Human invasiveness

S. aureus is by far the most important pathogen in SSTI including SSIs. Life-threatening nosocomial infections such as pneumonia and septicaemia also occur. Treatment of invasive infections largely relies on antimicrobial agents (antimicrobials), in this respect penicillinase-stable β-lactams (isoxazolylpenicillins, cephalosporins) are of utmost importance for human medicine. Resistance to these agents drastically limits therapeutic options and is a worldwide emerging problem [Reference de Lencastre, Oliveira and Tomasz6]. It should be noted that in this document the applied definition of an antimicrobial does not include commonly used local antiseptics and disinfectants, e.g. chlorhexidine, alcohol, or soaps.

S. aureus can also produce toxins associated with food intoxications. Other rare but severe syndromes including toxic shock syndrome (TSS) have also been documented [Reference Morgan7].

Epidemiological definitions of MRSA groups

S. aureus is intrinsically susceptible to β-lactam agents that inhibit cell-wall formation due to binding with proteins involved in the formation of peptidoglycan, as previously reviewed [Reference Haesebrouck8]. The mechanism of resistance to penicillinase-stable β-lactams including methicillin, isoxazolylpenicillins and cephalosporins in S. aureus (MRSA) is an altered target site due to an acquired penicillin-binding protein (PBP2a, also called PBP2′) encoded by the gene mecA.

Different types of MRSA may be distinguished based on epidemiological groupings. This can be a simplistic approach since in some cases strains of MRSA have spread between the groups [Reference Morgan7]. Thus it might be difficult to determine which epidemiological pattern a certain MRSA strain is associated with. The grouping is of relevance for the remainder of this document although only MRSA-related to animals will be discussed. It should be noted that virulence may differ between strains within groups and that toxin-producing strains may be found in any of the groups.

Emergence in animals

During the period 1970–2000, MRSA has been sporadically isolated from animals, in particular cows, small companion animals, and horses. With the exception of some equine isolates, the nature of these cases suggested a human origin and no epidemics have been reported [Reference Leonard and Markey1]. Thus, until the end of the 20th century both the scientific community and policy makers were convinced that animal husbandry was of little relevance to MRSA causing diseases in humans, but was rather a problem solely based on the antimicrobial use in human medicine [11]. The situation has now changed, with an increased number of reports on MRSA in livestock, especially swine and veal calves. MRSA has also been reported in companion animals and horses, as well as transmission between humans and animals. This has recently been reviewed [Reference Leonard and Markey1]. Sometimes distinct animal specific-lineages such as LA-MRSA have been involved [Reference Cuny12, Reference Voss13], but on many occasions human-associated MRSA genotypes have been identified [Reference Weese14]. A note of caution in assessing the impact of ‘animal’ MRSA in human infections is that the increased awareness of such organisms is likely to have influenced the concentration of studies dealing with MRSA in animals. Interpretation and comparisons over time and between studies should be carefully performed since different procedures and approaches (study design) may have influenced prevalences.

Zoonotic concerns

Persons in direct contact with MRSA-positive animals have been shown to have an increased risk of carrying the same MRSA strains as the animals. This has been observed in small-animal healthcare, equine hospitals and livestock environments [Reference Morgan7, Reference Weese14]. Severe manifestations of LA-MRSA in humans have been documented, including a recent outbreak in a Dutch hospital [Reference Declercq15, Reference Wulf16]. This emerging phenomenon represents a hazard that demands a bilateral management approach, taking both animals and humans as potential sources of MRSA.

Molecular typing

The mecA gene is located on the mobile staphylococcal chromosomal cassette (SCCmec), and six major types have been found (I–VI). SCCmec types I–III are the most common in HA-MRSA [Reference de Lencastre, Oliveira and Tomasz6]. These strains often carry additional plasmids or transposons enhancing the spread of resistance to two or more unrelated classes of antimicrobials (multiresistant). CA-MRSA typically harbour the smaller and possibly more mobile SCCmec type IV, and also type V, while multiresistance is less common. These strains often carry an exotoxin Panton–Valentine leukocidin (PVL) toxin; the pathogenicity of this toxin is still under debate [Reference Appelbaum17]. HA- and CA-MRSA cannot be strictly separated because genotypic CA-MRSA are reported with increasing frequency in the healthcare environment [Reference de Lencastre, Oliveira and Tomasz6, Reference David18]. LA-MRSA carry SCCmec types IV or V.

