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Methicillin-resistant Staphylococcus aureus

February 15, 2024

"MRSA" redirects here. For other uses, see MRSA (disambiguation).

Methicillin-resistant Staphylococcus aureus (MRSA) is a group of gram-positive bacteria that are genetically distinct from other strains of Staphylococcus aureus. MRSA is responsible for several difficult-to-treat infections in humans. It caused more than 100,000 deaths worldwide attributable to antimicrobial resistance in 2019.

Scanning electron micrograph of a human neutrophil ingesting MRSA

MRSA is any strain of S. aureus that has developed (through natural selection) or acquired (through horizontal gene transfer) a multiple drug resistance to beta-lactam antibiotics. Beta-lactam (β-lactam) antibiotics are a broad-spectrum group that include some penams (penicillin derivatives such as methicillin and oxacillin) and cephems such as the cephalosporins.[1] Strains unable to resist these antibiotics are classified as methicillin-susceptible S. aureus, or MSSA.

MRSA infection is common in hospitals, prisons, and nursing homes, where people with open wounds, invasive devices such as catheters, and weakened immune systems are at greater risk of healthcare-associated infection. MRSA began as a hospital-acquired infection but has become community-acquired, as well as livestock-acquired. The terms HA-MRSA (healthcare-associated or hospital-acquired MRSA), CA-MRSA (community-associated MRSA), and LA-MRSA (livestock-associated MRSA) reflect this.[citation needed]

Signs and symptoms edit

 
Although usually carried without symptoms, MRSA often presents as small red pustular skin infections

In humans, Staphylococcus aureus is part of the normal microbiota present in the upper respiratory tract,[2] and on skin and in the gut mucosa.[3] However, along with similar bacterial species that can colonize and act symbiotically, they can cause disease if they begin to take over the tissues they have colonized or invade other tissues; the resultant infection has been called a "pathobiont".[2]

After 72 hours, MRSA can take hold in human tissues and eventually become resistant to treatment. The initial presentation of MRSA is small red bumps that resemble pimples, spider bites, or boils; they may be accompanied by fever and, occasionally, rashes. Within a few days, the bumps become larger and more painful; they eventually open into deep, pus-filled boils. About 75 percent of CA-MRSA infections are localized to skin and soft tissue and usually can be treated effectively.[4]

Risk factors edit

A select few of the populations at risk include:

As many as 22% of people infected with MRSA do not have any discernable risk factors.[21]: 637 

Hospitalized people edit

People who are hospitalized, including the elderly, are often immunocompromised and susceptible to infection of all kinds, including MRSA; an infection by MRSA is called healthcare-associated or hospital-acquired methicillin-resistant S. aureus (HA-MRSA).[1][5][22][23] Generally, those infected by MRSA stay infected for just under 10 days, if treated by a doctor, although effects may vary from person to person.[24]

Both surgical and nonsurgical wounds can be infected with HA-MRSA.[1][5][22] Surgical site infections occur on the skin surface, but can spread to internal organs and blood to cause sepsis.[1] Transmission can occur between healthcare providers and patients because some providers may neglect to perform preventative hand-washing between examinations.[12][25]

People in nursing homes are at risk for all the reasons above, further complicated by their generally weaker immune systems.[13][26]

Prison inmates and military personnel edit

Prisons and military barracks[19] can be crowded and confined, and poor hygiene practices may proliferate, thus putting inhabitants at increased risk of contracting MRSA.[18] Cases of MRSA in such populations were first reported in the United States and later in Canada. The earliest reports were made by the Centers for Disease Control and Prevention in US state prisons. In the news media, hundreds of reports of MRSA outbreaks in prisons appeared between 2000 and 2008. For example, in February 2008, the Tulsa County jail in Oklahoma started treating an average of 12 S. aureus cases per month.[27]

Animals edit

Antibiotic use in livestock increases the risk that MRSA will develop among the livestock and other animals that may reside near them; strains MRSA ST 398 and CC398 are transmissible to humans.[19][28] Generally, animals are asymptomatic.[1]

Domestic pets are susceptible to MRSA infection by transmission from their owners; conversely, MRSA-infected pets can also transmit MRSA to humans.[29]

Athletes edit

Locker rooms, gyms, and related athletic facilities offer potential sites for MRSA contamination and infection.[30] Athletes have been identified as a high-risk group.[19] A study linked MRSA to the abrasions caused by artificial turf.[31] Three studies by the Texas State Department of Health found the infection rate among football players was 16 times the national average. In October 2006, a high-school football player was temporarily paralyzed from MRSA-infected turf burns. His infection returned in January 2007 and required three surgeries to remove infected tissue, and three weeks of hospital stay.[32]

In 2013, Lawrence Tynes, Carl Nicks, and Johnthan Banks of the Tampa Bay Buccaneers were diagnosed with MRSA. Tynes and Nicks apparently did not contract the infection from each other, but whether Banks contracted it from either individual is unknown.[33] In 2015, Los Angeles Dodgers infielder Justin Turner was infected while the team visited the New York Mets.[34] In October 2015, New York Giants tight end Daniel Fells was hospitalized with a serious MRSA infection.[35]

Children edit

MRSA is becoming a critical problem in children;[36] studies found 4.6% of patients in U.S. health-care facilities, (presumably) including hospital nurseries,[37] were infected or colonized with MRSA.[38] Children and adults who come in contact with day-care centers,[19] playgrounds, locker rooms, camps, dormitories, classrooms and other school settings, and gyms and workout facilities are at higher risk of contracting MRSA. Parents should be especially cautious of children who participate in activities where sports equipment is shared, such as football helmets and uniforms.[39]

Intravenous drug users edit

Needle-required drugs have caused an increase of MRSA,[40] with injection drug use (IDU) making up 24.1% (1,839 individuals) of Tennessee Hospital's Discharge System. The unsanitary methods of injection causes an access point for the MRSA to enter the blood stream and begin infecting the host. Furthermore, with MRSA's high contagion rate,[11] a common risk factor is individuals who are in constant contact with someone who has injected drugs in the past year.

Mechanism edit

Antimicrobial resistance is genetically based; resistance is mediated by the acquisition of extrachromosomal genetic elements containing genes that confer resistance to certain antibiotics. Examples of such elements include plasmids, transposable genetic elements, and genomic islands, which can be transferred between bacteria through horizontal gene transfer.[41] A defining characteristic of MRSA is its ability to thrive in the presence of penicillin-like antibiotics, which normally prevent bacterial growth by inhibiting synthesis of cell wall material. This is due to a resistance gene, mecA, which stops β-lactam antibiotics from inactivating the enzymes (transpeptidases) critical for cell wall synthesis.[42]

SCCmec edit

Staphylococcal cassette chromosome mec (SCCmec) is a genomic island of unknown origin containing the antibiotic resistance gene mecA.[43][44] SCCmec contains additional genes beyond mecA, including the cytolysin gene psm-mec, which may suppress virulence in HA-acquired MRSA strains.[45] In addition, this locus encodes strain-dependent gene regulatory RNAs known as psm-mecRNA.[46] SCCmec also contains ccrA and ccrB; both genes encode recombinases that mediate the site-specific integration and excision of the SCCmec element from the S. aureus chromosome.[43][44] Currently, six unique SCCmec types ranging in size from 21 to 67 kb have been identified;[43] they are designated types I–VI and are distinguished by variation in mec and ccr gene complexes.[41] Owing to the size of the SCCmec element and the constraints of horizontal gene transfer, a minimum of five clones are thought to be responsible for the spread of MRSA infections, with clonal complex (CC) 8 most prevalent.[43][47] SCCmec is thought to have originated in the closely related Staphylococcus sciuri species and transferred horizontally to S. aureus.[48]

Different SCCmec genotypes confer different microbiological characteristics, such as different antimicrobial resistance rates.[49] Different genotypes are also associated with different types of infections. Types I–III SCCmec are large elements that typically contain additional resistance genes and are characteristically isolated from HA-MRSA strains.[44][49] Conversely, CA-MRSA is associated with types IV and V, which are smaller and lack resistance genes other than mecA.[44][49]

These distinctions were thoroughly investigated by Collins et al. in 2001, and can be explained by the fitness differences associated with carriage of a large or small SCCmec plasmid. Carriage of large plasmids, such as SCCmecI–III, is costly to the bacteria, resulting in a compensatory decrease in virulence expression.[50] MRSA is able to thrive in hospital settings with increased antibiotic resistance but decreased virulence – HA-MRSA targets immunocompromised, hospitalized hosts, thus a decrease in virulence is not maladaptive.[50] In contrast, CA-MRSA tends to carry lower-fitness cost SCCmec elements to offset the increased virulence and toxicity expression required to infect healthy hosts.[50]

mecA edit

mecA is a biomarker gene responsible for resistance to methicillin and other β-lactam antibiotics. After acquisition of mecA, the gene must be integrated and localized in the S. aureus chromosome.[43] mecA encodes penicillin-binding protein 2a (PBP2a), which differs from other penicillin-binding proteins as its active site does not bind methicillin or other β-lactam antibiotics.[43] As such, PBP2a can continue to catalyze the transpeptidation reaction required for peptidoglycan cross-linking, enabling cell wall synthesis even in the presence of antibiotics. As a consequence of the inability of PBP2a to interact with β-lactam moieties, acquisition of mecA confers resistance to all β-lactam antibiotics in addition to methicillin.[43][51]

mecA is under the control of two regulatory genes, mecI and mecR1. MecI is usually bound to the mecA promoter and functions as a repressor.[41][44] In the presence of a β-lactam antibiotic, MecR1 initiates a signal transduction cascade that leads to transcriptional activation of mecA.[41][44] This is achieved by MecR1-mediated cleavage of MecI, which alleviates MecI repression.[41] mecA is further controlled by two co-repressors, blaI and blaR1. blaI and blaR1 are homologous to mecI and mecR1, respectively, and normally function as regulators of blaZ, which is responsible for penicillin resistance.[43][52] The DNA sequences bound by mecI and blaI are identical;[43] therefore, blaI can also bind the mecA operator to repress transcription of mecA.[52]

Arginine catabolic mobile element edit

The arginine catabolic mobile element (ACME) is a virulence factor present in many MRSA strains but not prevalent in MSSA.[53] SpeG-positive ACME compensates for the polyamine hypersensitivity of S. aureus and facilitates stable skin colonization, wound infection, and person-to-person transmission.[54]

Strains edit

 
Diagram depicting antibiotic resistance through alteration of the antibiotic's target site, modeled after MRSA's resistance to penicillin. Beta-lactam antibiotics permanently inactivate PBP enzymes, which are essential for cell wall synthesis and thus for bacterial life, by permanently binding to their active sites. Some forms of MRSA, however, express a different PBP that will not allow the antibiotic into its active site.

