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Fecal Colonization with Vancomycin-Resistant Enterococci in Australia.


To assess the rate of fecal vancomycin-resistant enterococci enterococci

bacteria in the genus Enterococcus.
 (VRE VRE

vancomycin-resistant enterococcus.

VRE Vancomycin-resistent enterococcus, see there
) colonization in Australia, we examined specimens from 1,085 healthy volunteers. VRE was cultured from 2 (0.2%) of 1,085 specimens; both were vanB Enterococcus faecium Enterococcus faecium A nosocomial pathogen resistant to most antibiotics–eg, penicillin, teicoplanin, aminoglycosides, glycopeptides; ID of E faecium in a clinical specimen requires Pt isolation with barrier precautions. , identical by pulsed-field gel electrophoresis, but with a pattern rare in Melbourne hospitals.

Colonization and infection with vancomycin-resistant enterococci (VRE) are emerging worldwide. In Europe, agricultural use of the glycopeptide growth promoter avoparcin has been implicated im·pli·cate  
tr.v. im·pli·cat·ed, im·pli·cat·ing, im·pli·cates
1. To involve or connect intimately or incriminatingly: evidence that implicates others in the plot.

2.
 in the emergence of vanA VRE in the food chain (1), and fecal colonization rates of 2%-28% have been reported in some communities (2,3). In the United States, where avoparcin is not used, both vanA and vanB VRE strains appear to be largely nosocomially spread, with fecal VRE colonization rare in nonhospitalized patients (4,5). By contrast, in Australia, where avoparcin has been used widely (10,000 kg/year) in agriculture for many years (6) and the per capita [Latin, By the heads or polls.] A term used in the Descent and Distribution of the estate of one who dies without a will. It means to share and share alike according to the number of individuals.  consumption of antibiotics is one of the highest in the world (7), VRE (mostly vanB [8]) has only recently emerged as an important nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital.

nos·o·co·mi·al
adj.
1. Of or relating to a hospital.

2.
 pathogen. We assessed the rate of fecal VRE colonization in a population of healthy Australians.

The Study

In mid-1997, fecal specimens from 1,085 healthy volunteers were collected and frozen at -70 [degrees] C as baseline specimens for a water quality study in Melbourne, Australia. These previously described (9) volunteers were from 294 families with young children who lived in a lower- to middle-class suburb. They were specifically chosen because they were representative of young Australian families in eating habits and medical care. Thus, the elderly, the unmarried, and the very poor were not represented. Study participants had no history of diarrhea or antibiotic use at the time of specimen collection.

For VRE screening, frozen samples were thawed and spread onto enterococcosel agar (BBL "Be back later." See digispeak.

(chat) BBL - (I will) be back later.
 Microbiology Systems, Cockeysville, MD) containing 6 [micro]g/mL vancomycin and incubating at 35 [degrees] C for 48-72 hours. Each sample was also incubated in enterococcosel broth (BBL) without vancomycin for 48 hours, before being spread onto enterococcosel agar containing 6 [micro]g/mL vancomycin. From esculin-positive colonies, three of each morphologic appearance were selected from the direct agar and the subcultured enterococcosel broth cultures of each specimen and provisionally identified as either Enterococcus faecium or E. faecalis by routine criteria (gram-positive cocci cocci /coc·ci/ (kok´si) plural of coccus.

cocci

[L.] plural of coccus.
, L-pyrrolidonyl-[Beta]-naphthylamide hydrolase-positive, nonmotile, catalase-negative, and pigment-negative) (10,11). All isolates fulfilling these criteria were assessed for susceptibility to vancomycin and teicoplanin by the E-test method (AB Biodisk, Dalvagen, Sweden). Isolates with an MIC to vancomycin [is greater than or equal to] 2 [micro]g/mL were analyzed for the presence of vanA, B, C1, or C2/3 genes by polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is  (8); if vanA- or vanB-positive, they were then confirmed as either E. faecium or E. faecalis by automated biochemical analysis (BioMerieux Vitek Inc., MO) and by polymerase chain reaction, and were assessed by pulsed-field gel electrophoresis (PFGE PFGE Pulsed-Field Gel Electrophoresis ) (8,12,13).