In addition to SCCmec typing which is relatively new and was discussed above, two important molecular-typing techniques for differentiation of MRSA are pulsed-field gel electrophoresis (PFGE) and multilocus sequence typing (MLST). In contrast to MLST, PFGE has the disadvantage of considerable variation of results between laboratories. MLST and PFGE can assist in ascertaining if strains are clonally related, but not all strains are typable with these methods. For example the typical LA-MRSA strain which belongs to sequence type (ST)398 resists digestion by the SmaI restriction enzyme by traditional PFGE and results are therefore not interpretable [Reference van Loo19]. Some reports call these strains untypable or non-typable MRSA (UT or NT-MRSA). Recent evolutions in the genome can alter the MLST profiles, and strains approaching a certain type are defined as belonging to a clonal complex (CC). Spa typing is an upcoming important genotyping method which can differentiate strains that are indistinguishable by PFGE or MLST. ST398 belongs to CC398, and examples of spa types found are t108, t011, t034 [Reference van Loo19]. The aforementioned and other techniques are under evaluation to increase the discriminative power especially with regard to MRSA ST398 [Reference Rasschaert20].

Throughout this document and unless otherwise specified, LA-MRSA is the preferred term used as a synonym for UT-MRSA, NT-MRSA, MRSA ST398, and MRSA CC398.

The term colonization or carriage as used in the document refers to an individual person or animal that tests positive for MRSA in swabs from nares or throat (or other body sites) due to multiplication and settlement of MRSA not causing clinical symptoms [5].

Occurrence in livestock

The first report of MRSA in livestock was a case of bovine mastitis in Belgium [Reference Devriese, Van Damme and Fameree21]. Although molecular-typing methods were not available, biotyping strongly suggested a human origin. Four decades later, investigations have found cattle also to be colonized by LA-MRSA, with 88% of farms positive in Dutch veal-calf rearing units [Reference Graveland22]. Only occasional reports exist on dairy farms but in one study in Belgium, up to 15% of lactating cows in herds with a previous history of MRSA were positive [Reference Vanderhaeghen23]. In general, the occurrence of MRSA in bovine mastitis isolates is well studied and its prevalence seems to be very low [Reference Hendriksen24].

In 2005, a high prevalence of LA-MRSA was found in Dutch pigs in slaughterhouses [Reference De Neeling25]. This study was undertaken following high colonization rates of pig farmers and relatives without known risk factors for MRSA [Reference Voss13]. Other reports have confirmed these findings in different countries, e.g. Denmark [Reference Guardabassi, Stegger and Skov26], Germany [Reference Meemken27], Canada [Reference Khanna28] and Belgium [Reference Denis29], and the predominant spa types found were t108, t034, and t011, all close relatives within CC398. The SCCmec element predominantly found was IV. In 2002 the isolation of this clone from pigs was reported in France for the first time, but the isolate was susceptible to methicillin (MSSA) [Reference Armand-Lefevre, Ruimy and Andremont30]. In a recent Canadian study [Reference Khanna28] an endemic HA-MRSA (US100) strain was found in pigs in addition to CC398. Of the cited porcine studies, the highest percentage of positive farms (living animals, not slaughterhouse) was found in Belgium with 34/50 fattening pig farms studied being positive (68%). Recent investigations from Asia have demonstrated that pig farms also can act as a reservoir for other sequence types of MRSA, e.g. ST9 in China [Reference Wagenaar31] and Malaysia [Reference Neela32].

In poultry, a Belgian study revealed a new spa type t1456 within CC398 to be present in 2/14 randomly selected broiler farms (14·3%), but it was not found in 10 layer farms [Reference Persoons33]. Similarly, Nemati et al. [Reference Nemati34] found 5/39 Belgian broiler farms (12·8%) to be positive for LA-MRSA (CC398).