Acquisition of SCCmec in methicillin-sensitive S. aureus (MSSA) gives rise to a number of genetically different MRSA lineages. These genetic variations within different MRSA strains possibly explain the variability in virulence and associated MRSA infections.[55] The first MRSA strain, ST250 MRSA-1, originated from SCCmec and ST250-MSSA integration.[55] Historically, major MRSA clones ST2470-MRSA-I, ST239-MRSA-III, ST5-MRSA-II, and ST5-MRSA-IV were responsible for causing hospital-acquired MRSA (HA-MRSA) infections.[55] ST239-MRSA-III, known as the Brazilian clone, was highly transmissible compared to others and distributed in Argentina, Czech Republic, and Portugal.[55]

In the UK, the most common strains of MRSA are EMRSA15 and EMRSA16.[56] EMRSA16 has been found to be identical to the ST36:USA200 strain, which circulates in the United States, and to carry the SCCmec type II, enterotoxin A and toxic shock syndrome toxin 1 genes.[57] Under the new international typing system, this strain is now called MRSA252. EMRSA 15 is also found to be one of the common MRSA strains in Asia. Other common strains include ST5:USA100 and EMRSA 1.[58] These strains are genetic characteristics of HA-MRSA.[59]

Community-acquired MRSA (CA-MRSA) strains emerged in late 1990 to 2000, infecting healthy people who had not been in contact with healthcare facilities.[59] Researchers suggest that CA-MRSA did not evolve from HA-MRSA.[59] This is further proven by molecular typing of CA-MRSA strains[60] and genome comparison between CA-MRSA and HA-MRSA, which indicate that novel MRSA strains integrated SCCmec into MSSA separately on its own.[59] By mid-2000, CA-MRSA was introduced into healthcare systems and distinguishing CA-MRSA from HA-MRSA became a difficult process.[59] Community-acquired MRSA is more easily treated and more virulent than hospital-acquired MRSA (HA-MRSA).[59] The genetic mechanism for the enhanced virulence in CA-MRSA remains an active area of research. The Panton–Valentine leukocidin (PVL) genes are of particular interest because they are a unique feature of CA-MRSA.[55]

In the United States, most cases of CA-MRSA are caused by a CC8 strain designated ST8:USA300, which carries SCCmec type IV, Panton–Valentine leukocidin, PSM-alpha and enterotoxins Q and K,[57] and ST1:USA400.[61] The ST8:USA300 strain results in skin infections, necrotizing fasciitis, and toxic shock syndrome, whereas the ST1:USA400 strain results in necrotizing pneumonia and pulmonary sepsis.[55] Other community-acquired strains of MRSA are ST8:USA500 and ST59:USA1000. In many nations of the world, MRSA strains with different genetic background types have come to predominate among CA-MRSA strains; USA300 easily tops the list in the U.S. and is becoming more common in Canada after its first appearance there in 2004. For example, in Australia, ST93 strains are common, while in continental Europe ST80 strains, which carry SCCmec type IV, predominate.[62][63] In Taiwan, ST59 strains, some of which are resistant to many non-beta-lactam antibiotics, have arisen as common causes of skin and soft tissue infections in the community. In a remote region of Alaska, unlike most of the continental U.S., USA300 was found only rarely in a study of MRSA strains from outbreaks in 1996 and 2000 as well as in surveillance from 2004 to 2006.[64]

A MRSA strain, CC398, is found in intensively reared production animals (primarily pigs, but also cattle and poultry), where it can be transmitted to humans as LA-MRSA (livestock-associated MRSA).[58][65][66]

Diagnosis edit

 
A selective and differential chromogenic medium for the qualitative direct detection of MRSA
 
MRSA resistance to oxacillin being tested. The top S. aureus isolate is a control that is not resistant to oxacillin; the other three isolates are MRSA-positive.
 
Mueller–Hinton agar showing MRSA resistant to an oxacillin disk

Diagnostic microbiology laboratories and reference laboratories are key for identifying outbreaks of MRSA. Normally, a bacterium must be cultured from blood, urine, sputum, or other body-fluid samples, and in sufficient quantities to perform confirmatory tests early-on. Still, because no quick and easy method exists to diagnose MRSA, initial treatment of the infection is often based upon "strong suspicion" and techniques by the treating physician; these include quantitative PCR procedures, which are employed in clinical laboratories for quickly detecting and identifying MRSA strains.[67][68]

Another common laboratory test is a rapid latex agglutination test that detects the PBP2a protein. PBP2a is a variant penicillin-binding protein that imparts the ability of S. aureus to be resistant to oxacillin.[69]

Microbiology edit

Like all S. aureus (also abbreviated SA at times), methicillin-resistant S. aureus is a gram-positive, spherical (coccus) bacterium about 1 micron in diameter. It does not form spores and it is not motile. It is frequently found in grape-like clusters or chains.[70]: 390  Unlike methicillin-susceptible S. aureus (MSSA), MRSA is slow-growing on a variety of media and has been found to exist in mixed colonies of MSSA. The mecA gene, which confers resistance to a number of antibiotics, is always present in MRSA and usually absent in MSSA; however, in some instances, the mecA gene is present in MSSA but is not expressed. Polymerase chain reaction (PCR) testing is the most precise method for identifying MRSA strains. Specialized culture media have been developed to better differentiate between MSSA and MRSA and, in some cases, such media can be used to identify specific strains that are resistant to different antibiotics.[70]: 402 

Other strains of S. aureus have emerged that are resistant to oxacillin, clindamycin, teicoplanin, and erythromycin. These resistant strains may or may not possess the mecA gene. S. aureus has also developed resistance to vancomycin (VRSA). One strain is only partially susceptible to vancomycin and is called vancomycin-intermediate S. aureus (VISA). GISA, a strain of resistant S. aureus, is glycopeptide-intermediate S. aureus and is less suspectible to vancomycin and teicoplanin. Resistance to antibiotics in S. aureus can be quantified by determining the amount of the antibiotic that must be used to inhibit growth. If S. aureus is inhibited at a concentration of vancomycin less than or equal to 4 μg/ml, it is said to be susceptible. If a concentration greater than 32 μg/ml is necessary to inhibit growth, it is said to be resistant.[21]: 637 

Prevention edit

Screening edit

In health-care settings, isolating those with MRSA from those without the infection is one method to prevent transmission. Rapid culture and sensitivity testing and molecular testing identifies carriers and reduces infection rates.[71] It is especially important to test patients in these settings since 2% of people are carriers of MRSA, even though in many of these cases the bacteria reside in the nostril and the patient will not present any symptoms.[72]

MRSA can be identified by swabbing the nostrils and isolating the bacteria found there. Combined with extra sanitary measures for those in contact with infected people, swab screening people admitted to hospitals has been found to be effective in minimizing the spread of MRSA in hospitals in the United States, Denmark, Finland, and the Netherlands.[73]

Handwashing edit

The Centers for Disease Control and Prevention offers suggestions for preventing the contraction and spread of MRSA infection which are applicable to those in community settings, including incarcerated populations, childcare center employees, and athletes. To prevent the spread of MRSA, the recommendations are to wash hands thoroughly and regularly using soap and water or an alcohol-based sanitizer. Additional recommendations are to keep wounds clean and covered, avoid contact with other people's wounds, avoid sharing personal items such as razors or towels, shower after exercising at athletic facilities, and shower before using swimming pools or whirlpools.[74]

Isolation edit

Excluding medical facilities, current US guidance does not require workers with MRSA infections to be routinely excluded from the general workplace.[75] The National Institutes of Health recommend that those with wound drainage that cannot be covered and contained with a clean, dry bandage and those who cannot maintain good hygiene practices be reassigned,[75] and patients with wound drainage should also automatically be put on "Contact Precaution," regardless of whether or not they have a known infection.[76] Workers with active infections are excluded from activities where skin-to-skin contact is likely to occur.[77] To prevent the spread of staphylococci or MRSA in the workplace, employers are encouraged to make available adequate facilities that support good hygiene. In addition, surface and equipment sanitizing should conform to Environmental Protection Agency-registered disinfectants.[75] In hospital settings, contact isolation can be stopped after one to three cultures come back negative.[78] Before the patient is cleared from isolation, it is advised that there is dedicated patient-care or single-use equipment for that particular patient. If this is not possible, the equipment must be properly disinfected before it is used on another patient.[76]

To prevent the spread of MRSA in the home, health departments recommend laundering materials that have come into contact with infected persons separately and with a dilute bleach solution; to reduce the bacterial load in one's nose and skin; and to clean and disinfect those things in the house that people regularly touch, such as sinks, tubs, kitchen counters, cell phones, light switches, doorknobs, phones, toilets, and computer keyboards.[79]

Restricting antibiotic use edit

Glycopeptides, cephalosporins, and in particular, quinolones are associated with an increased risk of colonisation of MRSA. Reducing use of antibiotic classes that promote MRSA colonisation, especially fluoroquinolones, is recommended in current guidelines.[12][25]

Public health considerations edit

Mathematical models describe one way in which a loss of infection control can occur after measures for screening and isolation seem to be effective for years, as happened in the UK. In the "search and destroy" strategy that was employed by all UK hospitals until the mid-1990s, all hospitalized people with MRSA were immediately isolated, and all staff were screened for MRSA and were prevented from working until they had completed a course of eradication therapy that was proven to work. Loss of control occurs because colonised people are discharged back into the community and then readmitted; when the number of colonised people in the community reaches a certain threshold, the "search and destroy" strategy is overwhelmed.[80] One of the few countries not to have been overwhelmed by MRSA is the Netherlands: an important part of the success of the Dutch strategy may have been to attempt eradication of carriage upon discharge from hospital.[81]

Decolonization edit

Main article: Decolonization (medicine)

