Skin and soft tissue infections caused by methicillin-resistant Staphylococcus aureus USA300 clone.Until recently, methicillin-resistant Staphylococcus aureus methicillin-resistant Staphylococcus aureus Methicillin-aminoglycoside resistant Staphylococcus aureus, MRSA An organism with multiple antibiotic resistances–eg, aminoglycosides, chloramphenicol, clindamycin, erythromycin, rifampin, tetracycline, (MRSA MRSA Methicillin-resistant Staphylococcus aureus. See MARSA. ) has caused predominantly healthcare-associated infections. We studied MRSA infections and overall skin and soft tissue infections (SSTIs) in outpatients receiving care at the Baltimore Veterans Affairs Medical Center Emergency Care Service during 2001-2005. We found an increase in MRSA infections, from 0.2 to 5.9 per 1,000 visits (p<0.01); most were community-associated SSTIs. Molecular typing showed that >80% of MRSA infections were caused by USA300. In addition, SSTI SSTI State Science & Technology Institute (Westerville, OH) SSTI Skin and Soft Tissue Infection SSTI Small Spacecraft Technology Initiative SSTI Skin and Skin Structure Infection SSTI Six Sigma Technical Institute visits increased from 20 to 61 per 1,000 visits (p<0.01). The proportion of SSTI cultures that yielded MRSA increased from 4% to 42% (p<0.01), while the proportion that yielded methicillin-sensitive S. aureus The aureus (pl. aurei) was a gold coin of ancient Rome valued at 25 silver denarii. The aureus was regularly issued from the 1st century BC to the beginning of the 4th century AD, when it was replaced by the solidus. remained the same (10% to 13%, p = 0.5). The increase in community-associated MRSA infections and the overall increase in SSTIs in our population suggest that USA300 is becoming more virulent and has a greater to cause SSTIs. ********** Methicillin-resistant Staphylococcus aureus (MRSA) has been a cause of predominantly nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. or healthcare-associated infections. MRSA infections usually affect patients during hospitalization, after surgery, and during stays in long-term care facilities. In addition, MRSA infections are common in patients who have indwelling indwelling /in·dwell·ing/ (in´dwel-ing) pertaining to a catheter or other tube left within an organ or body passage for drainage, to maintain patency, or for the administration of drugs or nutrients. vascular catheters for dialysis or other medical treatments. However, during the past decade, multiple reports of community-associated MRSA (CA-MRSA CA-MRSA Community Acquired Methicillin-Resistant Staphylococcus Aureus ) infections have been reported in patients who lack the above risk factors (1-4). CA-MRSA infections differ from healthcare-associated MRSA (HA-MRSA) infections in a number of ways. CA-MRSA infections are predominantly skin and soft tissue infections (SSTIs), are often susceptible to other non-[beta]-1actam antimicrobial drugs, and carry a type IV or V staphylococcal staphylococcal pertaining to Staphylococcus spp. staphylococcal clumping test used as a means of measuring the quantity of fibrinogen-split products in a sample of blood. cassette chromosome (SCC SCC - strongly connected component ) with the mecA gene. In contrast, HA-MRSA infections are found at multiple sites, are usually multidrug resistant, and carry the SCCmec types I, II, and III (5,6). In the United States, 2 major clones of CA-MRSA have been identified by pulsed-field gel electrophoresis (PFGE PFGE Pulsed-Field Gel Electrophoresis ) and named USA300 and USA400 by the Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. (CDC See Control Data, century date change and Back Orifice. CDC - Control Data Corporation ) (7). Among the community-associated types, the USA300 clone has recently emerged as the predominant cause of SSTIs in the United States (8,9). Toxin expression between CA-MRSA and HA-MRSA strains differs. Most CA-MRSA strains carry the intracellular toxin intracellular toxin n. See endotoxin. Panton-Valentine leukocidin Panton-Valentine leukocidin a nonhemolytic toxin produced by Staphylococcus aureus which kills segmented neutrophils and macrophages. (PVL PVL Periventricular Leukomalacia PVL Prevail PVL Parameter Value Language PVL Pade Via Lanczos (circuit modeling) PVL Physical Volume Library PVL Pascack