|Pigs as source of methicillin-resistant Staphylococcus aureus CC398 infections in humans, Denmark.|
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|PMID: 18760004 Owner: NLM Status: MEDLINE|
|An emerging subtype of methicillin-resistant Staphylococcus aureus (MRSA), clonal complex (CC) 398, is associated with animals, particularly pigs. We conducted a matched case-control and a case-case study comparing 21 CC398 case-patients with 2 controls randomly selected from the Danish Civil Registry and 2 case-patients infected with MRSA other than CC398. On farms of case-patients, animals were examined for MRSA. Thirteen case-patients reported pig exposure. Living or working on farms with animals was an independent risk factor for CC398 in the case-control (matched odds ratio [MOR] 35.4, 95% confidence interval [CI] 2.7-469.8) and the case-case study (MOR 14.5, 95%CI 2.7-76.7). History of hospitalization was associated with an increased risk only in the case-control study (MOR 11.4, 95% CI 1.4-94.8). A total of 23 of 50 pigs on 4 of 5 farms were positive for CC398. Our results, corroborated by microbiologic testing, demonstrate that pigs are a source of CC398 in Denmark.|
|Hannah C Lewis; Kåre Mølbak; Catrin Reese; Frank M Aarestrup; Mette Selchau; Marit Sørum; Robert L Skov|
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|Type: Journal Article; Research Support, Non-U.S. Gov't|
|Title: Emerging infectious diseases Volume: 14 ISSN: 1080-6059 ISO Abbreviation: Emerging Infect. Dis. Publication Date: 2008 Sep|
|Created Date: 2008-09-01 Completed Date: 2008-12-02 Revised Date: 2009-11-18|
Medline Journal Info:
|Nlm Unique ID: 9508155 Medline TA: Emerg Infect Dis Country: United States|
|Languages: eng Pagination: 1383-9 Citation Subset: IM|
|Statens Serum Institut, Copenhagen, Denmark.|
|APA/MLA Format Download EndNote Download BibTex|
Denmark / epidemiology
Staphylococcal Infections / epidemiology, microbiology*
Staphylococcus aureus / drug effects*
Journal ID (nlm-ta): Emerg Infect Dis
Journal ID (publisher-id): EID
Publisher: Centers for Disease Control and Prevention
Print publication date: Month: 9 Year: 2008
Volume: 14 Issue: 9
First Page: 1383 Last Page: 1389
Publisher Id: 07-1576
PubMed Id: 18760004
|Pigs as Source of Methicillin-Resistant Staphylococcus aureus CC398 Infections in Humans, Denmark Alternate Title:Pigs as Source of MRSA CC398 Infections, Denmark|
|Hannah C. Lewis|
|Frank M. Aarestrup|
|Robert L. Skov|
|Statens Serum Institut, Copenhagen, Denmark (H.C. Lewis, K. M?lbak, M. Selchau, M. S?rum, R.L. Skov)
|European Programme for Intervention Epidemiology Training (H.C. Lewis)
|Vejle Hospital, Vejle, Denmark (C. Reese)
|Technical University of Denmark, Copenhagen (F.M. Aarestrup)
|Correspondence: Address for correspondence: Robert L. Skov, Epidemiology Department, Statens Serum Institut, Artillerivej 5, 2300 K?benhavn S. Copenhagen, Denmark; email: firstname.lastname@example.org
Methicillin-resistant Stapylococcus aureus (MRSA) is becoming increasingly recognized among persons in the community without established risk factors (1,2). MRSA primarily causes human disease and animals have not, until now, been considered a source of infection.
It has recently become apparent that animals, particularly pigs, can constitute a separate MRSA reservoir and be a source of a novel and rapidly emerging type of MRSA in humans; namely MRSA clonal complex (CC)398 by multilocus sequence typing (MLST) (3). MRSA CC398 consists of 8 MLST types (www.saureus.mlst.net), the predominant type being sequence type (ST)398, and a range of closely related protein A (spa) gene types (i.e., t011, t034, t108, and t1793) (4,5).