A detailed overview on the occurrence in food-producing animals and derived products is provided elsewhere [5].

To date, clinical infections with LA-MRSA in food-producing animals have been described twice. The first report described a case of post-weaning dermatitis with 20% mortality in swine from The Netherlands, in which spa type t011 was found [Reference van Duijkeren35]. A second report showed LA-MRSA to be present in Belgian bovine clinical and subclinical mastitis isolates [Reference Vanderhaeghen23]. Thus far, the LA-MRSA strains in the living animal have not been reported to possess PVL [Reference Denis29, Reference van Duijkeren36]. On the contrary, in CC398 from predominantly healthy persons, a prevalence of 9·4% (3/32) of the PVL toxin was reported [Reference van Loo19] although an Asian subclone was suggested for these isolates [Reference Yu37]. Other MRSA clones harbouring PVL have nevertheless been found in living animals [Reference Morgan7].

Risk factors for colonization and infection in livestock

A causal relationship between the use of antibacterial drugs and MRSA has been demonstrated in human medicine for different antimicrobial compounds, e.g. quinolones, glycopeptides and β-lactams, in a recent meta-analysis [Reference Tacconelli38]. It is probable that similar conditions apply also to animals, particularly as LA-MRSA are often co-resistant to several other antimicrobials as indicated below.

An antimicrobial therapeutic regimen in the strict sense requires a diagnosis. However, many treated animals are not sick at the initiation of the antimicrobial regimen. First, prevention of mainly respiratory and digestive disorders can be done by treating the animals in a known risk period during the production cycle. In addition, healthy animals sharing the same space (barn) with diseased individuals may be treated. Many experts consider preventive therapy necessary in the modern livestock industry. Such practices are common in the majority of intensively reared animals like broilers, fattening pigs and veal calves. Of particular concern is that in preventive therapy, deviations from approved posology including underdosing and prolonged duration of treatment are common, and treatment is often initiated without diagnosis [Reference Timmerman39].

Since most LA-MRSA are resistant to tetracyclines (and trimethoprim) [Reference Kadlec and Schwarz40], an association between the use of antimicrobials in pig farming [Reference Timmerman39] and the widespread occurrence of MRSA has been hypothesized [Reference Wulf16, Reference De Neeling25]. Monitoring of antimicrobial consumption in The Netherlands [41] and Denmark [42] has revealed an increased use of tetracyclines during the last 5 years. So far there has been only one report demonstrating an association between the occurrence of MRSA in livestock and the use of antimicrobials. Van Duijkeren et al. [Reference van Duijkeren36] found the number of colonized pigs in farms applying oral group treatments, often with tetracyclines, to be higher compared to farms with no such use of antimicrobials. On the other hand, preliminary results from another ongoing porcine study found no such association [Reference Broens43]. The isolation of LA-MRSA in the case report of dermatitis in swine [Reference van Duijkeren35] was preceded by unsuccessful therapy with different antimicrobial classes including cephalosporins (ceftiofur and cefquinome), macrolides, and potentiated sulphonamides. Additional genetic resistance markers, including the multidrug resistance gene cfr, could speed up the emergence of MRSA ST398 due to co-selection [Reference Kehrenberg44].

S. aureus infections in veterinary medicine are seldom treated with β-lactamase-resistant penicillins. The exception is intramammary use of isoxazolylpenicillins, amoxicillin combined with clavulanic acid and cephalosporins for dairy cows. Despite this practice for several decades, the prevalence of MRSA in bovine S. aureus isolates has hitherto been low or absent [Reference Virgin45].

A lower prevalence of MRSA was found in sows compared to piglets and finishers in a Belgian survey. In addition this survey revealed a marked difference in the number of MRSA-positive animals between open (94%) and closed (56%) farms [Reference Denis29]. This is in line with a Dutch survey which indicated transmission of LA-MRSA within the production chain, e.g. from multiplier to finisher farms [Reference van Duijkeren36]. Piglets in multiplier farms can be colonized by different routes or vectors, and longitudinal studies are needed to indicate if the environment, e.g. feed or dust or the sows are the primary source of colonization [Reference De Neeling25].