Valley Line (New Jersey Transit commuter rail line) ), which is known for pore formation on polymorphonuclear polymorphonuclear /poly·mor·pho·nu·cle·ar/ (-noo´kle-er) having a nucleus so deeply lobed or so divided as to appear to be multiple. pol·y·mor·pho·nu·cle·ar adj. Having a lobed nucleus. cells of the host (10,11). In addition, the USA300 clone contains the arginine arginine (är`jənĭn), organic compound, one of the 20 amino acids commonly found in animal proteins. Only the l-stereoisomer participates in the biosynthesis of proteins. catabolic Catabolic A metabolic process in which energy is released through the conversion of complex molecules into simpler ones. Mentioned in: Anabolic Steroid Use catabolic see catabolism. mobile element (ACME), which inhibits polymorphonuclear cell production (10). In the summer of 2004, physicians in our Emergency Care Service (ECS See eComStation. ) alerted us to an increased number of outpatients who had SSTIs caused by MRSA. This observation led us to begin this investigation with the following objectives: 1) to measure the incidence of MRSA infections in our ECS, 2) to describe these infections and their isolates, and 3) to measure the incidence of SSTIs in our ECS and the entire associated healthcare system over the past 5 years. We present molecular and epidemiologic evidence that the emergence of the USA300 clone has led to not only an increase in CA-MRSA infections but also an overall increase in SSTIs in our patient population. Methods Setting The population for our retrospective study retrospective study, a study in which a search is made for a relationship between one phenomenon or condition and another that occurred in the past (e.g. was derived from the Veterans Affairs Maryland Health Care System (VAMHCS VAMHCS Veterans Affairs Maryland Health Care System ), which provides comprehensive health care to >45,000 veterans in the Maryland area. Outpatient care is provided at 2 medical centers and 3 community-based outpatient clinics. Our ECS is located in the Baltimore VA Medical Center and serves [approximately equal to] 85 patients a day. MRSA Infections We reviewed microbiology cultures obtained during an ECS visit from October 1, 2000, through September 30, 2005 (fiscal years [FYs] 2001-2005), in which MRSA was first isolated from a patient's culture. The total number of ECS visits per FY was obtained from administrative records. The MRSA infection risk was calculated by dividing the total number of ECS patients whose culture results were MRSA positive for the first time by the number of ECS visits per FY. Information about patient demographics, clinical manifestations, and risk factors for nosocomial acquisition of MRSA was obtained from manual review of the VA's computerized patient record system. Patients were categorized as to site of infection as follows: SST SST: see airplane. 1 (wound culture positive for MRSA in the setting of new erythema erythema (ĕr'əthē`mə), more or less diffuse redness of the skin due to concentration of an abnormally large amount of blood within the small vessels of the skin (hyperemia), as in burns. , induration induration /in·du·ra·tion/ (in?du-ra´shun) 1. sclerosis or hardening. 2. hardness. 3. an abnormally hard spot or place. , warmth or pain at that site), urinary tract infection urinary tract infection (UTI), n infection in one or more of the structures that make up the urinary system. Occurs more often in women and is most commonly caused by bacteria. (positive urine culture Urine Culture Definition A urine culture is a diagnostic laboratory test performed to detect the presence of bacteria in the urine (bacteriuria). in addition to at least 1 sign or symptom of a urinary tract infection), and pneumonia (positive sputum culture Sputum Culture Definition Sputum is material coughed up from the lungs and expectorated (spit out) through the mouth. A sputum culture is done to find and identify the microorganism causing an infection of the lower respiratory tract such as pneumonia for MRSA in addition to a new infiltrate on chest radiograph radiograph /ra·dio·graph/ (-graf?) the film produced by radiography. ra·di·o·graph n. ). The infection was classified as healthcare-associated if the patient had a history of hospitalization, surgery, dialysis, or had been a resident in a