As of 2013, no randomized clinical trials had been conducted to understand how to treat nonsurgical wounds that had been colonized, but not infected, with MRSA,[22] and insufficient studies had been conducted to understand how to treat surgical wounds that had been colonized with MRSA.[1] As of 2013, whether strategies to eradicate MRSA colonization of people in nursing homes reduced infection rates was not known.[26]

Care should be taken when trying to drain boils, as disruption of surrounding tissue can lead to larger infections, including infection of the blood stream.[82] Mupirocin 2% ointment can be effective at reducing the size of lesions. A secondary covering of clothing is preferred.[79] As shown in an animal study with diabetic mice, the topical application of a mixture of sugar (70%) and 3% povidone-iodine paste is an effective agent for the treatment of diabetic ulcers with MRSA infection.[83]

Community settings edit

Maintaining the necessary cleanliness may be difficult for people if they do not have access to facilities such as public toilets with handwashing facilities. In the United Kingdom, the Workplace (Health, Safety and Welfare) Regulations 1992[84] require businesses to provide toilets for their employees, along with washing facilities including soap or other suitable means of cleaning. Guidance on how many toilets to provide and what sort of washing facilities should be provided alongside them is given in the Workplace (Health, Safety and Welfare) Approved Code of Practice and Guidance L24, available from , but no legal obligations exist on local authorities in the United Kingdom to provide public toilets, and although in 2008, the House of Commons Communities and Local Government Committee called for a duty on local authorities to develop a public toilet strategy,[85] this was rejected by the Government.[86]

Agriculture edit

See also: Antibiotic use in livestock

The World Health Organization advocates regulations on the use of antibiotics in animal feed to prevent the emergence of drug-resistant strains of MRSA.[28] MRSA is established in animals and birds.[19]

Treatment edit

Antibiotics edit

See also: Medications used to treat MRSA

Treatment of MRSA infection is urgent and delays can be fatal.[20]: 328  The location and history related to the infection determines the treatment. The route of administration of an antibiotic varies. Antibiotics effective against MRSA can be given by IV, oral, or a combination of both, and depend on the specific circumstances and patient characteristics.[4] The use of concurrent treatment with vancomycin or other beta-lactam agents may have a synergistic effect.[21]: 637 

Both CA-MRSA and HA-MRSA are resistant to traditional anti-staphylococcal beta-lactam antibiotics, such as cephalexin. CA-MRSA has a greater spectrum of antimicrobial susceptibility to sulfa drugs (like co-trimoxazole (trimethoprim/sulfamethoxazole), tetracyclines (like doxycycline and minocycline) and clindamycin (for osteomyelitis).[4] MRSA can be eradicated with a regimen of linezolid,[87] though treatment protocols vary and serum levels of antibiotics vary widely from person to person and may affect outcomes.[88] The effective treatment of MRSA with linezolid has been successful[87] in 87% of people. Linezolid is more effective in soft tissue infections than vancomycin.[89][1] This is compared to eradication of infection in those with MRSA treated with vancomycin. Treatment with vancomycin is successful in approximately 49% of people.[1] Linezolid belongs to the newer oxazolidinone class of antibiotics which has been shown to be effective against both CA-MRSA and HA-MRSA. The Infectious Disease Society of America recommends vancomycin, linezolid, or clindamycin (if susceptible) for treating those with MRSA pneumonia.[4]Ceftaroline, a fifth-generation cephalosporin, is the first beta-lactam antibiotic approved in the US to treat MRSA infections in skin and soft tissue or community-acquired pneumonia.[90]

Vancomycin and teicoplanin are glycopeptide antibiotics used to treat MRSA infections.[91] Teicoplanin is a structural congener of vancomycin that has a similar activity spectrum but a longer half-life.[92] Because the oral absorption of vancomycin and teicoplanin is very low, these agents can be administered intravenously to control systemic infections.[93] Treatment of MRSA infection with vancomycin can be complicated, due to its inconvenient route of administration. Moreover, the efficacy of vancomycin against MRSA is inferior to that of anti-staphylococcal beta-lactam antibiotics against methicillin-susceptible S. aureus (MSSA).[94][95]

Several newly discovered strains of MRSA show antibiotic resistance even to vancomycin and teicoplanin. Strains with intermediate (4–8 μg/ml) levels of resistance, termed glycopeptide-intermediate S. aureus (GISA) or vancomycin-intermediate S. aureus (VISA),[96][97] began appearing in the late 1990s. The first identified case was in Japan in 1996, and strains have since been found in hospitals in England, France, and the US. The first documented strain with complete (>16 μg/ml) resistance to vancomycin, termed vancomycin-resistant S. aureus (VRSA), appeared in the United States in 2002.[98] In 2011, a variant of vancomycin was tested that binds to the lactate variation and also binds well to the original target, thus reinstating potent antimicrobial activity.[99] Linezolid, quinupristin/dalfopristin, daptomycin, ceftaroline, and tigecycline are used to treat more severe infections that do not respond to glycopeptides such as vancomycin.[100] Current guidelines recommend daptomycin for VISA bloodstream infections and endocarditis.[4]

Oxazolidinones such as linezolid became available in the 1990s and are comparable to vancomycin in effectiveness against MRSA. Linezolid resistance in S. aureus was reported in 2001,[101] but infection rates have been at consistently low levels. In the United Kingdom and Ireland, no linezolid resistance was found in staphylococci collected from bacteremia cases between 2001 and 2006.[102]

Skin and soft-tissue infections edit

In skin abscesses, the primary treatment recommended is removal of dead tissue, incision, and drainage. More information is needed to determine the effectiveness of specific antibiotics therapy in surgical site infections (SSIs).[4] Examples of soft-tissue infections from MRSA include ulcers, impetigo, abscesses, and SSIs.[89] In surgical wounds, evidence is weak (high risk of bias) that linezolid may be better than vancomycin to eradicate MRSA SSIs.[1]

MRSA colonization is also found in nonsurgical wounds such as traumatic wounds, burns, and chronic ulcers (i.e.: diabetic ulcer, pressure ulcer, arterial insufficiency ulcer, venous ulcer). No conclusive evidence has been found about the best antibiotic regimen to treat MRSA colonization.[22]

Children edit

In skin infections and secondary infection sites, topical mupirocin is used successfully. For bacteremia and endocarditis, vancomycin or daptomycin is considered. For children with MRSA-infected bone or joints, treatment is individualized and long-term. Neonates can develop neonatal pustulosis as a result of topical infection with MRSA.[4] Clindamycin is not approved for the treatment of MRSA infection, but it is still used in children for soft-tissue infections.[4]

Endocarditis and bacteremia edit

Evaluation for the replacement of a prosthetic valve is considered. Appropriate antibiotic therapy may be administered for up to six weeks. Four to six weeks of antibiotic treatment is often recommended, and is dependent upon the extent of MRSA infection.[4]

Respiratory infections edit

CA-MRSA in hospitalized patients pneumonia treatment begins before culture results. After the susceptibility to antibiotics is performed, the infection may be treated with vancomycin or linezolid for up to 21 days. If the pneumonia is complicated by the accumulation of pus in the pleural cavity surrounding the lungs, drainage may be done along with antibiotic therapy.[4] People with cystic fibrosis may develop respiratory complications related to MRSA infection. The incidence of MRSA in those with cystic fibrosis increased during 2000 to 2015 by five times. Most of these infections were HA-MRSA. MRSA accounts for 26% of lung infections in those with cystic fibrosis.[103]

There is insufficient evidence to support the use of topical or systematic antibiotics for nasal or extra-nasal MRSA infection.[104]

Bone and joint infections edit

Cleaning the wound of dead tissue and draining abscesses is the first action to treat the MRSA infection. Administration of antibiotics is not standardized and is adapted by a case-by-case basis. Antibiotic therapy can last up to 3 months and sometimes even longer.[4]

Infected implants edit

MRSA infection can occur associated with implants and joint replacements. Recommendations on treatment are based upon the length of time the implant has been in place. In cases of a recent placement of a surgical implant or artificial joint, the device may be retained while antibiotic therapy continues. If the placement of the device has occurred over 3 weeks ago, the device may be removed. Antibiotic therapy is used in each instance sometimes long-term.[4]

Central nervous system edit

MRSA can infect the central nervous system and form brain abscess, subdural empyema, and spinal epidural abscess. Excision and drainage can be done along with antibiotic treatment. Septic thrombosis of cavernous or dural venous sinus can sometimes be a complication.[4]

Other infections edit

Treatment is not standardized for other instances of MRSA infection in a wide range of tissues. Treatment varies for MRSA infections related to: subperiosteal abscesses, necrotizing pneumonia, cellulitis, pyomyositis, necrotizing fasciitis, mediastinitis, myocardial, perinephric, hepatic, and splenic abscesses, septic thrombophlebitis, and severe ocular infections, including endophthalmitis.[4] Pets can be reservoirs and pass on MRSA to people. In some cases, the infection can be symptomatic and the pet can develop a MRSA infection. Health departments recommend that the pet be taken to the veterinarian if MRSA infections keep occurring in the people who have contact with the pet.[79]

Epidemiology edit

Worldwide, an estimated 2 billion people carry some form of S. aureus; of these, up to 53 million (2.7% of carriers) are thought to carry MRSA.[105] S. aureus was identified as one of the six leading pathogens for deaths associated with resistance in 2019 and 100,000 deaths caused by MRSA were attributable to antimicrobial resistance.[106]

HA-MRSA edit

In a US cohort study of 1,300 healthy children, 2.4% carried MRSA in their nose.[107] Bacterial sepsis occurs with most (75%) of cases of invasive MRSA infection.[4] In 2009, there were an estimated 463,017 hospitalizations due to MRSA, or a rate of 11.74 per 1,000 hospitalizations.[108] Many of these infections are less serious, but the Centers for Disease Control and Prevention (CDC) estimate that there are 80,461 invasive MRSA infections and 11,285 deaths due to MRSA annually.[109] In 2003, the cost for a hospitalization due to MRSA infection was US$92,363; a hospital stay for MSSA was $52,791.[89]

Infection after surgery is relatively uncommon, but occurs as much as 33% in specific types of surgeries. Infections of surgical sites range from 1% to 33%. MRSA sepsis that occurs within 30 days following a surgical infection has a 15–38% mortality rate; MRSA sepsis that occurs within one year has a mortality rate of around 55%. There may be increased mortality associated with cardiac surgery. There is a rate of 12.9% in those infected with MRSA while only 3% infected with other organisms. SSIs infected with MRSA had longer hospital stays than those who did not.[1]