Human contact hazard related to livestock

Epidemiological studies in The Netherlands have indicated that contact with veal calves or pigs was significantly associated with CC398 [Reference Voss13, Reference Van Rijen, Van Keulen and Kluytmans46]. In The Netherlands, farmers of swine and veal calves are now considered a defined risk group, and are screened upon admission to hospitals [Reference Wulf16].

The occupational hazard for LA-MRSA colonization through (the intensity of) pig contact has been confirmed in Belgian farmers [Reference Denis29], regional German investigations [Reference Meemken27] and at an international veterinarian conference in Denmark [Reference Wulf47]. Markedly, in two of the studies, current hygiene measures (e.g. wearing a mask) were not found to be protective for MRSA carriage [Reference Denis29, Reference Wulf47]. These findings were in contrast with conclusions drawn from a Canadian study on horse units [Reference Anderson, Lefebvre and Weese48]. Veterinary practitioners are at risk for MRSA, which is clearly demonstrated in countries with a low overall MRSA prevalence like Denmark [Reference Moodley49].

Infections of humans with LA-MRSA have been described since 2004 [Reference Voss13], with an increasing frequency in The Netherlands [Reference Van Rijen, Van Keulen and Kluytmans46] and Denmark [Reference Lewis50]. Examples of severe infections are an aggressive soft tissue infection of a pig-inflicted bite wound [Reference Declercq15] and endocarditis [Reference Ekkelenkamp51]. An outbreak in a surgical ward at a Dutch hospital has also been described [Reference Wulf16].

Occurrence in horses

The first report on the isolation of MRSA in horses was published in the 1990s; from 1989 to 1991 MRSA was isolated from 13 mares with metritis in Japan. The source was thought to be a stallion on a stud farm which 10 of the mares had visited. PFGE showed that the isolates had indistinguishable patterns [Reference Anzai52, Reference Shimizu53]. To date, MRSA has been isolated from horses in Europe, Asia and North America [Reference Shimizu53-Reference Weese and Rousseau60]. Wound and post-operative infections with MRSA tend to be most common [Reference Leonard and Markey1, Reference Anderson61].

Weese et al. [Reference Weese62] found that 5·3% of horses at a Canadian veterinary teaching hospital and 4·7% of horses on farms in Canada and the USA [Reference Weese63] were colonized with MRSA. Cuny et al. [Reference Cuny12] reported 24 MRSA infections in 768 clinical samples from horses at a veterinary teaching hospital in Austria and an estimated infection rate of 4.8 MRSA cases/1000 equine admissions. In a recent study investigating 110 horses presenting at a Belgian equine clinic 10·9% of the horses carried MRSA. All isolates in this latter study were LA-MRSA (non-typable by PFGE using SmaI digestion) and belonged to spa types t011 and t1451 [Reference van Den Eede59]. In the Netherlands, the percentage of MRSA isolates found in equine clinical samples at the Veterinary Microbiological Diagnostic Center of Utrecht University increased from 0% in 2002 to 37% in 2008. MRSA of spa type t064, belonging to MLST ST8 and spa types t011 and t2123, both belonging to the livestock-associated MLST ST398, predominated [Reference Van Duijkeren64]. In Sweden, one of 300 horses admitted to four equine clinics carried MRSA CC398 spa type t011 [65]. In an equine clinic in Belgium MRSA CC398 spa type t011 were isolated from various infections of 13 hospitalized horses [Reference Hermans66]. Busscher et al. [Reference Busscher, van Duijkeren and Sloet van Oldruitenborgh-Oosterbaan67] did not find any MRSA in 200 healthy horses in the community in The Netherlands, similarly no MRSA was detected in nasal samples of 300 healthy horses from 14 farms in Slovenia by Vengust et al. [Reference Vengust68]. MRSA colonization was also not identified in 497 healthy horses on farms in Atlantic Canada [Reference Burton69].