long-term care facility within 1 year before infection or had a percutaneous medical device or permanent indwelling catheter indwelling catheter Any catheter, usually understood to be for the urinary bladder–eg, a 'Foley' left in place for a prolonged period of time at the time of infection. An infection in a patient without these risk factors was categorized as community-associated (12). MRSA Isolates Clinical cultures were sent to the clinical microbiology laboratory of the VAMHCS. S. aureus was identified by following standard laboratory protocols. MRSA was defined as an S. aureus isolate that grew on oxacillin oxacillin /ox·a·cil·lin/ (ok?sah-sil´in) a semisynthetic penicillinase-resistant penicillin used as the sodium salt in infections due to penicillin-resistant, gram-positive organisms. screen agar; methicillin-susceptible S. aureus (MSSA MSSA Methicillin-Sensitive Staphylococcus Aureus MSSA Microscopy Society of Southern Africa MSSA Maryland Saltwater Sportfishermen's Association MSSA Military Selective Service Act MSSA Mid-South Sociological Association MSSA Minnesota Social Service Association ) was defined as an isolate that did not grow on oxacillin screen agar. Anti-microbial drug susceptibility was determined by following the methods and interpretation guidelines of the Clinical and Laboratory Standards Institute (13). Erythromycin-resistant and clindamycin-susceptible isolates were tested for inducible resistance by the D-test, following the guidelines that began on January 30, 2004. Clindamycin resistance data include all isolates that are truly resistant by breakpoint The location in a program used to temporarily halt the program for testing and debugging. Lines of code in a source program are marked for breakpoints. When those instructions are about to be executed, the program stops, allowing the programmer to examine the status of the program and isolates that have inducible resistance detected by the D-test. All isolates were frozen at -70[degrees]C in trypticase soy broth with 30% glycerol glycerol, glycerin, glycerine, or 1,2,3-propanetriol (prō`pāntrī'ŏl), CH2OHCHOHCH2OH, colorless, odorless, sweet-tasting, syrupy liquid. . MRSA isolates (n = 329) were typed by DNA sequencing analysis of the protein A (spa) gene hypervariable region hypervariable region regions present on light and heavy chains of immunoglobulins where most of the variation in amino acid sequences occurs. These are also sites of antigen binding. as described (14). Allele allele (əlēl`): see genetics. allele Any one of two or more alternative forms of a gene that may occur alternatively at a given site on a chromosome. identification was based on comparison with sequences in an S. aureus database (www.ridom.de/spaserver). PVL (15) and ACME (10) virulence factors were detected by following published protocols. PFGE was performed according to McDougal et al. (7). Photographic images of the gels were saved digitally with the Geldoc EQ (BioRad Laboratories, Hercules, CA, USA); gel analysis was saved with Fingerprinting II Software (BioRad Laboratories). The reference standard S. aureus NCTC NCTC National Conservation Training Center NCTC National Counterterrorism Center (9/11 Commission Report) NCTC National Cable Television Cooperative NCTC National Collection of Type Cultures (UK laboratory) 8325 was included in the first and fifteenth lane of each gel, and all isolates were normalized to this global standard. The band patterns were compared by means of the Dice coefficient by using the unweighted pair-group method to determine band similarity and following the criteria established by Tenover et al. to define the pulsed-field type clusters (16). We defined USA300 as isolates that had the MBQBLO repeat motif and were positive for PVL and ACME. SSTIs For SSTIs, the total number of ECS visits (n = 3,688) and VAMHCS visits (n = 13,041) per FY, according to codes from the International Classification of Disease, Clinical Modification 9 (ICD-9-CM ICD-9-CM International Classification of Disease, 9th edition, Clinical Modification A standardized classification of disease, injuries, and causes of death, by etiology and anatomic localization and codified into a 6-digit number, which allows ) (680, carbuncle carbuncle, acute inflammatory nodule of the skin caused by bacterial invasion