Globally, MRSA infection rates are dynamic and vary year to year.[110] According to the 2006 SENTRY Antimicrobial Surveillance Program report, the incidence of MRSA bloodstream infections was 35.9% in North America. MRSA blood infections in Latin America was 29%. European incidence was 22.8%. The rate of all MRSA infections in Europe ranged from 50% in Portugal down to 0.8% in Sweden. Overall MRSA infection rates varied in Latin America: Colombia and Venezuela combined had 3%, Mexico had 50%, Chile 38%, Brazil 29%, and Argentina 28%.[89]

The Centers for Disease Control and Prevention (CDC) estimated that about 1.7 million nosocomial infections occurred in the United States in 2002, with 99,000 associated deaths.[111] The estimated incidence is 4.5 nosocomial infections per 100 admissions, with direct costs (at 2004 prices) ranging from $10,500 (£5300, €8000 at 2006 rates) per case (for bloodstream, urinary tract, or respiratory infections in immunocompetent people) to $111,000 (£57,000, €85,000) per case for antibiotic-resistant infections in the bloodstream in people with transplants. With these numbers, conservative estimates of the total direct costs of nosocomial infections are above $17 billion. The reduction of such infections forms an important component of efforts to improve healthcare safety. (BMJ 2007)[citation needed] MRSA alone was associated with 8% of nosocomial infections reported to the CDC National Healthcare Safety Network from January 2006 to October 2007.[112]

The British National Audit Office estimated that the incidence of nosocomial infections in Europe ranges from 4% to 10% of all hospital admissions. As of early 2005, the number of deaths in the United Kingdom attributed to MRSA has been estimated by various sources to lie in the area of 3,000 per year.[113]

In the United States, an estimated 95 million people carry S. aureus in their noses; of these, 2.5 million (2.6% of carriers) carry MRSA.[114] A population review conducted in three U.S. communities showed the annual incidence of CA-MRSA during 2001–2002 to be 18–25.7/100,000; most CA-MRSA isolates were associated with clinically relevant infections, and 23% of people required hospitalization.[115]

CA-MRSA edit

In a US cohort study of 1,300 healthy children, 2.4% carried MRSA in their noses.[107] There are concerns that the presence of MRSA in the environment may allow resistance to be transferred to other bacteria through phages (viruses that infect bacteria). The source of MRSA could come from hospital waste, farm sewage, or other waste water.[4]

LA-MRSA edit

In 2004, MRSA was first isolated on a Dutch pig farm leading to further investigations of livestock associated MRSA (LA-MRSA).[116] Livestock associated MRSA (LA-MRSA) has been observed in Korea, Brazil, Switzerland, Malaysia, India, Great Britain, Denmark, and China.[19]

History edit

 
Incidence of MRSA in human blood samples in countries which took part in the study in 2017

In 1961, the first known MRSA isolates were reported in a British study, and from 1961 to 1967, infrequent hospital outbreaks occurred in Western Europe and Australia,[17] with methicillin then being licensed in England to treat resistant infections. Other reports of MRSA began to be described in the 1970s.[1] Resistance to other antibiotics was documented in some strains of S. aureus. In 1996, vancomycin resistance was reported in Japan.[21]: 637  In many countries, outbreaks of MRSA infection were reported to be transmitted between hospitals.[70]: 402  The rate had increased to 22% by 1995, and by 1997 the level of hospital S. aureus infections attributable to MRSA had reached 50%.

The first report of community-associated MRSA (CA-MRSA) occurred in 1981, and in 1982, a large outbreak of CA-MRSA occurred among intravenous drug users in Detroit, Michigan.[17] Additional outbreaks of CA-MRSA were reported through the 1980s and 1990s, including outbreaks among Australian Aboriginal populations that had never been exposed to hospitals. In the mid-1990s, scattered reports of CA-MRSA outbreaks among US children were made. While HA-MRSA rates stabilized between 1998 and 2008, CA-MRSA rates continued to rise. A report released by the University of Chicago Children's Hospital comparing two periods (1993–1995 and 1995–1997) found a 25-fold increase in the rate of hospitalizations due to MRSA among children in the United States.[117] In 1999, the University of Chicago reported the first deaths from invasive MRSA among otherwise healthy children in the United States.[17] By 2004, the genome for various strains of MRSA were described.[118]

The observed increased mortality among MRSA-infected people arguably may be the result of the increased underlying morbidity of these people. Several studies, however, including one by Blot and colleagues, that have adjusted for underlying disease still found MRSA bacteremia to have a higher attributable mortality than methicillin-susceptible S. aureus (MSSA) bacteremia.[119]

A population-based study of the incidence of MRSA infections in San Francisco during 2004–05 demonstrated that nearly one in 300 residents had such an infection in the course of a year and that greater than 85% of these infections occurred outside of the healthcare setting.[120] A 2004 study showed that people in the United States with S. aureus infection had, on average, three times the length of hospital stay (14.3 vs. 4.5 days), incurred three times the total cost ($48,824 vs. $14,141), and experienced five times the risk of in-hospital death (11.2% vs 2.3%) than people without this infection.[121] In a meta-analysis of 31 studies, Cosgrove et al.,[122] concluded that MRSA bacteremia is associated with increased mortality as compared with MSSA bacteremia (odds ratio= 1.93; 95% CI = 1.93 ± 0.39).[123] In addition, Wyllie et al. report a death rate of 34% within 30 days among people infected with MRSA, a rate similar to the death rate of 27% seen among MSSA-infected people.[124]

In the US, the CDC issued guidelines on October 19, 2006, citing the need for additional research, but declined to recommend such screening.[125] According to the CDC, the most recent estimates of the incidence of healthcare-associated infections that are attributable to MRSA in the United States indicate a decline in such infection rates. Incidence of MRSA central line-associated blood-stream infections as reported by hundreds of intensive care units decreased 50–70% from 2001 to 2007.[126] A separate system tracking all hospital MRSA bloodstream infections found an overall 34% decrease between 2005 and 2008.[126] In 2010, vancomycin was the drug of choice.[4]

Across Europe, based mostly on data from 2013, seven countries (Iceland, Norway, Sweden, the Netherlands, Denmark, Finland, and Estonia, from lowest to highest) had low levels of hospital-acquired MRSA infections compared to the others,[127]: 92–93  and among countries with higher levels, significant improvements had been made only in Bulgaria, Poland, and the British Isles.[127]: 40 

A 1,000-year-old eye salve recipe found in the medieval Bald's Leechbook at the British Library, one of the earliest known medical textbooks, was found to have activity against MRSA in vitro and in skin wounds in mice.[128][129][130]

In the media edit

MRSA is frequently a media topic, especially if well-known personalities have announced that they have or have had the infection.[131][132][133] Word of outbreaks of infection appears regularly in newspapers and television news programs. A report on skin and soft-tissue infections in the Cook County jail in Chicago in 2004–05 demonstrated MRSA was the most common cause of these infections among those incarcerated there.[134] Lawsuits filed against those who are accused of infecting others with MRSA are also popular stories in the media.[135][136]

MRSA is the topic of radio programs,[137] television shows,[138][139][140] books,[141] and movies.[142]

Research edit

Various antibacterial chemical extracts from various species of the sweetgum tree (genus Liquidambar) have been investigated for their activity in inhibiting MRSA. Specifically, these are: cinnamic acid, cinnamyl cinnamate, ethyl cinnamate, benzyl cinnamate, styrene, vanillin, cinnamyl alcohol, 2-phenylpropyl alcohol, and 3-phenylpropyl cinnamate.[143]

The delivery of inhaled antibiotics along with systematic administration to treat MRSA are being developed. This may improve the outcomes of those with cystic fibrosis and other respiratory infections.[103] Phage therapy has been used for years in MRSA in eastern countries, and studies are ongoing in western countries.[144][145]

A 2015 Cochrane systematic review aimed to assess the effectiveness of wearing gloves, gowns and masks to help stop the spread of MRSA in hospitals, however no eligible studies were identified for inclusion. The review authors concluded that there is a need for randomized controlled trials to be conducted to help determine if the use of gloves, gowns, and masks reduces the transmission of MRSA in hospitals.[146]

See also edit

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Further reading edit

 
Wikimedia Commons has media related to MRSA.
  • The Centers for Disease Control and Prevention information, prevention, statistics, at risk groups, causes, educational resources, and environmental factors.
  • National Institute for Occupational Safety and Health information on the bacteria, exposure in the workplace, and reducing risks of being infected.