Although transmission appears to be primarily between animals, indistinguishable isolates have been found in their human contacts, particularly those with occupational exposure (3?7). MRSA CC398 (ST398) was first detected in 4 pigs and 1 healthy pig farmer in France (3,8). Clinical infection was described in the daughter of a pig farmer in the Netherlands in 2004 (7). That study showed that 23% of pig farmers in a small survey in the same region were seropositive for MRSA CC398.
Denmark has a low incidence of MRSA. In 2006, only 706 new MRSA patients (colonization only or infection) were reported, which corresponds to 13/100,000 population (9). To maintain this status, Denmark has adopted a strict ?Search and Destroy? policy, which includes active screening of at-risk persons at admission to a hospital (10). Prompted by reports from the Netherlands, we identified a small (<1% of all MRSA patients) but increasing number of MRSA CC398 human patients after 2003. Furthermore, CC398 was detected in a pig in Denmark in 2006 (11). With an annual production of ?25 million slaughter pigs (www.dst.dk), Denmark has a large potential reservoir for MRSA CC398.
We report results of an analytical study of MRSA CC398, in parallel with systematic farm and microbiologic investigations, to identify risk factors for MRSA CC398 acquisition in persons in Denmark. Although farm and pig exposure have been postulated as risk factors after interviews with MRSA CC398 patients in other studies (4,6,7,12), no previous study has included interviews with control populations to determine if these exposures were higher than would be expected in the general population.
In Denmark, MRSA isolates from all human patients have been referred to Statens Serum Institut since 1988 for characterization and national surveillance. Epidemiologic and clinical information has been obtained prospectively since 1999 on all patients.
We conducted a matched case?control study comparing human case-patients with MRSA CC398 during 2004?2007 with 2 population controls. In parallel, we conducted a case?case study comparing the same MRSA CC398 case-patients to 2 case-patients of community-detected MRSA of a type other than CC398 (non-CC398 case-patients). Eligible case-patients were persons with a confirmed diagnosis of MRSA with spa types related to CC398 (carriage or infection) during the study period: October 29, 2003 (first human diagnosed) to May 31, 2007. Where household clusters were identified, secondary case-patients were excluded from the study. Population controls were selected randomly from the Danish Civil Registry System and matched by sex, date of birth, and residence in the same municipality. Non-CC398 case-patients were selected from the national MRSA database and matched by sex, residence in the same region (Zealand, Jutland, or Funen), age group (? 10 years for adults and ? 3 years for persons <18 years of age) according to whether infected or a carrier, and similar time of diagnosis (90% ? 4 months) to limit differential recall bias. When >2 non-CC398 MRSA case-patients were identified within ? 4 months of diagnosis of the case-patient, 2 were randomly selected from the list generated.
After written informed consent was obtained, case-patients, controls, and non-CC398 case-patients were interviewed by using a structured telephone-administered questionnaire. Questions captured demographic and clinical data as well as information on known/identified risk factors for MRSA (including hospitalization and other medical exposures, contact sports, and travel) and hypothesized farm and animal exposures for MRSA CC398 (including living or working on a farm, exposure to farm animals, contact with farm workers, preference for eating, and contact with pets) in the year before case-patient diagnosis. Data were double-entered into Epidata version 3.1 (Statens Serum Institut, Copenhagen, Denmark) and collected and handled according to the requirements of the Danish Data Protection Agency. The study did not require ethical approval.
Univariable and multivariable conditional logistic regression analyses were conducted to estimate matched odds ratios (MORs). Unmatched logistic regression was used for variables for which MORs could not be calculated because not enough controls were exposed to MRSA. Multivariable conditional logistic regression analysis included significant variables (based on a p value of 0.05) from univariable analysis. Stepwise exclusion was used, and variables were tested for significance by using the likelihood ratio test. Stata version 9.2 software (StataCorp, College Station, TX, USA) was used for all analyses.
For case-patients, controls, and non-CC398 case-patients reporting contact with production animals, the farm owner was contacted. If the owner consented, nasal swabs were taken from 10 randomly selected animals (from 10 different pens where possible) and tested for MRSA.