into the hair follicles or sebaceous gland ducts. It is actually a boil, but one that has more than one focus of infection, i.e., involves several follicles or ducts. and furuncle furuncle /fu·run·cle/ (fu´rung-k'l) a boil; a painful nodule formed in the skin by circumscribed inflammation of the dermis and subcutaneous tissue, enclosing a central slough or “core”; due to staphylococci entering the skin through ; 681, cellulitis Cellulitis Definition Cellulitis is a spreading bacterial infection just below the skin surface. It is most commonly caused by Streptococcus pyogenes or Staphylococcus aureus. and abscess abscess, localized inflamation associated with tissue necrosis. Abscesses are characterized by inflamation, which is due to the accumulation of pus in the local tissues, and often painful swelling. of finger and toe; 682, other cellulitis and abscess; 704.8, folliculitis Folliculitis Definition Folliculitis is inflammation or infection of one or more hair follicles (openings in the skin that enclose hair). Description Folliculitis can affect both women and men at any age. ), were obtained from administrative records. The rate of SSTIs was calculated for the ECS and the VAMHCS by dividing the number of total visits for SSTIs by the number of visits per FY for each site. We also measured the number of patients who had SSTIs by taking the first patient visit for each year. Finally, we assessed whether patients' infections were cultured during their visits for SSTI and whether that culture grew MRSA or MSSA. Statistical Analysis Rates were computed as previously mentioned. Proportions were used to describe categorical variables and means to describe continuous variables. Categorical variables were compared by using ;(2 or Fisher exact tests, as appropriate; continuous variables were compared by using Student t test. Statistical analysis was performed by using SPSS A statistical package from SPSS, Inc., Chicago (www.spss.com) that runs on PCs, most mainframes and minis and is used extensively in marketing research. It provides over 50 statistical processes, including regression analysis, correlation and analysis of variance. version 12.5 (SPSS Inc., Chicago, IL, USA). Results The proportion of ECS visits for MRSA infections for patients with no history of MRSA colonization or infection increased significantly from 0.2 per 1,000 ECS visits in FY01 to 5.9 per 1,000 visits in FY05 (p<0.01, [chi square chi square (kī), n a nonparametric statistic used with discrete data in the form of frequency count (nominal data) or percentages or proportions that can be reduced to frequencies. ] test; Figure 1). The absolute number rose from 6 in FY01 to 180 in FY05, and 280 (81%) of 329 cases occurred during FY04 and FY05. In FY01, only 3 SSTIs were caused by MRSA compared with 159 in FY05. [FIGURE 1 OMITTED] The mean age of patients with new MRSA infections (n = 329) was 56 years; 98% were male, 69% were African American African American Multiculture A person having origins in any of the black racial groups of Africa. See Race. , 84% had an SSTI, 8% had a urinary tract infection, 2% had pneumonia, and 6% had other sites of infection. Of these 329 MRSA isolates, 76% were susceptible to clindamycin, 85% to tetracycline tetracycline (tĕ'trəsī`klēn), any of a group of antibiotics produced by bacteria of the genus Streptomyces. They are effective against a wide range of Gram positive and Gram negative bacteria, interfering with protein (n = 257), and 97% to trimethoprim-sulfamethoxazole. Overall, 217 (66%) of the 329 patients with MRSA infections had no known contact with the healthcare system in the year before their infection and most likely acquired MRSA in the community. Molecular typing was performed on 296 (90%) of the 329 MRSA isolates from these infections. Spa typing showed a single dominant clonal type with the MBQBLO repeat motif (Table 1). The proportion of isolates tested with this spa type group significantly increased from 0% in FY01 to 89% in FY05 (p<0.01, [chi square] test). Isolates that contained the virulence factors PVL and ACME also increased significantly from 0% in FY01 to 93% in FY04 and 89% in FY05 (p<0.01, [chi square] test) and strongly correlated with isolates of the MBQBLO repeat motif. Molecular studies showed that isolates defined as USA300 