To be certain that this analysis of frozen specimens was a valid assessment of the rate of fecal VRE carriage in this population, two additional studies were conducted. First, to verify that -70 [degrees] C storage did not affect the overall recovery of enterococci, a randomly selected subset of 112 of the 1,085 specimens were cultured on enterococcosel agar (BBL) without antibiotic and assessed for enterococci by routine identification techniques (10,11). In addition, to assess whether -70 [degrees] C storage could selectively impair recovery of VRE, fresh fecal specimens were spiked with concentrations ([10.sup.4]-[10.sup.8]/mL) of isolates of E. faecalis (vanA, n-l, vanB, n=2) or E. faecium (vanA, n=2; vanB, n=2), then stored at -70 [degrees] C for 2 weeks before being thawed and cultured.

Results

Enterococci were identified in 106 of the subset of 112 specimens, a rate consistent with previous reports (14). VRE were also consistently recovered from our frozen spiked specimens. These findings suggest that -70 [degrees] C storage of specimens does not affect the recovery of enterococci in general, or VRE in particular.

In the community study, VRE was isolated from 2 (0.2%) of the 1,085 (95% confidence intervals 0%-0.4%) specimens. Both isolates were vanB E. faecium and were detected in both agar and broth cultures. E-test MIC results at 24 hours for both isolates were 12 [micro]g/mL for vancomycin and 0.125 [micro]g/mL for teicoplanin. Although they were identical by PFGE, they displayed a PFGE pattern that is uncommon among VRE isolates from Melbourne hospitals. The two participants who were vanB E. faecium positive were not related. One was a 34-year-old man and the other a 30-year-old woman; both were married, and each had two children. None of the other family members had detectable fecal VRE colonization. The man had a history of stable ulcerative colitis ulcerative colitis

Inflammation of the colon, especially of its mucous membranes. The inflamed membranes develop patches of tiny ulcers, and the diarrhea contains blood and mucus.
 and was receiving sulfasalazine sulfasalazine /sul·fa·sal·a·zine/ (-sal´ah-zen) a sulfonamide used in the treatment and prophylaxis of inflammatory bowel disease and the treatment of rheumatoid arthritis. .

Conclusions

This study suggests that fecal colonization with VRE is present but uncommon in Australia. Despite widespread agricultural use of avoparcin and high community rates of antibiotic use, vanA E. faecium was not identified, vanB E. faecium, which is the most common clinical VRE strain in Australia (8) and whose nosocomial transmission remains a concern (15), was identified in healthy Australians.

Acknowledgments

The authors thank the staff' at the Microbiological Diagnostic Unit, University of Melbourne
  • AsiaWeek is now discontinued.
Comments:

In 2006, Times Higher Education Supplement ranked the University of Melbourne 22nd in the world. Because of the drop in ranking, University of Melbourne is currently behind four Asian universities - Beijing University,
, for the PFGE analysis.

Funding for this project was provided by the Department of Infectious Diseases and Clinical Epidemiology, Monash Medical Centre Monash Medical Centres (MMC) is a multicampus teaching hospital in Melbourne, Victoria, Australia. The Clayton campus is in Clayton, the Moorabbin Campus at East Bentleigh. It provides specialist care to the State's south-east. .

References

(1.) Wegener HC, Aarestrup FM, Jensen LB, Hammerum AM, Bager F. Use of antimicrobial growth promoters in food animals and Enterococcus faecium resistance to therapeutic antimicrobial drugs in Europe. Emerg Infect Dis 1999;5:329-35.

(2.) Endtz HP, van den Braak N, van Belkum A, Kluytmans JA, Koeleman JG, Spanjaard L, et al. Faecal fae·cal  
adj. Chiefly British
Variant of fecal.

Adj. 1. faecal - of or relating to feces; "fecal matter"
fecal
 carriage of vancomycin-resistant enterococci in hospitalized patients and those living in the community in the Netherlands. J Clin Microbiol 1997;35:3026-31.

(3.) Van der Auwera P, Pensart N, Korten V, Murray BE, Leclercq R. Influence of oral glycopeptides on the fecal flora of human volunteers: selection of highly glycopeptide-resistant enterococci. J Infect Dis 1996;173:1129-36.

(4.) Coque T, Tomayko JF, Ricke SC, Okhyusen PC, Murray BE. Vancomycin-resistant enterococci from nosocomial community and animal sources in the United States. Antimicrob Agents Chemother 1996;40:2605-9.

(5.) Eliopoulos GM. Vancomycin-resistant enterococci: Mechanism and clinical relevance. Infect Dis Clin North Am 1997;11:851-65.

