanism of resistance in daptomycin-resistant enterococci could be the transfer of antibiotic resistance genes encountered in animal products [Reference Kelesidis5]. In addition, the daptomycin-resistant enterococci may have developed in animals with the original daptomycin-resistant strains being passed to humans via the food chain [Reference Kelesidis5].

In a recent study, Enterococcus spp. were frequently isolated from beef products (up to 62%) and up to 25% of these isolates were resistant to daptomycin [Reference Zhang9]. Of note, in a recent series of nine patients with de novo DNSE infections, three (33·3%) patients had a history of prior exposure to livestock and four (44·4%) patients reported frequent ingestion of beef [Reference Kelesidis5]. Clonal spread was not detected in this series, suggesting a large role of gene transfer in the dissemination of antibiotic resistance [Reference Kelesidis5]. We have also reported cases of DNSE E. gallinarum, which are common intestinal commensal bacteria in poultry [Reference Kelesidis3, Reference Kelesidis5, Reference Kelesidis10]. Interestingly, in our recent cohort of 11 patients with DNSE isolated from the urinary tract, all three de novo DNSE isolates in the urine were E. faecalis (T. Kelesidis et al. unpublished data). The importance of E. faecalis as a reservoir of resistance genes and their potential transfer to humans through consumption of contaminated undercooked meat, which can be a reservoir for DNSE isolates [Reference Kelesidis5, Reference Zhang9] has recently been validated [Reference Aslam1]. However, these observations need to be validated in further studies and their significance remains unclear. The origin of de novo community-acquired DNSE urinary isolates remains to be determined.

To safeguard public health, the selection and dissemination of resistant bacteria from animals should be controlled. It is possible that transport of gene elements of daptomycin resistance from food and animal Enterococcus spp. to human strains is a mechanism of development of de novo daptomycin resistance in enterococci. The findings from Geenen et al. indicate that people worldwide in contact with live broilers are at risk for MRSA carriage [Reference Geenen2] and it should also be investigated whether such epidemiological exposures place these subjects at increased risk for DNSE carriage.

Declaration of Interest

None.

References

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