Human isolates were tested by using PCR to identify the mecA gene (13), pulsed-field gel electrophoresis (PFGE) with the Harmony protocol (14), spa typing (15), and staphylococcal cassette chromosome mec (SCCmec) typing (16). Isolates were also tested for lukF/lukS genes encoding Panton-Valentine leukocidin (PVL) (17). Results of PFGE and spa typing were interpreted by using BioNumerics version 4.6 software (Applied Maths, Sint-Martens-Latem, Belgium). Because spa typing is acknowledged as being a proxy for MLST, the MLST clonal complex annotation was inferred on the basis of spa types. One of the human isolates was typed by MLST for confirmation. Furthermore, a random selection of 7 isolates were tested by PCR for the exotoxin genes tst, eta, and etb encoding staphylococcal toxic shock syndrome toxin 1, exfoliative toxin A, and exfoliative toxin B, respectively (18).
Animal swabs were plated directly on CHROM-MRSA agar (Becton Dickinson, Heidelberg, Germany) and blood agar (containing 5% bovine blood) and subsequently placed in selective broth (tryptic soy broth, 2.5% salt, aztreonam [20 mg/L], and cefoxitin [3.5 mg/L]; SSI Diagnostika, Hiller?d, Denmark). After incubation for 24 hours, the CHROM-MRSA agar was inspected for putative MRSA. Subcultivation on CHROM-MRSA was conducted with samples from the enrichment broth. Possible MRSA colonies were subcultivated on blood agar plates, identified by PCR for the mecA gene (13), and subjected to spa typing and SCCmec typing.
Human and animal isolates underwent antimicrobial drug susceptibility testing by using disc diffusion (D) with Neosensitabs (Rosco, Taastrup, Denmark) on Danish blood agar (SSI Diagnostika) or microbroth dilution (M) (19). Susceptibility tests were performed for tetracycline (D and M), erythromycin (D and M), streptomycin (D and M), kanamycin (D), norfloxacin (D), pencillin (D), clindamycin (D), fusidic acid (D), rifampicin (D), cefoxitin (D), ceftiofur (M), chloramphenicol (M), ciprofloxacin (M), florfenicol (M), spectinomycin (M), sulfamethoxazole (M), tiamulin (M), and trimethoprim (M).
Thirty-one case-patients with MRSA with spa types related to MRSA CC398 were detected from October 29, 2003, through February 16, 2007. Of these, 6 were excluded from the study because they were secondary case-patients (3 family clusters). Of the remaining eligible case-patients, we were unable to interview 4 because of a death (n = 1) and refusal to participate (n = 3). The questionnaire was therefore administered to 21 of 25 primary case-patients. Median age of the case-patients was 29 years (age range 8 months to 80 years), and 13 (62%) were female. Three case-patients reported having Dutch relatives, and 2 case-patients had a connection to the People?s Republic of China; 1 case-patient was an adopted child from China and another case-patient had adopted a child from China.
Ten case-patients (48%) reported having had an infection, of which all were skin and soft tissue infections. Moreover, sinusitis developed in 1 case-patient, and a severe invasive infection with multiorgan failure after knee surgery developed in another case-patient.
Several exposure variables related to farms and animals were associated with CC398 in the case?control and case?case studies (Table 1). Case?control analysis also identified 4 medical-related risk factors (Table 1). No association was found in the case?control and case?case studies for the following exposures: travel 12 months before diagnosis, working in the healthcare sector, contact with primary healthcare sector (doctor, specialist), visiting an emergency department, presence of a person in the household with a skin condition, presence of a person in the household with staphylococcal infection, smoking daily, contact sports, owning or having contact with dog(s) or horse(s), preference for eating pork, and being born outside Denmark.
Logistic regression models were applied separately to the case?control and case?case studies. In both studies, the first model only included farm and animal-related exposures: lived or worked on a farm with animals, worked with animals or meat, exposed to pigs, exposed to cattle, exposed to other farm animals, provided antimicrobial drugs to animals, owned cat(s), and had contact with any farm workers. Other farm and animal exposures were excluded because of colinearity. In both case?control and case?case studies, living or working on a farm with animals remained the independent association in this first model. A second model combined living or working on a farm with animals with medical-related exposures: contact with a person having a skin sore or other skin infection, history of hospital admission in the 12 months before diagnosis, antimicrobial drug use in the 12 months before diagnosis, and someone in the household with a chronic condition.