by having the MBQBLO repeat motif and being positive for PVL and ACME increased from 0% in FY01 to 84% in FY05 and that USA300 was the dominant clone in FY03-FY05. To confirm that isolates of the spa clonal type that had the MBQBLO repeat motif and were positive for ACME and PVL represent USA300, we performed PFGE on a subset of the isolates (n = 31). This subset consisted of a random selection of 10% of the total isolates. Sixteen isolates were positive for USA300 by both typing methods: 1) PFGE and 2) containing the MBQBLO repeat motif, PVL, and ACME. Three isolates had PFGE types similar to USA300 and PVL but had neither the MBQBLO repeat motif nor ACME. Twelve of the isolates did not have PFGE or spa types similar to USA300. No isolate was positive for MBQBLO repeat motif, PVL, and ACME and negative for USA300 by PFGE. When the MBQBLO that were ACME and PVL positive were compared with PFGE patterns for USA300, the sensitivity was 84% and the specificity was 100%; positive predicted value was 100% and negative predicted value was 80%. Not all isolates that were USA300 according to PFGE correlated with the MBQBLO repeat motif and were positive for PVL and ACME. One isolate had an unrelated spa type (BQBPO repeat motif), and 2 isolates were negative for ACME. Eighteen of these isolates had the MBQBLO repeat motif, and PFGE showed a similarity to PFGE type USA300 (Figure 2). PFGE in our study determined that all of these related USA300 isolates carried PVL and all except 2 carried the ACME virulence factor. The 2 without ACME were closely related to SCCmec IVb type. However, of the overall 329 MRSA isolates, 5 had the MBQBLO repeat motif and were PVL positive but ACME negative. Four isolates had the MBQBLO repeat motif (spa type t064) but were negative for PVL and ACME and similar to USA500 according to PFGE; these isolates were excluded from our definition of USA300. [FIGURE 2 OMITTED] Because most of these MRSA infections were SSTIs and because our ECS physicians thought they were seeing more abscesses, we looked at the rate of SSTIs in the ECS. The rate of ECS visits for SST1 significantly increased from 20 per 1,000 ECS visits in FY01 to 61 per 1,000 visits in FY05 (Figure 3). Because of concerns that some of the same patients had multiple visits, we looked at patients with SSTIs in each year. The results were similar to SSTI visits and showed an increase over the years in the number of patients with SSTIs (Table 2). The absolute number and the proportion of patients for whom culture was performed increased from FY01-03 through FY04-05 (p<0001, [chi square] test). We then examined the absolute number and the proportion of patients for whom cultures were performed and grew S. aureus (MRSA or MSSA). For our comparison of MRSA and MSSA, we chose this measurement to account for the increase in culturing. For MRSA, the absolute number and proportion of patients for whom cultures were performed and grew MRSA increased significantly from FY01-03 through FY04-05 (p<0001, [chi square] test). For MSSA, the absolute number of patients for whom cultures were performed and grew MSSA increased from FY01-03 through FY04 05, but the proportion of patients for whom cultures were performed and grew MSSA remained the same (p = 0.10, [chi square] test). Because of concerns that there may have been shifts in where care was delivered within our healthcare system, we also examined the number and rate of SSTIs for the entire VAMHCS. Absolute numbers of visits increased, with 2,020 visits in FY01, 1,972 in FY02, 2,190 in FY03, 3,337 in FY04, and 3,522 in FY05. The rate of SSTI visits also increased (2.75 SSTI visits per 1,000 visits in FY01-03 vs. 3.89 SSTI visits per 1,000 visits in FY04-05; p<0.001). [FIGURE 3 OMITTED] Discussion During our 5-year study, we had an [approximately equal to]4-fold increase in the incidence of MRSA infections, primarily SSTls in people who had no risk factors for acquiring the infection from a healthcare setting. We showed that this increase was due to the USA300 clone and associated with an overall increase in SSTIs in our ECS and in the healthcare system as a whole. For these patients with SSTIs, the absolute number and proportion of those for whom a culture was performed and grew MRSA increased. We believe this reflects the increase in MRSA infections