February 15, 2024
methicillin, resistant, staphylococcus, aureus, mrsa, redirects, here, other, uses, mrsa, disambiguation, mrsa, group, gram, positive, bacteria, that, genetically, distinct, from, other, strains, staphylococcus, aureus, mrsa, responsible, several, difficult, t. MRSA redirects here For other uses see MRSA disambiguation Methicillin resistant Staphylococcus aureus MRSA is a group of gram positive bacteria that are genetically distinct from other strains of Staphylococcus aureus MRSA is responsible for several difficult to treat infections in humans It caused more than 100 000 deaths worldwide attributable to antimicrobial resistance in 2019 Scanning electron micrograph of a human neutrophil ingesting MRSAMRSA is any strain of S aureus that has developed through natural selection or acquired through horizontal gene transfer a multiple drug resistance to beta lactam antibiotics Beta lactam b lactam antibiotics are a broad spectrum group that include some penams penicillin derivatives such as methicillin and oxacillin and cephems such as the cephalosporins 1 Strains unable to resist these antibiotics are classified as methicillin susceptible S aureus or MSSA MRSA infection is common in hospitals prisons and nursing homes where people with open wounds invasive devices such as catheters and weakened immune systems are at greater risk of healthcare associated infection MRSA began as a hospital acquired infection but has become community acquired as well as livestock acquired The terms HA MRSA healthcare associated or hospital acquired MRSA CA MRSA community associated MRSA and LA MRSA livestock associated MRSA reflect this citation needed Contents 1 Signs and symptoms 2 Risk factors 2 1 Hospitalized people 2 2 Prison inmates and military personnel 2 3 Animals 2 4 Athletes 2 5 Children 2 6 Intravenous drug users 3 Mechanism 3 1 SCCmec 3 2 mecA 3 3 Arginine catabolic mobile element 3 4 Strains 4 Diagnosis 4 1 Microbiology 5 Prevention 5 1 Screening 5 2 Handwashing 5 3 Isolation 5 4 Restricting antibiotic use 5 5 Public health considerations 5 6 Decolonization 5 7 Community settings 5 8 Agriculture 6 Treatment 6 1 Antibiotics 6 2 Skin and soft tissue infections 6 3 Children 6 4 Endocarditis and bacteremia 6 5 Respiratory infections 6 6 Bone and joint infections 6 7 Infected implants 6 8 Central nervous system 6 9 Other infections 7 Epidemiology 7 1 HA MRSA 7 2 CA MRSA 7 3 LA MRSA 8 History 9 In the media 10 Research 11 See also 12 References 13 Further readingSigns and symptoms edit nbsp Although usually carried without symptoms MRSA often presents as small red pustular skin infectionsIn humans Staphylococcus aureus is part of the normal microbiota present in the upper respiratory tract 2 and on skin and in the gut mucosa 3 However along with similar bacterial species that can colonize and act symbiotically they can cause disease if they begin to take over the tissues they have colonized or invade other tissues the resultant infection has been called a pathobiont 2 After 72 hours MRSA can take hold in human tissues and eventually become resistant to treatment The initial presentation of MRSA is small red bumps that resemble pimples spider bites or boils they may be accompanied by fever and occasionally rashes Within a few days the bumps become larger and more painful they eventually open into deep pus filled boils About 75 percent of CA MRSA infections are localized to skin and soft tissue and usually can be treated effectively 4 Risk factors editA select few of the populations at risk include People with indwelling implants prostheses drains and catheters 1 5 People who are frequently in crowded places especially with shared equipment and skin to skin contact 6 People with weak immune systems HIV AIDS lupus or cancer patients transplant recipients severe asthmatics etc Diabetics 1 7 Intravenous drug users 8 9 10 Regular contact with someone who has injected drugs in the past year 11 Users of quinolone antibiotics 5 12 Elderly people 5 13 School children sharing sports and other equipment College students living in dormitories 6 People staying or working in a health care facility for an extended period of time 5 6 People who spend time in coastal waters where MRSA is present such as some beaches in Florida and the West Coast of the United States 14 15 People who spend time in confined spaces with other people including occupants of homeless shelters prison inmates and military recruits in basic training 16 17 Veterinarians livestock handlers and pet owners 18 People who ingest unpasteurized milk 19 People who are immunocompromised and also colonized 20 249 People with chronic obstructive pulmonary disease 5 People who have had thoracic surgery 5 As many as 22 of people infected with MRSA do not have any discernable risk factors 21 637 Hospitalized people edit People who are hospitalized including the elderly are often immunocompromised and susceptible to infection of all kinds including MRSA an infection by MRSA is called healthcare associated or hospital acquired methicillin resistant S aureus HA MRSA 1 5 22 23 Generally those infected by MRSA stay infected for just under 10 days if treated by a doctor although effects may vary from person to person 24 Both surgical and nonsurgical wounds can be infected with HA MRSA 1 5 22 Surgical site infections occur on the skin surface but can spread to internal organs and blood to cause sepsis 1 Transmission can occur between healthcare providers and patients because some providers may neglect to perform preventative hand washing between examinations 12 25 People in nursing homes are at risk for all the reasons above further complicated by their generally weaker immune systems 13 26 Prison inmates and military personnel edit Prisons and military barracks 19 can be crowded and confined and poor hygiene practices may proliferate thus putting inhabitants at increased risk of contracting MRSA 18 Cases of MRSA in such populations were first reported in the United States and later in Canada The earliest reports were made by the Centers for Disease Control and Prevention in US state prisons In the news media hundreds of reports of MRSA outbreaks in prisons appeared between 2000 and 2008 For example in February 2008 the Tulsa County jail in Oklahoma started treating an average of 12 S aureus cases per month 27 Animals edit Antibiotic use in livestock increases the risk that MRSA will develop among the livestock and other animals that may reside near them strains MRSA ST 398 and CC398 are transmissible to humans 19 28 Generally animals are asymptomatic 1 Domestic pets are susceptible to MRSA infection by transmission from their owners conversely MRSA infected pets can also transmit MRSA to humans 29 Athletes edit Locker rooms gyms and related athletic facilities offer potential sites for MRSA contamination and infection 30 Athletes have been identified as a high risk group 19 A study linked MRSA to the abrasions caused by artificial turf 31 Three studies by the Texas State Department of Health found the infection rate among football players was 16 times the national average In October 2006 a high school football player was temporarily paralyzed from MRSA infected turf burns His infection returned in January 2007 and required three surgeries to remove infected tissue and three weeks of hospital stay 32 In 2013 Lawrence Tynes Carl Nicks and Johnthan Banks of the Tampa Bay Buccaneers were diagnosed with MRSA Tynes and Nicks apparently did not contract the infection from each other but whether Banks contracted it from either individual is unknown 33 In 2015 Los Angeles Dodgers infielder Justin Turner was infected while the team visited the New York Mets 34 In October 2015 New York Giants tight end Daniel Fells was hospitalized with a serious MRSA infection 35 Children edit MRSA is becoming a critical problem in children 36 studies found 4 6 of patients in U S health care facilities presumably including hospital nurseries 37 were infected or colonized with MRSA 38 Children and adults who come in contact with day care centers 19 playgrounds locker rooms camps dormitories classrooms and other school settings and gyms and workout facilities are at higher risk of contracting MRSA Parents should be especially cautious of children who participate in activities where sports equipment is shared such as football helmets and uniforms 39 Intravenous drug users edit Needle required drugs have caused an increase of MRSA 40 with injection drug use IDU making up 24 1 1 839 individuals of Tennessee Hospital s Discharge System The unsanitary methods of injection causes an access point for the MRSA to enter the blood stream and begin infecting the host Furthermore with MRSA s high contagion rate 11 a common risk factor is individuals who are in constant contact with someone who has injected drugs in the past year Mechanism editAntimicrobial resistance is genetically based resistance is mediated by the acquisition of extrachromosomal genetic elements containing genes that confer resistance to certain antibiotics Examples of such elements include plasmids transposable genetic elements and genomic islands which can be transferred between bacteria through horizontal gene transfer 41 A defining characteristic of MRSA is its ability to thrive in the presence of penicillin like antibiotics which normally prevent bacterial growth by inhibiting synthesis of cell wall material This is due to a resistance gene mecA which stops b lactam antibiotics from inactivating the enzymes transpeptidases critical for cell wall synthesis 42 SCCmec edit Staphylococcal cassette chromosome mec SCCmec is a genomic island of unknown origin containing the antibiotic resistance gene mecA 43 44 SCCmec contains additional genes beyond mecA including the cytolysin gene psm mec which may suppress virulence in HA acquired MRSA strains 45 In addition this locus encodes strain dependent gene regulatory RNAs known as psm mecRNA 46 SCCmec also contains ccrA and ccrB both genes encode recombinases that mediate the site specific integration and excision of the SCCmec element from the S aureus chromosome 43 44 Currently six unique SCCmec types ranging in size from 21 to 67 kb have been identified 43 they are designated types I VI and are distinguished by variation in mec and ccr gene complexes 41 Owing to the size of the SCCmec element and the constraints of horizontal gene transfer a minimum of five clones are thought to be responsible for the spread of MRSA infections with clonal complex CC 8 most prevalent 43 47 SCCmec is thought to have originated in the closely related Staphylococcus sciuri species and transferred horizontally to S aureus 48 Different SCCmec genotypes confer different microbiological characteristics such as different antimicrobial resistance rates 49 Different genotypes are also associated with different types of infections Types I III SCCmec are large elements that typically contain additional resistance genes and are characteristically isolated from HA MRSA strains 44 49 Conversely CA MRSA is associated with types IV and V which are smaller and lack resistance genes other than mecA 44 49 These distinctions were thoroughly investigated by Collins et al in 2001 and can be explained by the fitness differences associated with carriage of a large or small SCCmec plasmid Carriage of large plasmids such as SCCmecI III is costly to the bacteria resulting in a compensatory decrease in virulence expression 50 MRSA is able to thrive in hospital settings with increased antibiotic resistance but decreased virulence HA MRSA targets immunocompromised hospitalized hosts thus a decrease in virulence is not maladaptive 50 In contrast CA MRSA tends to carry lower fitness cost SCCmec elements to offset the increased virulence and toxicity expression required to infect healthy hosts 50 mecA edit mecA is a biomarker gene responsible for resistance to methicillin and other b lactam antibiotics After acquisition of mecA the gene must be integrated and localized in the S aureus chromosome 43 mecA encodes penicillin binding protein 2a PBP2a which differs from other penicillin binding proteins as its active site does not bind methicillin or other b lactam antibiotics 43 As such PBP2a can continue to catalyze the transpeptidation reaction required for