Living or working on a farm with animals was an independent risk factor for CC398 in the case?control study (MOR 35.4, 95% confidence interval [CI] 2.7?469.8) and the case?case study (MOR 14.5, 95% CI 2.7?76.7). A history of hospital admission in the 12 months before diagnosis was associated with an increased risk in the case?control study (MOR 11.4, 95% CI 1.4?94.8) but not in the case?case study.
Nine pig farms and 2 cattle herds, with which 10 case-patients had contact, were identified. One case-patient had contact with 2 pig farms, and 2 case-patients had contact with the same pig farm. No controls or non-CC398 case-patients had direct contact with a pig or cattle farm. The owners of 5 pig farms and of the 2 cattle herds agreed to participate in the study. The length of time between date of patient diagnosis and farm sampling was 2?24 months.
All but 1 of 31 human isolates were nontypeable by PFGE after digestion with SmaI. Twenty-nine isolates had spa type t034, including the isolate typeable by PFGE, and the other 2 were related variants of t034 (t108 and t1793). Because of the strong correlation between spa typing and MLST, all isolates could be assigned to CC398. One isolate (PFGE nontypeable, spa type t034) was typed by MLST and confirmed to be ST398. SCCmec typing showed that 24 isolates harbored SCCmec type V. SCCmec type IV was also found in 2 isolates (PFGE nontypeable, spa type t034). Three isolates were ccrAB2 positive, which indicated either a type II or type IV variant, but the mec class could not be determined. Two isolates were nontypeable. Isolates from the 21 case-patients were spa types t034 (SSCmec IV, n = 2, SSCmec V, n = 16, and a type II or type IV variant, n = 1, typeable by PFGE), t108 (SSCmec V, n = 1), and t1793 (SSCmec V, n = 1). These isolates showed considerable variation in antimicrobial drug resistance patterns; most isolates were resistant to tetracycline and erythromycin. All isolates from case-patients who reported exposure to pigs were tetracycline resistant and PVL negative. Two isolates were PVL positive; these were from case-patients who reported a connection to China. All isolates tested for exotoxin showed negative results for all toxins examined.
Twenty-three (46%) of 50 pigs on 4 of 5 sampled farms carried CC398 spa type t034. All isolates were resistant to tetracycline and trimethoprim. Pig isolates were indistinguishable or only differed by 1 additional antimicrobial drug class when compared with isolates from case-patients who had contact with them (Table 2). MRSA was not detected in the 2 cattle herds.
This study provides compelling epidemiologic and microbiologic evidence that persons living or working on farms in Denmark, particularly pig farms, are at increased risk of being colonized or infected with MRSA CC398. We provide evidence for pigs being a substantial reservoir of human MRSA CC398 in Denmark, as appears to be the case in other European countries such as the Netherlands and France (3,4,7,12), and in Canada (6).
In the case?case analysis, only animal and farm-related exposures were associated with being a case-patient, which indicates that these exposures are the major factors associated with CC398 acquisition. Furthermore, comparison of results from the case?control study (where farm/animal and medical-related variables remained associated) indicates that medical-related exposures are risk determinants for community-detected MRSA in general but not specifically for subtype CC398. This finding can be deduced because the design of the case?case analysis controls for exposures common to both groups, which means that these exposures will not be identified as a risk or might be underestimated (20).
Because of evidence of prolonged MRSA carriage (21), questions related to exposures referred to a period of 1 year before patient diagnosis. This lengthy recall period is a limitation of this study. However, all questions related to memorable activities and lifestyle choices; any bias introduced is therefore thought to be minimal.