Risk factors for colonization and infection in horses

Antimicrobial administration within 30 days before admission to a veterinary teaching hospital has been demonstrated to be a risk factor for MRSA colonization in horses [Reference Weese and Lefebvre70]. Administration of ceftiofur or aminoglycosides during hospitalization was a risk factor associated with nosocomial MRSA colonization of horses [Reference Weese62].

Weese & Lefebvre [Reference Weese and Lefebvre70] evaluated factors associated with MRSA colonization of horses at the time of admission to a veterinary teaching hospital. Previous colonization of the horse, presence of colonized horses on the farm, admission to the neonatal ICU and admission to a service other than the surgical service were risk factors for community-associated colonization. Weese et al. [Reference Weese62] found that horses colonized at admission at a horse clinic were more likely to develop clinical MRSA infection than those not colonized at admission. The overall incidence rate of nosocomial MRSA colonization was 23/1000 admissions and that of nosocomial MRSA infection was 1·8/1000 admissions, with an incidence density of 0·88/1000 patient-days. Residence on a farm that housed more than 20 horses was a factor significantly associated with MRSA colonization [Reference Weese63]. In a retrospective multicentre study investigating MRSA infections in 115 horses, previous hospitalization and treatment with gentamicin were associated significantly with CA-MRSA, whereas infected incision sites were associated significantly with HA-MRSA [Reference Anderson61].

Human contact hazard related to horses

Occupational or recreational exposure to horses has been incriminated as a risk factor for human MRSA colonization [Reference Weese71]. Nasal carriage was significantly higher in veterinary practitioners (3·9%) than in persons not professionally exposed to animals (0·7%) or in healthy persons in the Danish community (<1%). Exposure to horses was found to be a risk factor [Reference Moodley49]. Colonization with MRSA was found in 10·1% of veterinary personnel attending an international equine veterinary conference. An increased risk of being colonized was associated with having treated a horse diagnosed with MRSA or having been personally diagnosed with MRSA in the past year. Hand-washing between infected patients and hand-washing between farms was protective [Reference Anderson, Lefebvre and Weese48].

Several studies report that MRSA isolates from horses and people working with horses are indistinguishable and differ from MRSA isolates from humans in the general population [Reference O'Mahony58, Reference Weese63, Reference Van Duijkeren64, Reference Cuny72, Reference Seguin73]. In Austria ST254, spa type t036, SCCmec type IV predominated in horses followed by ST398 (t011, SCCmecIV) and ST1 (t127, SCCmecIV) [Reference Cuny72]. In Canada the majority of equine isolates are ST8 (t008, SCCmecIV) classified by PFGE as Canadian MRSA-5. The predominance of this clone in horses and horse personnel in Canada suggests that this human-origin clone is horse-adapted [Reference Weese and Van Duijkeren2]. In The Netherlands most equine MRSA are either ST398 spa type t011 or ST8 spa type t064 [Reference Van Duijkeren64]. From 2000 to 2002, 27 persons were found colonized with MRSA at a Canadian veterinary teaching hospital and 10 horse farms. Only one person, a veterinarian working at the clinic, had clinical infection, and the same strain was isolated from two horses he had cared for [Reference Weese74]. Human skin infections were also reported from three persons working in a foal nursery and MRSA isolates from the humans and the foal were indistinguishable by PFGE [Reference Weese71]. Screening of personnel during an outbreak of MRSA infections of horses at a veterinary teaching hospital showed that persons in close contact with horses were more often MRSA-positive than those without [Reference Van Duijkeren64].

Occurrence in companion animals

In 1988 Scott et al. [Reference Scott75] reported the first companion animal-related outbreak of MRSA in a rehabilitation geriatric ward where the ward cat was colonized and was implicated as reservoir for re-infection. Infection control measures and removal of the cat led to rapid resolution of the outbreak. Since then the number of reports on infections and colonization with MRSA from companion animals has increased [Reference Leonard and Markey1]. The transmission of a PVL-positive MRSA strain between humans and a dog has been reported [Reference van Duijkeren76]. The available evidence suggests that humans are the source of infection or colonization of companion animals and thus a probable ‘humanosis’ exists, but animals can act as carriers and pass the infecting strain to humans in contact [Reference Strommenger77]. Molecular-typing methods support the hypothesis that MRSA of human origin have adapted to companion animals. Clonal complexes tend to be those predominating in people in the region [Reference Weese and Van Duijkeren2].