due to USA300. The absolute number of patients for whom a culture was performed and grew MSSA also increased, but the proportion remained the same. We believe the absolute numbers increased because more cultures were performed, not because MSSA infections increased. Other reports of community-onset MRSA infections throughout the United States have been published (5,8,17-19). A recent publication by King et al. showed that USA300 was the predominant cause of SSTIs in the community (8). Carlton et al. also documented an increase in the number of total MRSA infections in San Francisco during 1996-2002 (9). This increase was shown to coincide with a statistically significant temporal increase in the number of community-onset MRSA infections. This study and our study support the hypothesis that CA-MRSA strains have factors that facilitate their spread in the community (18,20,21). Despite the retrospective nature of our investigation, we were able to obtain 90% of the MRSA isolates for molecular typing. Molecular characterization of new cases of MRSA showed a dramatic increase in isolates with the MBQBLO repeat motif in the later years. This increase in these related spa types is consistent with the increase in the PFGE type USA300 seen by others (6,19). Not surprisingly, with the increase in the MBQBLO repeat motif, we also observed an increase in the virulence factors PVL and ACME. We did find 4 isolates of the spa type 65 that were negative for PVL and ACME and were similar to USA500 by PFGE and 5 isolates that were spa type 8 and positive for PVL but negative for ACME. This finding was not surprising because this phenomenon has been recently described; only isolates with the SCC mec IVa harbored the ACME gene (22). We noted that SSTIs more than doubled during the 5 years of our investigation. The increase in SSTIs has also been observed throughout the United States. For example, a study by CDC showed that the visit rate for SSTIs during 2001-2003 was 410.7 per 10,000 persons (23). Although an overall increase in SSTIs was not seen, SSTIs in the ECS increased by 59% and for hospital outpatient department visits increased by 31%. These increases could be associated with the emergence of CA-MRSA infections and are consistent with our study findings, which showed that this increase was due to the USA300 clone and also with an overall increase in SSTIs. The potential limitations of this study include the study population and its retrospective nature. Because the study population consisted of veterans who received treatment through the VA Maryland Healthcare System, and thus were mainly male patients of low socioeconomic status socioeconomic status, n the position of an individual on a socio-economic scale that measures such factors as education, income, type of occupation, place of residence, and in some populations, ethnicity and religion. , the study was not a true population-based study. Although we focused only on the veteran population, we believe that our findings are consistent with those of other scientific studies and are relevant to most emergency department populations. The use of a veteran population is also an advantage. We were able to obtain more comprehensive medical information from the VA's computerized medical record system than would likely be available for a nonveteran population. This study was a retrospective review retrospective review, a posttreatment assessment of services on a case-by-case or aggregate basis after the services have been performed. of information obtained for the clinical treatment of infections, and therefore many SSTIs were not cultured. Although the increased frequency of culturing may have led to some increase in MRSA, the fact that the proportion of SSTIs that were MSSA stayed the same suggests that the increase in MRSA infections is real. In conclusion, we showed an increase in CA-MRSA infections of the USA300 clone and an increase in SSTIs during a 5-year period in the ECS and systemwide at the VAMHCS. The emergence of the USA300 clone has led to not only to an increase in CA-MRSA infections but also an overall increase in SSTIs in our patient population. This finding suggests that this clone is becoming more virulent with a greater propensity to cause SSTIs. Acknowledgments We thank Andrea Feller, Eric Tai, and Deborah Grady for chart abstraction; our ECS physicians for promptly bringing this situation to our attention; Judy Johnson and the staff in the VA Microbiology Laboratory for retrieval of MRSA isolates; Li Tang for genotyping assistance; and our colleagues at CDC for expert consultation. This work was supported by a VA Research and Development Merit Award to M.C.R. and the University of Maryland University of Maryland can refer to:
Dr. Johnson is assistant professor at the University of Maryland School of Medicine, Department of Pathology, and associate director of the clinical microbiology laboratory at the University of Maryland Medical Center. Her main research interest is antibiotic resistance antibiotic resistance, n the ability of certain strains of microorganisms to develop resistance to antibiotics. antibiotic resistance , focusing on MRSA and resistant mobile genetic elements Mobile genetic elements (MGE) are a type of DNA that can move around within the genome. They include:
References (1.) Centers for Disease Control and Prevention. Methicillin-resistant Staphylococcus aureus infections in correctional facilities--Georgia, California, and Texas, 2001-2003. MMWR MMWR Morbidity & Mortality Weekly Report Epidemiology A news bulletin published by the CDC, which provides epidemiologic data–eg, statistics on the incidence of AIDS, rabies, rubella, STDs and other communicable diseases, causes of mortality–eg, Morb Mortal Wkly Rep. 2003;52:992 6. (2.) Centers for Disease Control and Prevention. Methicillin-resistant Staphylococcus aureus infections among competitive sports participants--Colorado, Indiana, Pennsylvania, and Los Angeles County, 2000-2003. MMWR Morb Mortal Wkly Rep. 2003;52:793-5. (3.) Centers for Disease Control and Prevention. Outbreaks of community-associated methicillin-resistant Staphylococcus aureus skin infections--Los Angeles County, California, 2002-2003. MMWR Morb Mortal Wkly Rep. 2003;52:88. (4.) Chambers HF. The changing epidemiology of Staphylococcus aureus Staphylococcus au·re·us n. A bacterium that causes furunculosis, pyemia, osteomyelitis, suppuration of wounds, and food poisoning. Staphylococcus aureus Staphylococcus pyogenes ? Emerg Infect Dis. 2001 ;7:178-82. (5.) Graham PL, Lin SX, Larson EL. A U.S. population-based survey of Staphylococcus aureus colonization. Ann Intern Med. 2006;144:318-25. (6.) Naimi TS, LeDell KH, Como-Sabetti K, Borchardt SM, Boxrud DJ, Etienne J, et al. Comparison of community- and health care-associated methicillin-resistant Staphylococcus aureus infection. JAMA JAMA abbr. Journal of the American Medical Association . 2003;290:2976-84. (7.) McDougal LK, Steward CD, Killgore GE, Chaitram JM, McAllister SK, Tenover FC. Pulsed-field gel electrophoresis typing of oxacillinresistant Staphylococcus aureus isolates from the United States: establishing a national database. J Clin Microbiol. 2003;41:5113 20. (8.) King MD, Humphrey B J, Wang YF, Kourbatova EV, Ray SM, Blumberg HM. Emergence of community-acquired methicillin-resistant Staphylococcus aureus USA 300 clone as the predominant cause of skin and soft-tissue infections. Ann Intern Med. 2006; 144:309-17. (9.) Carleton HA, Diep BA, Charlebois ED, Sensabaugh GF, Perdreau-Remington F. Community-adapted methicillin-resistant Staphylococcus aureus (MRSA): population dynamics of an expanding community reservoir of MRSA. J Infect Dis. 2004; 190:1730-8. (10.) Diep BA, Gill SR, Chang RF, Phan TH, Chen JH, Davidson MG, et al. Complete genome sequence of USA300, an epidemic clone of community-acquired methicillin-resistant Staphylococcus aureus. Lancet. 2006;367:731-9. (11.) Said-Salim B, Mathema B, Braughton K, Davis S, Sinsimer D, Eisner W, et al. Differential distribution and expression of Panton-Valentine leucocidin among community-acquired methicillin-resistant Staphylococcus staphylococcus (stăf'ələkŏk`əs), any of the pathogenic bacteria, parasitic to humans, that belong to the genus Staphylococcus. The spherical bacterial cells (cocci) typically occur in irregular clusters [Gr. areus strains. J Clin Microbiol. 2005;43:3373-9. (12.) Fridkin SK, Hageman JC, Morrison M, Sanza LT, Como-Sabetti K, Jernigan JA, et al. Methicillin-resistant Staphylococcus aureus disease in three communities. N Engl J Med. 2005;352:143644. (13.) Clinical and Laboratory Standards Institute (CLSI CLSI Clinical and Laboratory Standards Institute (Wayne, PA) CLSI Cisco Link Services Interface ). Methods for dilution antimicrobial susceptibility test for bacteria that grow areobically; approved standard. 