Our finding that living or working on a farm with animals is associated with CC398 acquisition reinforces results of studies in France, the Netherlands, and Canada that indicated that CC398 is transmissible from animals to humans (3,4,6,7). Also in the Netherlands, a CC398 prevalence of 3.9% in 179 veterinarians has been described; all positive persons had recent or regular contact with pigs and cows (22). Screening participants from 38 countries at a veterinary conference in Denmark in 2006 found a CC398 prevalence of 9.6% (26/272); the highest prevalence was in German and Dutch delegates (23). In comparison, the prevalence of CC398 among delegates attending several national animal conferences in Denmark was 0.7% (4/576) (24).
Pig isolates from contact herds were indistinguishable, or only differed by 1 additional antimicrobial drug class, from the isolates from human case-patients who worked or lived on farms where these pigs were located. These samples were obtained months, in some cases years, after the human case-patient?s infection was diagnosed, findings that lend weight to the hypotheses that CC398 carriage in animals is unlikely to be transient and that animals are a reservoir of CC398. Although we isolated CC398 from 23 pigs on 4 of 5 pig farms, but not from cattle farms, this type may not be exclusive to pigs. CC398 has been shown to have a prevalence of 39% in pigs in the Netherlands (25). However, it has also been found in horses and dogs in Germany and Austria (5) and in cattle and poultry in the Netherlands (26,27). These findings are particularly interesting because S. aureus is usually host specific (28).
Our study has highlighted other important human epidemiologic aspects of CC398. The clinical picture for CC398, with ?50% of case-patients having had an infection and all reporting skin and soft tissue infections, is similar to that seen in community-acquired MRSA isolates in general (29,30). There was a serious invasive infection with MRSA reported in a man in Denmark after surgery on his knee; arthritis and multiorgan failure also developed (31). Serious complications from CC398 have also been described in other reports including ventilator-associated pneumonia (5) and endocarditis (32). Because no statistical association was found with travel abroad, this finding indicates that CC398 is endemic among pigs in Denmark. Nevertheless, there was an overrepresentation of case-patients or their family members who have had contact with another country, 2 with adopted children from China and 3 case-patients with relatives from the Netherlands. Likewise, in the Netherlands, a child adopted from China was found to be an MRSA CC398 carrier in 2004 (12). Three family clusters were identified in the present study, which indicates that CC398 can be transmitted from person to person. This finding is not surprising because of the adaptability of MRSA. Its potential for transmission between humans has also been observed in the Netherlands (4,7). MRSA has been isolated from dairy products, beef, chicken and pork (33?37) and although foodborne transmission is plausible (34), the risk is thought to be low. Preference for eating pork was not associated with being a CC398 case-patient in our study.
A high degree of variability in the types of CC398 (resistance patterns, spa types, and SCCmec types) suggests that this type is either rapidly evolving or emerging from a hitherto unrecognized reservoir. In the latter case, CC398 must have been introduced into Denmark on more than 1 occasion or by various routes to explain the high degree of variance. When one considers the rapid adaptability of MRSA, it may only be a matter of time before we see an increased prevalence of CC398 in humans, including those in hospitals as has been recently reported in the Netherlands (12). A high prevalence of tetracycline resistance in CC398 patients in contact with pigs has also been observed in the Netherlands; this finding suggests that use of tetracyclines and possibly other antimicrobial drugs in food animals is selecting these multidrug-resistant bacteria (25). Two case-patients who were positive for PVL had direct connections to China. To our knowledge, there are no published reports of CC398 patients in China but isolates from pigs have recently been reported from Singapore, with Indonesian origin (38).
In conclusion, transmission of CC398 from a zoonotic reservoir to humans could undermine existing MRSA control programs. We therefore recommend increased awareness among healthcare professionals that animals are a possible source of MRSA infection and that the potential for person-to-person spread exists. To limit further spread, pig farmers may warrant screening and isolation on admission to hospitals as has been implemented in the Netherlands (39). However, further studies are required to better understand the human and veterinary epidemiology of this emerging zoonosis. Areas of study should include size of the reservoir in pigs, whether other animals constitute a reservoir of CC398, and how frequently CC398 is transmitted from animals to humans and from humans to humans. The European Union baseline survey on the prevalence of MRSA in breeding pigs, initiated in January 2008, is an important step in addressing the first of these points (40).