Healthy animals can be colonized for variable periods of time without developing clinical disease [Reference Weese78], but the overall prevalence of the colonization remains low in dogs and cats [Reference Leonard and Markey1, Reference Leonard and Markey57, Reference Murphy79–Reference Weese83]. Potential differences with the human epidemiology of the disease, particularly the dynamics of colonization in companion animals (e.g. shedding, type of contacts and duration of colonization) may exist and are inadequately identified. A recent study concluded on the lack of transmission of MRSA between apparently healthy dogs in a rescue kennel in the absence of risk factors (e.g. infected MRSA animal) [Reference Loeffler84].

Little is known about the prevalence of MRSA infections in companion animals. MRSA infections cannot be recognized from their clinical presentations alone because they resemble those caused by methicillin-susceptible S. aureus (MSSA), S. intermedius/pseudintermedius and coagulase-negative staphylococci [Reference Lloyd, Boag and Loeffler85]. S. aureus can give rise to a wide diversity of suppurative infections in animals. In line with that, MRSA have been isolated from diverse skin and STIs including abscesses, dermatitis, post-operative wound infections, and intravenous catheter or surgical implant infections [Reference Leonard and Markey1, Reference Baptiste55, Reference Middleton57, Reference Seguin73, Reference Weese83, Reference Bender86, Reference Duquette and Nuttall87–Reference Tomlin90]. Morris et al. [Reference Morris91] reported that MRSA were significantly more frequently associated with deep pyoderma in dogs than other strains of S. aureus. Less frequently MRSA has been isolated from lower urinary tract infection, pneumonia, and chronic rhinitis [Reference Baptiste55, Reference Weese83] [Reference Gortel92]. A recent study compared MRSA and MSSA infection outcomes in dogs and cats and reported a high survival rate in both groups, probably because of the high frequency of non-invasive infections.

Risk factors for colonization and infection in companion animals

Little information is available on the risk of antimicrobial usage with regard to MRSA infection or colonization in companion animals. According to case reports quoted above, many animals infected or colonized with MRSA have been treated with antimicrobials prior to the diagnosis. Fluoroquinolone administration has been identified as a risk factor for MRSA infections in dogs and cats [Reference Baptiste55, Reference Faires and Weese93].

Studies on risk factors other than antimicrobials for MRSA infections in companion animals are scarce. Owners from MRSA-positive households or healthcare workers constitute possible risk factors for this companion animal humanosis [Reference Baptiste55, Reference van Duijkeren76, Reference Faires and Weese93, Reference van Duijkeren94].

MRSA infections in small animals have also been associated with exposure to medical hospitals, extensive wounds, prolonged hospitalization and immunosuppression [Reference Duquette and Nuttall87]. In a retrospective case-control study at three veterinary referral hospitals significant risk factors for the acquisition of a MRSA infection compared to a MSSA infection was the presence of a urinary catheter or a joint infection [Reference Faires and Weese93]. Invasive procedures, including the presence of foreign material such as suture material, orthopaedic implants, urinary catheters, central venous lines and chest drains appear to be associated with the persistence of MRSA infections [Reference Leonard88, 95]. Other identified risk factors associated with SSIs in general, but highly relevant in particular for staphylococci infections, include: improper surgical site clipping and aseptic preparation before surgery, duration of surgery, duration of anaesthesia, emergency vs. daytime surgery, surgical tissue handling, number of persons present in the operating room, and total length of hospital stay [95]. Small-animal ICUs may be at particular risk for periodic outbreaks of colonization and disease as reported by Weese et al. [Reference Weese96].