(6.) Report of the Joint Expert Technical Advisory Committee on Antibiotic Resistance antibiotic resistance,
n the ability of certain strains of microorganisms to develop resistance to antibiotics.

antibiotic resistance 
 (JETACAR). The use of antibiotics in food-producing animals: antibiotic-resistant bacteria in animals and humans. Australia: Commonwealth Department of Health and Aged Care. Commonwealth Department of Agriculture, Fisheries and Forestry. Australia; 1999.

(7.) McManus P, Hammond ML, Whicker SD, Primrose JG, Mant A, Fairall SR. Antibiotic use in the Australian community, 1990-1995. Med J Aust 1997;167:124-7.

(8.) Bell JM, Paton JC, Turnidge J. Emergence of vancomycin-resistant enterococci in Australia: phenotypic and genotypic characteristics of isolates. J Clin Microbiol 1998; 36:2187-90.

(9.) Hellard ME, Sinclair MI, Hogg GG, Fairley CK. Prevalence of enteric enteric /en·ter·ic/ (en-ter´ik) within or pertaining to the small intestine.

en·ter·ic
adj.
1. Of, relating to, or within the intestine.

2.
 pathogens among community based asymptomatic individuals. J Gastroenterol Hepatol 2000; 15:290-3.

(10.) Facklam RR, Collins MD. Identification of Enterococcus enterococcus /en·tero·coc·cus/ (en?ter-o-kok´us) pl. enterococ´ci   an organism belonging to the genus Enterococcus.
Enterococcus /En·tero·coc·cus/ (
 species isolated from human infections by a conventional test scheme. J Clin Microbiol 1989;27:731-4.

(11.) Facklam RR, Sahm DF, Teixeira LM. Enterococcus. In: Murray PR, Baron EJ, Pfaller MA, Tenover FC, Yolken YH, editors. Manual of clinical microbiology--1999. Washington: American Society for Microbiology The American Society for Microbiology (ASM) is a scientific organization, based in the United States although with over 43,000 members throughout the world. It is the largest single life science professional organization and its members include those whose interests encompass basic ; 1999. p. 297-305.

(12.) Dutka-Malen A, Evers S, Courvalin P. Detection of glycopeptide resistance genotypes and identification to the species level of clinically relevant enterococci by PCR PCR polymerase chain reaction.

PCR
abbr.
polymerase chain reaction


Polymerase chain reaction (PCR) 
. J Clin Microbiol 1995;33:24-7.

(13.) Miranda AG, Singh KV, Murray BE. A fingerprinting of Enterococcusfaecium by pulsed-field gel electrophoresis may be a useful epidemiologic tool. J Clin Microbiol 1991; 29:2752-7.

(14.) Murray BE. The life and times of the Enterococcus. Clin Microbiol Rev 1990;3:46-65.

(15.) Grayson M, Grabsch EA, Johnson PDR PDR

A trademark for Physicians' Desk Reference, a group of reference books containing drug listings, especially one for prescription drugs.


PDR 
, Olden old·en  
adj.
Of, relating to, or belonging to time long past; old or ancient: olden days.



[Middle English : old, old; see old + -en, adj.
 D, Aberline M, Li HY, et al. Outcome of a screening program for vancomycin-resistant enterococci (VRE) in a hospital in Victoria. Med J Aust 1999;171:133-6.

Address for correspondence: Alexander Padiglione, Infectious Diseases & Clinical Epidemiology Department, Monash Medical Centre, 246 Clayton Rd., Clayton, Victoria, Australia 3168; fax: +61-3-9594-4533; e-mail: alex.padiglione@med.monash.edu.au.

Alexander A. Padiglione,(*)([dagger]) Elizabeth A. Grabsch,(*) Dianne Olden,(*) Margaret Hellard,([dagger]) Martha I. Sinclair,([dagger]) Christopher K Fairley,([dagger]) and M. Lindsay Grayson(*)([dagger])

(*) Monash Medical Centre, Melbourne, Australia; ([dagger]) Monash University, Melbourne, Australia

Dr. Padiglione is an infectious diseases physician at the Monash Medical Centre and a member of the Department of Epidemiology and Preventative Medicine, Monash University, Melbourne, Australia.
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Author:Grayson, M. Lindsay
Publication:Emerging Infectious Diseases
Geographic Code:8AUST
Date:Sep 1, 2000
Words:1439
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