peptidoglycan cross linking enabling cell wall synthesis even in the presence of antibiotics As a consequence of the inability of PBP2a to interact with b lactam moieties acquisition of mecA confers resistance to all b lactam antibiotics in addition to methicillin 43 51 mecA is under the control of two regulatory genes mecI and mecR1 MecI is usually bound to the mecA promoter and functions as a repressor 41 44 In the presence of a b lactam antibiotic MecR1 initiates a signal transduction cascade that leads to transcriptional activation of mecA 41 44 This is achieved by MecR1 mediated cleavage of MecI which alleviates MecI repression 41 mecA is further controlled by two co repressors blaI and blaR1 blaI and blaR1 are homologous to mecI and mecR1 respectively and normally function as regulators of blaZ which is responsible for penicillin resistance 43 52 The DNA sequences bound by mecI and blaI are identical 43 therefore blaI can also bind the mecA operator to repress transcription of mecA 52 Arginine catabolic mobile element edit The arginine catabolic mobile element ACME is a virulence factor present in many MRSA strains but not prevalent in MSSA 53 SpeG positive ACME compensates for the polyamine hypersensitivity of S aureus and facilitates stable skin colonization wound infection and person to person transmission 54 Strains edit nbsp Diagram depicting antibiotic resistance through alteration of the antibiotic s target site modeled after MRSA s resistance to penicillin Beta lactam antibiotics permanently inactivate PBP enzymes which are essential for cell wall synthesis and thus for bacterial life by permanently binding to their active sites Some forms of MRSA however express a different PBP that will not allow the antibiotic into its active site Acquisition of SCCmec in methicillin sensitive S aureus MSSA gives rise to a number of genetically different MRSA lineages These genetic variations within different MRSA strains possibly explain the variability in virulence and associated MRSA infections 55 The first MRSA strain ST250 MRSA 1 originated from SCCmec and ST250 MSSA integration 55 Historically major MRSA clones ST2470 MRSA I ST239 MRSA III ST5 MRSA II and ST5 MRSA IV were responsible for causing hospital acquired MRSA HA MRSA infections 55 ST239 MRSA III known as the Brazilian clone was highly transmissible compared to others and distributed in Argentina Czech Republic and Portugal 55 In the UK the most common strains of MRSA are EMRSA15 and EMRSA16 56 EMRSA16 has been found to be identical to the ST36 USA200 strain which circulates in the United States and to carry the SCCmec type II enterotoxin A and toxic shock syndrome toxin 1 genes 57 Under the new international typing system this strain is now called MRSA252 EMRSA 15 is also found to be one of the common MRSA strains in Asia Other common strains include ST5 USA100 and EMRSA 1 58 These strains are genetic characteristics of HA MRSA 59 Community acquired MRSA CA MRSA strains emerged in late 1990 to 2000 infecting healthy people who had not been in contact with healthcare facilities 59 Researchers suggest that CA MRSA did not evolve from HA MRSA 59 This is further proven by molecular typing of CA MRSA strains 60 and genome comparison between CA MRSA and HA MRSA which indicate that novel MRSA strains integrated SCCmec into MSSA separately on its own 59 By mid 2000 CA MRSA was introduced into healthcare systems and distinguishing CA MRSA from HA MRSA became a difficult process 59 Community acquired MRSA is more easily treated and more virulent than hospital acquired MRSA HA MRSA 59 The genetic mechanism for the enhanced virulence in CA MRSA remains an active area of research The Panton Valentine leukocidin PVL genes are of particular interest because they are a unique feature of CA MRSA 55 In the United States most cases of CA MRSA are caused by a CC8 strain designated ST8 USA300 which carries SCCmec type IV Panton Valentine leukocidin PSM alpha and enterotoxins Q and K 57 and ST1 USA400 61 The ST8 USA300 strain results in skin infections necrotizing fasciitis and toxic shock syndrome whereas the ST1 USA400 strain results in necrotizing pneumonia and pulmonary sepsis 55 Other community acquired strains of MRSA are ST8 USA500 and ST59 USA1000 In many nations of the world MRSA strains with different genetic background types have come to predominate among CA MRSA strains USA300 easily tops the list in the U S and is becoming more common in Canada after its first appearance there in 2004 For example in Australia ST93 strains are common while in continental Europe ST80 strains which carry SCCmec type IV predominate 62 63 In Taiwan ST59 strains some of which are resistant to many non beta lactam antibiotics have arisen as common causes of skin and soft tissue infections in the community In a remote region of Alaska unlike most of the continental U S USA300 was found only rarely in a study of MRSA strains from outbreaks in 1996 and 2000 as well as in surveillance from 2004 to 2006 64 A MRSA strain CC398 is found in intensively reared production animals primarily pigs but also cattle and poultry where it can be transmitted to humans as LA MRSA livestock associated MRSA 58 65 66 Diagnosis edit nbsp A selective and differential chromogenic medium for the qualitative direct detection of MRSA nbsp MRSA resistance to oxacillin being tested The top S aureus isolate is a control that is not resistant to oxacillin the other three isolates are MRSA positive nbsp Mueller Hinton agar showing MRSA resistant to an oxacillin diskDiagnostic microbiology laboratories and reference laboratories are key for identifying outbreaks of MRSA Normally a bacterium must be cultured from blood urine sputum or other body fluid samples and in sufficient quantities to perform confirmatory tests early on Still because no quick and easy method exists to diagnose MRSA initial treatment of the infection is often based upon strong suspicion and techniques by the treating physician these include quantitative PCR procedures which are employed in clinical laboratories for quickly detecting and identifying MRSA strains 67 68 Another common laboratory test is a rapid latex agglutination test that detects the PBP2a protein PBP2a is a variant penicillin binding protein that imparts the ability of S aureus to be resistant to oxacillin 69 Microbiology edit Like all S aureus also abbreviated SA at times methicillin resistant S aureus is a gram positive spherical coccus bacterium about 1 micron in diameter It does not form spores and it is not motile It is frequently found in grape like clusters or chains 70 390 Unlike methicillin susceptible S aureus MSSA MRSA is slow growing on a variety of media and has been found to exist in mixed colonies of MSSA The mecA gene which confers resistance to a number of antibiotics is always present in MRSA and usually absent in MSSA however in some instances the mecA gene is present in MSSA but is not expressed Polymerase chain reaction PCR testing is the most precise method for identifying MRSA strains Specialized culture media have been developed to better differentiate between MSSA and MRSA and in some cases such media can be used to identify specific strains that are resistant to different antibiotics 70 402 Other strains of S aureus have emerged that are resistant to oxacillin clindamycin teicoplanin and erythromycin These resistant strains may or may not possess the mecA gene S aureus has also developed resistance to vancomycin VRSA One strain is only partially susceptible to vancomycin and is called vancomycin intermediate S aureus VISA GISA a strain of resistantS aureus is glycopeptide intermediate S aureus and is less suspectible to vancomycin and teicoplanin Resistance to antibiotics in S aureus can be quantified by determining the amount of the antibiotic that must be used to inhibit growth If S aureus is inhibited at a concentration of vancomycin less than or equal to 4 mg ml it is said to be susceptible If a concentration greater than 32 mg ml is necessary to inhibit growth it is said to be resistant 21 637 Prevention editScreening edit In health care settings isolating those with MRSA from those without the infection is one method to prevent transmission Rapid culture and sensitivity testing and molecular testing identifies carriers and reduces infection rates 71 It is especially important to test patients in these settings since 2 of people are carriers of MRSA even though in many of these cases the bacteria reside in the nostril and the patient will not present any symptoms 72 MRSA can be identified by swabbing the nostrils and isolating the bacteria found there Combined with extra sanitary measures for those in contact with infected people swab screening people admitted to hospitals has been found to be effective in minimizing the spread of MRSA in hospitals in the United States Denmark Finland and the Netherlands 73 Handwashing edit The Centers for Disease Control and Prevention offers suggestions for preventing the contraction and spread of MRSA infection which are applicable to those in community settings including incarcerated populations childcare center employees and athletes To prevent the spread of MRSA the recommendations are to wash hands thoroughly and regularly using soap and water or an alcohol based sanitizer Additional recommendations are to keep wounds clean and covered avoid contact with other people s wounds avoid sharing personal items such as razors or towels shower after exercising at athletic facilities and shower before using swimming pools or whirlpools 74 Isolation edit Excluding medical facilities current US guidance does not require workers with MRSA infections to be routinely excluded from the general workplace 75 The National Institutes of Health recommend that those with wound drainage that cannot be covered and contained with a clean dry bandage and those who cannot maintain good hygiene practices be reassigned 75 and patients with wound drainage should also automatically be put on Contact Precaution regardless of whether or not they have a known infection 76 Workers with active infections are excluded from activities where skin to skin contact is likely to occur 77 To prevent the spread of staphylococci or MRSA in the workplace employers are encouraged to make available adequate facilities that support good hygiene In addition surface and equipment sanitizing should conform to Environmental Protection Agency registered disinfectants 75 In hospital settings contact isolation can be stopped after one to three cultures come back negative 78 Before the patient is cleared from isolation it is advised that there is dedicated patient care or single use equipment for that particular patient If this is not possible the equipment must be properly disinfected before it is used on another patient 76 To prevent the spread of MRSA in the home health departments recommend laundering materials that have come into contact with infected persons separately and with a dilute bleach solution to reduce the bacterial load in one s nose and skin and to clean and disinfect those things in the house that people regularly touch such as sinks tubs kitchen counters cell phones light switches doorknobs phones toilets and computer keyboards 79 Restricting antibiotic use edit Glycopeptides cephalosporins and in particular quinolones are associated with an increased risk of colonisation of MRSA Reducing use of antibiotic classes that promote MRSA colonisation especially fluoroquinolones is recommended in current guidelines 12 25 Public health considerations edit Mathematical models describe one way in which a loss of infection control can occur after measures for screening and isolation seem to be effective for years as happened in the UK In the search and destroy strategy that was employed by all UK hospitals until the mid 1990s all hospitalized people with MRSA were immediately isolated and all staff were screened for MRSA and were prevented from working until they had completed a course of eradication therapy that was proven to work Loss of control occurs because colonised people are discharged back into the community and then readmitted when the number of colonised people in the community reaches a certain threshold the search and destroy strategy is overwhelmed 80 One of