Transmission of MRSA infection between dogs apparently can be associated with contamination of the floor in a veterinary clinic (Y. Abbott and F. C. Leonard, personal communication). Thus, in veterinary medicine cleanliness of floors appears to be as important as hand-touch sites in the control of human MRSA infections.

Human contact hazard related to companion animals

Several studies have examined the prevalence of MRSA in veterinary hospitals in the UK [Reference O'Mahony58, Reference Hanselman, Kruth and Weese81, Reference Loeffler82]. These studies have shown that veterinary staff and their pets have a higher prevalence of MRSA, although they are mostly asymptomatic carriers. A recent study by Moodley et al. [Reference Moodley49] showed that MRSA carriage was significantly (P<0·02) higher in veterinary practitioners (3·9%) than in participants not professionally exposed to animals (0·7%). The results from this study indicate that veterinary professionals are at risk of MRSA carriage and thus should be informed about this emerging occupational health risk and educated about preventive measures.

MRSA infections in owners having involvement with companion animals such as dogs and cats have been suggested for many years, and evidence for this hazard has increased during recent years [Reference Leonard and Markey1, Reference Morgan7, Reference van Duijkeren76, Reference van Duijkeren94]. Larger epidemiological studies are required to provide more information on specific risk factors.

Reduction of antimicrobial selective pressure in livestock

A reduction of the selective pressure by avoiding routine mass medication, could be a major potential control measure. An additional benefit of this measure would be to preserve the efficacy of the current antimicrobials for veterinary and human use.

To confirm a reduction of antimicrobial consumption and to evaluate a possible benefit, detailed information on the applied therapies is necessary, with respect for animal species and the route of administration. Preferably the indication, the production system (e.g. broiler vs. layer), and the regimens applied needs to be documented in detail (dose, duration, formulation, treatment interval).

Prevention of transmission of MRSA between and within livestock farms

Given the efficient transmission of LA-MRSA throughout the production chain as shown for swine [Reference van Duijkeren36], one way to reduce the dissemination of MRSA from farm to farm would be to improve sanitary control measures between herds and during transport. The piglet suppliers form a first target for this approach, which then might be gradually implemented throughout the food chain. Prevention of trade from MRSA-positive to MRSA-negative herds could be considered.

The stand-alone period is a cornerstone in reducing the persistence of bacterial organisms between production cycles. Research on disinfection measures in different production types are needed in view of the current MRSA situation, primarily in pigs, veal calves and broilers. Conversion of the current stable structures might be considered for a more efficient disinfection via mechanical, physical (drying), chemical (chlorhexidine), and thermal (burning, steaming, cold) cleansing.

Reduce carriers in MRSA-positive livestock farms

Control options for colonized livestock animals

Control options for infected livestock animals

Prevention of transmission of MRSA strains in livestock

Because of the high colonization frequency in healthy animals and the relatively few documented infections, control options suggested in an earlier section entitled ‘Prevention of transmission of MRSA between and within farms’ are applicable.

In addition, control options given below in a more specified form for horses and small companion animals [99] have been extrapolated in line with general principles for control of bacterial infections as developed.

• • Identification and isolation of animals to minimize the risk of zoonotic transmission.

• • Use contact precautions such as protective outerwear, e.g. overalls, aprons or coats and boots or overshoes that are not worn elsewhere.

• • Protective outerwear and all items handled during the treatment of MRSA-positive animals (e.g. boards to drive livestock), should be regarded as potentially contaminated.

• • Hand hygiene, e.g. through alcohol gel pouches is essential but must be performed correctly.

• • Proper cleaning and disinfection of contaminated environments, including transport vehicles. Special attention should be paid to dust in stables.

• • Owners should be informed about the risks and required precautions.