Suggested citation for this article: Lewis HC, M?lbak K, Reese C, Aarestrup FM, Selchau M, S?rum M, et al. Pigs as source of methicillin-resistant Staphylococcus aureus CC398 infections in humans, Denmark. Emerg Infect Dis [serial on the Internet]. 2008 Sep [date cited]. Available from http://www.cdc.gov/EID/content/14/9/1383.htm
This study was supported by the Statens Serum Institut.
Ms Lewis is a fellow with the European Programme for Intervention Epidemiology Training at the Statens Serum Institut in Copenhagen. Her primary research interest is intervention epidemiology, particularly in relation to zoonoses.
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|Exposure variable||No. (%) case-patients exposed (n = 21)||Odds ratio (95% confidence interval) for MRSA infection
|Case?control study, population controls (n = 42)||Case?case study, non-CC398 case-patients (n = 39)|
|Animal and farm-related exposures|
|Lived or worked on farm with animals||14 (67)||22.1 (2.9?170.3)||11.6 (2.6?51.7)|
|Worked with animals or meat||11 (50)||16.2 (2.0?127.8)||??|
|Worked on farm with animals||10 (48)||??||??|
|Lived on farm with animals||9 (43)||6.9 (1.5?32.8)||7.9 (1.7?36.7)|
|Exposure to pigs||13 (62)||??||??|
|Exposure to cattle||6 (29)||??||??|
|Exposure to other farm animals (hens, goats, ? sh eep)||7 (33)||11.1 (1.4?92.4)||5.9 (1.2?28.8)|
|Provided antimicrobial drugs to animals||10 (48)||??||??|
|Contact with farm workers||16 (76)||5.2 (1.4?19.3)||??|
|Contact with farmer||14 (67)||3.2 (1.0?10.6)||??|
|Contact with veterinarian||7 (33)||6.3 (1.3?30.7)||6.6 (1.4?31.8)|
|Lived in countryside||13 (62)||7.2 (1.5?33.8)||5.2 (1.4?18.9)|
|Had cat in home||11 (50)||3.2 (1.0?10.6)||3.4 (1.1?9.9)|
|Used manure in garden||7 (33)||3.2 (0.9?11.0)||6.6 (1.4?31.8)|
| Visited farm, zoo, or stables
|Admission to hospital in 12 mo before? diagnosis||13 (62)||6.8 (1.9?24.4)||1.5 (0.4?5.2)|
|Someone in household with chronic condition||12 (57)||3.8 (1.2?12.5)||2.0 (0.8?9.3)|
|Antimicrobial drug use in 12 mo before ? diagnosis||9 (43)||3.4 (1.0?11.5)||2.6 (0.8?9.2)|
|Contact with person with skin sore or other ? skin infection||5 (26)||8.6 (1?74.9)||0.6 (0.2?1.9)|
*MRSA, methicillin-resistant Staphylococcus aureus; CC, clonal complex.??p<0.01, by unmatched analysis.
|Case-patient no.||Date of diagnosis||Resistance pattern||spa type||Contact herd||No. isolates||Resistance pattern||spa type|
||tet, ery, cli, str, tmp
||tet, ery, cli, str, spe, tmp
|2||2005 Oct||tet, tmp||t034||B||5||tet, tmp||t034|
|4||tet, str, tmp||t034|
||tet, str, tmp
|3||2006 Oct||tet, ery, cli, str, spe, tmp||t034||C||1||tet, ery, cli,str, spe, tmp||t034|
||tet, str, spe, tmp
|4||2006 Nov||tet, kan, str, spe, tmp||t034||D||1||tet, ery, cli, kan, str, spe, tmp||t034|
*spa, staphylococcal protein A; tet, tetracycline; ery, erythromycin; cli, clindamycin; str, streptomycin; tmp, trimethoprim; spe, spectinomycin; kan, kananmycin.
Keywords: Keywords: Staphylococcus aureus, methicillin resistance, community-acquired infections, epidemiology, case-control studies, animals, domestic swine (pig), CC398, research.
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