the few countries not to have been overwhelmed by MRSA is the Netherlands an important part of the success of the Dutch strategy may have been to attempt eradication of carriage upon discharge from hospital 81 Decolonization edit Main article Decolonization medicine As of 2013 no randomized clinical trials had been conducted to understand how to treat nonsurgical wounds that had been colonized but not infected with MRSA 22 and insufficient studies had been conducted to understand how to treat surgical wounds that had been colonized with MRSA 1 As of 2013 whether strategies to eradicate MRSA colonization of people in nursing homes reduced infection rates was not known 26 Care should be taken when trying to drain boils as disruption of surrounding tissue can lead to larger infections including infection of the blood stream 82 Mupirocin 2 ointment can be effective at reducing the size of lesions A secondary covering of clothing is preferred 79 As shown in an animal study with diabetic mice the topical application of a mixture of sugar 70 and 3 povidone iodine paste is an effective agent for the treatment of diabetic ulcers with MRSA infection 83 Community settings edit The examples and perspective in this section deal primarily with the United Kingdom and do not represent a worldwide view of the subject You may improve this section discuss the issue on the talk page or create a new section as appropriate August 2020 Learn how and when to remove this template message Maintaining the necessary cleanliness may be difficult for people if they do not have access to facilities such as public toilets with handwashing facilities In the United Kingdom the Workplace Health Safety and Welfare Regulations 1992 84 require businesses to provide toilets for their employees along with washing facilities including soap or other suitable means of cleaning Guidance on how many toilets to provide and what sort of washing facilities should be provided alongside them is given in the Workplace Health Safety and Welfare Approved Code of Practice and Guidance L24 available from Health and Safety Executive Books but no legal obligations exist on local authorities in the United Kingdom to provide public toilets and although in 2008 the House of Commons Communities and Local Government Committee called for a duty on local authorities to develop a public toilet strategy 85 this was rejected by the Government 86 Agriculture edit See also Antibiotic use in livestock The World Health Organization advocates regulations on the use of antibiotics in animal feed to prevent the emergence of drug resistant strains of MRSA 28 MRSA is established in animals and birds 19 Treatment editAntibiotics edit See also Medications used to treat MRSA Treatment of MRSA infection is urgent and delays can be fatal 20 328 The location and history related to the infection determines the treatment The route of administration of an antibiotic varies Antibiotics effective against MRSA can be given by IV oral or a combination of both and depend on the specific circumstances and patient characteristics 4 The use of concurrent treatment with vancomycin or other beta lactam agents may have a synergistic effect 21 637 Both CA MRSA and HA MRSA are resistant to traditional anti staphylococcal beta lactam antibiotics such as cephalexin CA MRSA has a greater spectrum of antimicrobial susceptibility to sulfa drugs like co trimoxazole trimethoprim sulfamethoxazole tetracyclines like doxycycline and minocycline and clindamycin for osteomyelitis 4 MRSA can be eradicated with a regimen of linezolid 87 though treatment protocols vary and serum levels of antibiotics vary widely from person to person and may affect outcomes 88 The effective treatment of MRSA with linezolid has been successful 87 in 87 of people Linezolid is more effective in soft tissue infections than vancomycin 89 1 This is compared to eradication of infection in those with MRSA treated with vancomycin Treatment with vancomycin is successful in approximately 49 of people 1 Linezolid belongs to the newer oxazolidinone class of antibiotics which has been shown to be effective against both CA MRSA and HA MRSA The Infectious Disease Society of America recommends vancomycin linezolid or clindamycin if susceptible for treating those with MRSA pneumonia 4 Ceftaroline a fifth generation cephalosporin is the first beta lactam antibiotic approved in the US to treat MRSA infections in skin and soft tissue or community acquired pneumonia 90 Vancomycin and teicoplanin are glycopeptide antibiotics used to treat MRSA infections 91 Teicoplanin is a structural congener of vancomycin that has a similar activity spectrum but a longer half life 92 Because the oral absorption of vancomycin and teicoplanin is very low these agents can be administered intravenously to control systemic infections 93 Treatment of MRSA infection with vancomycin can be complicated due to its inconvenient route of administration Moreover the efficacy of vancomycin against MRSA is inferior to that of anti staphylococcal beta lactam antibiotics against methicillin susceptible S aureus MSSA 94 95 Several newly discovered strains of MRSA show antibiotic resistance even to vancomycin and teicoplanin Strains with intermediate 4 8 mg ml levels of resistance termed glycopeptide intermediate S aureus GISA or vancomycin intermediate S aureus VISA 96 97 began appearing in the late 1990s The first identified case was in Japan in 1996 and strains have since been found in hospitals in England France and the US The first documented strain with complete gt 16 mg ml resistance to vancomycin termed vancomycin resistant S aureus VRSA appeared in the United States in 2002 98 In 2011 a variant of vancomycin was tested that binds to the lactate variation and also binds well to the original target thus reinstating potent antimicrobial activity 99 Linezolid quinupristin dalfopristin daptomycin ceftaroline and tigecycline are used to treat more severe infections that do not respond to glycopeptides such as vancomycin 100 Current guidelines recommend daptomycin for VISA bloodstream infections and endocarditis 4 Oxazolidinones such as linezolid became available in the 1990s and are comparable to vancomycin in effectiveness against MRSA Linezolid resistance in S aureus was reported in 2001 101 but infection rates have been at consistently low levels In the United Kingdom and Ireland no linezolid resistance was found in staphylococci collected from bacteremia cases between 2001 and 2006 102 Skin and soft tissue infections edit In skin abscesses the primary treatment recommended is removal of dead tissue incision and drainage More information is needed to determine the effectiveness of specific antibiotics therapy in surgical site infections SSIs 4 Examples of soft tissue infections from MRSA include ulcers impetigo abscesses and SSIs 89 In surgical wounds evidence is weak high risk of bias that linezolid may be better than vancomycin to eradicate MRSA SSIs 1 MRSA colonization is also found in nonsurgical wounds such as traumatic wounds burns and chronic ulcers i e diabetic ulcer pressure ulcer arterial insufficiency ulcer venous ulcer No conclusive evidence has been found about the best antibiotic regimen to treat MRSA colonization 22 Children edit In skin infections and secondary infection sites topical mupirocin is used successfully For bacteremia and endocarditis vancomycin or daptomycin is considered For children with MRSA infected bone or joints treatment is individualized and long term Neonates can develop neonatal pustulosis as a result of topical infection with MRSA 4 Clindamycin is not approved for the treatment of MRSA infection but it is still used in children for soft tissue infections 4 Endocarditis and bacteremia edit Evaluation for the replacement of a prosthetic valve is considered Appropriate antibiotic therapy may be administered for up to six weeks Four to six weeks of antibiotic treatment is often recommended and is dependent upon the extent of MRSA infection 4 Respiratory infections edit CA MRSA in hospitalized patients pneumonia treatment begins before culture results After the susceptibility to antibiotics is performed the infection may be treated with vancomycin or linezolid for up to 21 days If the pneumonia is complicated by the accumulation of pus in the pleural cavity surrounding the lungs drainage may be done along with antibiotic therapy 4 People with cystic fibrosis may develop respiratory complications related to MRSA infection The incidence of MRSA in those with cystic fibrosis increased during 2000 to 2015 by five times Most of these infections were HA MRSA MRSA accounts for 26 of lung infections in those with cystic fibrosis 103 There is insufficient evidence to support the use of topical or systematic antibiotics for nasal or extra nasal MRSA infection 104 Bone and joint infections edit Cleaning the wound of dead tissue and draining abscesses is the first action to treat the MRSA infection Administration of antibiotics is not standardized and is adapted by a case by case basis Antibiotic therapy can last up to 3 months and sometimes even longer 4 Infected implants edit MRSA infection can occur associated with implants and joint replacements Recommendations on treatment are based upon the length of time the implant has been in place In cases of a recent placement of a surgical implant or artificial joint the device may be retained while antibiotic therapy continues If the placement of the device has occurred over 3 weeks ago the device may be removed Antibiotic therapy is used in each instance sometimes long term 4 Central nervous system edit MRSA can infect the central nervous system and form brain abscess subdural empyema and spinal epidural abscess Excision and drainage can be done along with antibiotic treatment Septic thrombosis of cavernous or dural venous sinus can sometimes be a complication 4 Other infections edit Treatment is not standardized for other instances of MRSA infection in a wide range of tissues Treatment varies for MRSA infections related to subperiosteal abscesses necrotizing pneumonia cellulitis pyomyositis necrotizing fasciitis mediastinitis myocardial perinephric hepatic and splenic abscesses septic thrombophlebitis and severe ocular infections including endophthalmitis 4 Pets can be reservoirs and pass on MRSA to people In some cases the infection can be symptomatic and the pet can develop a MRSA infection Health departments recommend that the pet be taken to the veterinarian if MRSA infections keep occurring in the people who have contact with the pet 79 Epidemiology editWorldwide an estimated 2 billion people carry some form of S aureus of these up to 53 million 2 7 of carriers are thought to carry MRSA 105 S aureus was identified as one of the six leading pathogens for deaths associated with resistance in 2019 and 100 000 deaths caused by MRSA were attributable to antimicrobial resistance 106 HA MRSA edit In a US cohort study of 1 300 healthy children 2 4 carried MRSA in their nose 107 Bacterial sepsis occurs with most 75 of cases of invasive MRSA infection 4 In 2009 there were an estimated 463 017 hospitalizations due to MRSA or a rate of 11 74 per 1 000 hospitalizations 108 Many of these infections are less serious but the Centers for Disease Control and Prevention CDC estimate that there are 80 461 invasive MRSA infections and 11 285 deaths due to MRSA annually 109 In 2003 the cost for a hospitalization due to MRSA infection was US 92 363 a hospital stay for MSSA was 52 791 89 Infection after surgery is relatively uncommon but occurs as much as 33 in specific types of surgeries Infections of surgical sites range from 1 to 33 MRSA sepsis that occurs within 30 days following a surgical infection has a 15 38 mortality rate MRSA sepsis that occurs within one year has a mortality rate of around 55 There may be increased mortality associated with cardiac surgery There is a rate of 12 9 in those infected with MRSA while only 3 infected with other organisms SSIs infected with MRSA had longer hospital stays than those who did not 1 Globally MRSA infection rates are dynamic and vary year to year 110 According to the 2006 SENTRY Antimicrobial Surveillance Program report the incidence of MRSA bloodstream infections was 35 9 in North America MRSA blood