Control options for colonized horses

Control options for infected horses

Prevention of transmission of MRSA strains between horses

Guidelines on the management of MRSA in veterinary practices have been developed, e.g. by the British Small Animal Veterinary Association (BSAVA) [99] and are applicable also to equine hospitals. It is recommended that patients diagnosed with or suspected of MRSA infections are isolated in order to minimize the risk of nosocomial and zoonotic transmission. MRSA-infected animals should be nursed using barrier nursing precautions and staff contact should be limited to what is essential. Infected horses should only be handled using contact precautions such as protective outerwear, e.g. overalls, aprons or coats and boots or overshoes that are not worn elsewhere, gloves and masks. MRSA-infected wounds should be covered with clean bandages if possible. Personnel must avoid contaminating themselves. All items handled during the treatment of a MRSA-positive patient should be regarded as potentially contaminated, e.g. electric shavers.

Transmission of the organism on the hands is thought to be an important route of transmission within human and veterinary hospital settings. Therefore, hand hygiene should be an essential part of any infection control programme. Hand-washing should be carried out between patients. Alcohol gel pouches for wearing on uniforms can be used as a rapid and convenient method of hand sanitizing [Reference Leonard and Markey1].

Proper cleaning and disinfection of contaminated environments is also highly recommended, because widespread contamination of the environment of a veterinary hospital environment has been reported [Reference Weese14, Reference Van Duijkeren64, Reference Weese100]. Environmental transmission may be of greater importance in stables than in hospitals [Reference Leonard and Markey1] as horse stables are often very dusty.

Routine screening of all horses before admission in order to identify colonized or infected animals could help to prevent the spread of MRSA, but is costly. Screening of hospitalized horses which have been in contact with MRSA-positive horses or personnel is recommended.

Owners of infected horses need to be informed about the risks of MRSA and the precautions they should take. Furthermore, the recommendation from BSAVA that owners visiting their infected animal should not visit other patients at the clinic [99] is also applicable to horse practices.

Control options for colonized companion animals

Control options for infected companion animals

Prevention of transmission of MRSA between companion animals

Guidelines for control and prevention of MRSA infection in small animals have been prepared, e.g. by BSAVA [99]. Stringent household infection control practices, in particular frequent hand hygiene and avoiding high-risk contact are important factors to minimize the risk of becoming colonized. In the event of rare situations where MRSA infections are uncontrolled in people in the household and the entire family is undergoing eradication therapy, kennelling the pet, preferably using contact isolation to other pets, for weeks is a reasonable option. This may allow the clearance of colonization and avoid cross-contamination. Little is known about the nature and length of colonization in companion animals. Further studies are required to reach conclusions.

Use of latex gloves and protection measures such as masks and eye protection may be helpful provided they are appropriately used and changed between patients. For instance, it is recommended to rub the hands with alcohol immediately after the gloves are removed. Hand hygiene and disinfection of surfaces and equipment should be carried out between all patients. Finally, additional barrier precautions must be considered based on the conditions present in the hospital.

Additional simple strategies can effectively reduce the risk of nosocomial infections – including MRSA – in small animal patients. First, limitation of the extrinsic risk factors is the most logical approach: (i) invasive procedures should be restricted, (ii) surgical interventions should be designed to avoid the many risk factors for surgical site infections, (iii) indwelling urinary catheters should be removed as soon as the patient's condition allows it, (iv) the consequences of antibiotic use in dogs and cats with indwelling urinary catheters should also be evaluated, and (v) proper care of intravenous and urinary catheters is essential to prevent complications [95]. Protocols for asepsis prior to and during placement of the catheter should exist. ICUs may be at particular risk for periodic outbreaks of colonization and disease, but can be curtailed by barrier precautions, and hand hygiene [Reference Weese96].

In veterinary hospitals, animals with suspected MRSA infections (animals with non-healing wounds, with non-antibiotic responsive infections or with nosocomial infections), animals from known MRSA-positive households, or those belonging to healthcare workers should be screened for MRSA colonization. The implementation of the ‘Search-and-destroy’ strategy as successfully applied in human medicine by certain Northern European countries could possibly be applied in small animal hospitals, given that the time for MRSA detection and the length of hospital stay allows for implementation of additional control options. Concerns have been raised about dogs involved in hospital visitation programmes such as therapy pets [Reference Enoch108].

Conclusions on ecology and epidemiology

Conclusion on control and therapeutic options