infections in Latin America was 29 European incidence was 22 8 The rate of all MRSA infections in Europe ranged from 50 in Portugal down to 0 8 in Sweden Overall MRSA infection rates varied in Latin America Colombia and Venezuela combined had 3 Mexico had 50 Chile 38 Brazil 29 and Argentina 28 89 The Centers for Disease Control and Prevention CDC estimated that about 1 7 million nosocomial infections occurred in the United States in 2002 with 99 000 associated deaths 111 The estimated incidence is 4 5 nosocomial infections per 100 admissions with direct costs at 2004 prices ranging from 10 500 5300 8000 at 2006 rates per case for bloodstream urinary tract or respiratory infections in immunocompetent people to 111 000 57 000 85 000 per case for antibiotic resistant infections in the bloodstream in people with transplants With these numbers conservative estimates of the total direct costs of nosocomial infections are above 17 billion The reduction of such infections forms an important component of efforts to improve healthcare safety BMJ 2007 citation needed MRSA alone was associated with 8 of nosocomial infections reported to the CDC National Healthcare Safety Network from January 2006 to October 2007 112 The British National Audit Office estimated that the incidence of nosocomial infections in Europe ranges from 4 to 10 of all hospital admissions As of early 2005 the number of deaths in the United Kingdom attributed to MRSA has been estimated by various sources to lie in the area of 3 000 per year 113 In the United States an estimated 95 million people carry S aureus in their noses of these 2 5 million 2 6 of carriers carry MRSA 114 A population review conducted in three U S communities showed the annual incidence of CA MRSA during 2001 2002 to be 18 25 7 100 000 most CA MRSA isolates were associated with clinically relevant infections and 23 of people required hospitalization 115 CA MRSA edit In a US cohort study of 1 300 healthy children 2 4 carried MRSA in their noses 107 There are concerns that the presence of MRSA in the environment may allow resistance to be transferred to other bacteria through phages viruses that infect bacteria The source of MRSA could come from hospital waste farm sewage or other waste water 4 LA MRSA edit In 2004 MRSA was first isolated on a Dutch pig farm leading to further investigations of livestock associated MRSA LA MRSA 116 Livestock associated MRSA LA MRSA has been observed in Korea Brazil Switzerland Malaysia India Great Britain Denmark and China 19 History edit nbsp Incidence of MRSA in human blood samples in countries which took part in the study in 2017In 1961 the first known MRSA isolates were reported in a British study and from 1961 to 1967 infrequent hospital outbreaks occurred in Western Europe and Australia 17 with methicillin then being licensed in England to treat resistant infections Other reports of MRSA began to be described in the 1970s 1 Resistance to other antibiotics was documented in some strains of S aureus In 1996 vancomycin resistance was reported in Japan 21 637 In many countries outbreaks of MRSA infection were reported to be transmitted between hospitals 70 402 The rate had increased to 22 by 1995 and by 1997 the level of hospital S aureus infections attributable to MRSA had reached 50 The first report of community associated MRSA CA MRSA occurred in 1981 and in 1982 a large outbreak of CA MRSA occurred among intravenous drug users in Detroit Michigan 17 Additional outbreaks of CA MRSA were reported through the 1980s and 1990s including outbreaks among Australian Aboriginal populations that had never been exposed to hospitals In the mid 1990s scattered reports of CA MRSA outbreaks among US children were made While HA MRSA rates stabilized between 1998 and 2008 CA MRSA rates continued to rise A report released by the University of Chicago Children s Hospital comparing two periods 1993 1995 and 1995 1997 found a 25 fold increase in the rate of hospitalizations due to MRSA among children in the United States 117 In 1999 the University of Chicago reported the first deaths from invasive MRSA among otherwise healthy children in the United States 17 By 2004 the genome for various strains of MRSA were described 118 The observed increased mortality among MRSA infected people arguably may be the result of the increased underlying morbidity of these people Several studies however including one by Blot and colleagues that have adjusted for underlying disease still found MRSA bacteremia to have a higher attributable mortality than methicillin susceptible S aureus MSSA bacteremia 119 A population based study of the incidence of MRSA infections in San Francisco during 2004 05 demonstrated that nearly one in 300 residents had such an infection in the course of a year and that greater than 85 of these infections occurred outside of the healthcare setting 120 A 2004 study showed that people in the United States with S aureus infection had on average three times the length of hospital stay 14 3 vs 4 5 days incurred three times the total cost 48 824 vs 14 141 and experienced five times the risk of in hospital death 11 2 vs 2 3 than people without this infection 121 In a meta analysis of 31 studies Cosgrove et al 122 concluded that MRSA bacteremia is associated with increased mortality as compared with MSSA bacteremia odds ratio 1 93 95 CI 1 93 0 39 123 In addition Wyllie et al report a death rate of 34 within 30 days among people infected with MRSA a rate similar to the death rate of 27 seen among MSSA infected people 124 In the US the CDC issued guidelines on October 19 2006 citing the need for additional research but declined to recommend such screening 125 According to the CDC the most recent estimates of the incidence of healthcare associated infections that are attributable to MRSA in the United States indicate a decline in such infection rates Incidence of MRSA central line associated blood stream infections as reported by hundreds of intensive care units decreased 50 70 from 2001 to 2007 126 A separate system tracking all hospital MRSA bloodstream infections found an overall 34 decrease between 2005 and 2008 126 In 2010 vancomycin was the drug of choice 4 Across Europe based mostly on data from 2013 seven countries Iceland Norway Sweden the Netherlands Denmark Finland and Estonia from lowest to highest had low levels of hospital acquired MRSA infections compared to the others 127 92 93 and among countries with higher levels significant improvements had been made only in Bulgaria Poland and the British Isles 127 40 A 1 000 year old eye salve recipe found in the medieval Bald s Leechbook at the British Library one of the earliest known medical textbooks was found to have activity against MRSA in vitro and in skin wounds in mice 128 129 130 In the media editMRSA is frequently a media topic especially if well known personalities have announced that they have or have had the infection 131 132 133 Word of outbreaks of infection appears regularly in newspapers and television news programs A report on skin and soft tissue infections in the Cook County jail in Chicago in 2004 05 demonstrated MRSA was the most common cause of these infections among those incarcerated there 134 Lawsuits filed against those who are accused of infecting others with MRSA are also popular stories in the media 135 136 MRSA is the topic of radio programs 137 television shows 138 139 140 books 141 and movies 142 Research editVarious antibacterial chemical extracts from various species of the sweetgum tree genus Liquidambar have been investigated for their activity in inhibiting MRSA Specifically these are cinnamic acid cinnamyl cinnamate ethyl cinnamate benzyl cinnamate styrene vanillin cinnamyl alcohol 2 phenylpropyl alcohol and 3 phenylpropyl cinnamate 143 The delivery of inhaled antibiotics along with systematic administration to treat MRSA are being developed This may improve the outcomes of those with cystic fibrosis and other respiratory infections 103 Phage therapy has been used for years in MRSA in eastern countries and studies are ongoing in western countries 144 145 A 2015 Cochrane systematic review aimed to assess the effectiveness of wearing gloves gowns and masks to help stop the spread of MRSA in hospitals however no eligible studies were identified for inclusion The review authors concluded that there is a need for randomized controlled trials to be conducted to help determine if the use of gloves gowns and masks reduces the transmission of MRSA in hospitals 146 See also editMRSA ST398References edit a b c d e f g h i j k l m Gurusamy KS Koti R Toon CD Wilson P Davidson BR August 2013 Antibiotic therapy for the treatment of methicillin resistant Staphylococcus aureus MRSA infections in surgical wounds The Cochrane Database of Systematic Reviews 8 CD009726 doi 10 1002 14651858 CD009726 pub2 PMID 23963687 a b Schenck LP Surette MG Bowdish DM November 2016 Composition and immunological significance of the upper respiratory tract microbiota FEBS 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PMID 26265721 Anonye BO Nweke V Furner Pardoe J Gabrilska R Rafiq A Ukachukwu F et al 2020 The safety profile of Bald s eyesalve for the treatment of bacterial infections Scientific Reports 10 1 17513 Bibcode 2020NatSR 1017513A doi 10 1038 s41598 020 74242 2 PMC 7562736 PMID 33060666 Thompson N Smith Spark L 31 March 2015 Thousand year old Anglo Saxon potion kills MRSA superbug CNN News CNN Time Warner Retrieved 1 April 2015 Bucs Nicks Tynes have MRSA infections Tampa Bay Times Retrieved 3 June 2017 Correspondent EC 12 October 2015 MRSA The tiny bacteria that can tackle giants CNN Retrieved 3 June 2017 a href Template Cite web html title Template Cite web cite web a CS1 maint multiple names authors list link Biddle S Cush A This Australian Says He and His Dead Friend Invented Bitcoin Gizmodo Retrieved 3 June 2017 Singh J Johnson RC Schlett CD Elassal EM Crawford KB Mor D et al 2016 10 26 Multi Body Site Microbiome and Culture Profiling of Military Trainees Suffering from Skin and Soft Tissue Infections at Fort Benning Georgia mSphere 1 5 e00232 16 doi 10 1128 mSphere 00232 16 PMC 5064451 PMID 27747300 Hospital Infection Lawsuits are on the Rise AboutLawsuits com www aboutlawsuits com 2 December 2008 Retrieved 3 June 2017 Doc who treated superbug vic was sued before New York Daily News November 2007 Retrieved 3 June 2017 MRSA The Drug Resistant Superbug That Won t Die NPR org Retrieved 3 June 2017 Should I Worry About MRSA TV Episode 2004 IMDb 23 September 2004 Retrieved 3 June 2017 McKenna M Resistance The Movie That Will Make You Care About Antibiotic Misuse Wired Retrieved 3 June 2017 Line of Duty series 4 Everything you need to know Digital Spy 24 April 2017 Retrieved 3 June 2017 results s 1 February 2011 Superbug The Fatal Menace of MRSA Free Press ISBN 978 1 4165 5728 9 Facing the Future of Antibiotic Resistance The Change Starts Here HuffPost UK 18 July 2016 Retrieved 3 June 2017 Lingbeck JM O Bryan CA Martin EM Adams JP Crandall PG 2015 Sweetgum An ancient source of beneficial compounds with modern benefits Pharmacognosy Reviews 9 17 1 11 doi 10 4103 0973 7847 156307 PMC 4441155 PMID 26009686 Reardon S June 2014 Phage therapy gets revitalized Nature 510 7503 15 6 Bibcode 2014Natur 510 15R doi 10 1038 510015a PMID 24899282 S2CID 205081324 Robson D The viruses that may save humanity Retrieved 2018 09 25 Lopez Alcalde J Mateos Mazon M Guevara M Conterno LO Sola I Cabir Nunes S et al July 2015 Gloves gowns and masks for reducing the transmission of meticillin resistant Staphylococcus aureus MRSA in the hospital setting The Cochrane Database of Systematic Reviews 2015 7 CD007087 doi 10 1002 14651858 cd007087 pub2 PMC 7026606 PMID 26184396 Further reading edit nbsp Wikimedia Commons has media related to MRSA The Centers for Disease Control and Prevention information prevention statistics at risk groups causes educational resources and environmental factors National Institute for Occupational Safety and Health information on the bacteria exposure in the workplace and reducing risks of being infected Retrieved from https en wikipedia org w index php title Methicillin resistant Staphylococcus aureus amp oldid 1201968652, wikipedia, wiki, book, books, library,

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