7th ed. CLSI document M7-A7. Wayne (PA): The Institute; 2006. (14.) Harmsen D, Claus H, Witte W, Rothganger J, Claus H, Turnwald D, et al. Typing of methicillin-resistant Staphylococcus aureus in a university hospital setting by using novel software for spa repeat determination and database management. J Clin Microbiol. 2003:41:5442-8. (15.) Lina G, Piemont Y, Godail-Gamot F, Bes M, Peter MO, Gauduchon V, et al. Involvement of Panton-Valentine leukocidin-producing Staphylococcus attreus in primary skin infections and pneumonia. Clin Infect Dis. 1999;29:1128-32. (16.) Tenover FC, Arbeit RD, Goering RV, Mickelsen PA, Murray BE, Persing DH, et al. Interpreting chromosomal DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. rcstriction patterns produced by pulsed-field gel elcctrophoresis: criteria for bacterial strain typing. J Clin Microbiol. 1995;33:2233-9. (17.) Moran G J, Amii RN, Abrahamian FM, Talan DA. Methicillin-resistant Staphylococcus aureus in community-acquired skin infections. Emerg Infect Dis. 2005;11:928 30. (18.) Moran GJ, Krishnadasan A, Gorwitz RJ, Fosheim GE, McDougal LK, Carey RB, et al. Methicillin-resistant S. aureus infections among patients in the emergency department. N Engl J Med. 2006;355:666-74. (19.) Tenover FC, McDougal LK, Goering RV, Killgore G, Projan S J, Patel JB, et al. Characterization of a strain of community-associated methicillin-resistant Staphylococclts aureus widely disseminated in the United States. J Clin Microbiol. 2006;44:108 18. (20.) Kaplan SL, Hulten KG, Gonzalez BE, Hammerman WA, Lamberth L, Versalovic J, et al. Three-year surveillance of community-acquired Staphylococcus aureus infections in children. Clin Infect Dis. 2005;40:1785-91. (21.) Crum NF, Lee RU, Thornton SA, Stine OC, Wallace MR, Barrozo C, et al. Fifteen-year study of the changing epidemiology of methicillin-resistant Staphylococcus aureus. Am J Med. 2006; 119:943-51. (22.) McDougal LK. Not all USA300 MRSA isolates contain the arginine catabolic mobile element (ACME). C2-603. San Francisco: Interscience Conference on Antimicrobial Agents and Chemotherapy Antimicrobial Agents and Chemotherapy (print-ISSN 0066-4804, CODEN AMACCQ; canceled ISSN 0074-9923, canceled CODEN AACHAX) is an academic journal published by the American Society for Microbiology. ; 2006. (23.) McCaig LF, McDonald LC, Mandal S, Jernigan DB. Staphylococcus aureus-associated skin and soft tissue infections in ambulatory care. Emerg Infect Dis. 2006;12:1715-23. Address for correspondence: Jennifer K. Johnson, Department of Pathology, University of Maryland School of Medicine, 22 South Greene St, Rm N2W N2W Not to Worry 69, Baltimore, MD 21201, USA: email: jkjohnson@som (1) (System Object Model) An object architecture from IBM that provides a full implementation of the CORBA standard. SOM is language independent and is supported by a variety of large compiler and application development vendors. . umaryland.edu Jennifer K. Johnson, * Tina Khoie, * Simone Shurland, * Kristen Kreisel, * O. Colin Stine, * Mary-Claire Roghmann * ([dagger]) * University of Maryland School of Medicine, Baltimore, Maryland, USA; and ([dagger]) Veterans Affairs Maryland Health Care System, Baltimore, Maryland, USA
Table 1. Molecular typing of isolates from patients with new MRSA
infections, Baltimore Veterans Affairs Medical Center Emergency
Care Service, 2001-2005 *
No. spa typing
Time isolates MBQBLO MDMGMK Other spa
period tested motif, motif, types,
[dagger] [double [section]
no. (%) dagger] no. (%)
no. (%)
FY01 2 0 2 (100) 0
FY02 13 4 (31) 5 (38) 4 (31)
FY03 21 15 (71) 6 (29) 0
FY04 94 77 (82) 14 (15) 3 (3)
FY05 166 147 (89) 15 (9) 4 (2)
Total 296 243 (82) 42 (14) 11 (4)
Time MBQBLO
period motif, PVL,
PVL, ACME, and ACME,
no. (%) no. (%) no. (%)
FY01 0 0 0
FY02 3 (23) 3 (23) 2 (27)
FY03 15 (71) 15 (71) 15 (71)
FY04 74 (80) 70 (75) 68 (74)
FY05 154 (93) 147 (89) 138 (84)
Total 246 (83) 235 (79) 223(76)
* MRSA, methicillin-resistant Staphylococcus aureus; PVL,
Panton-Valentine leukocidin; ACME, arginine catabolic mobile element;
FY, fiscal year.
[dagger] spa types t008, t024, tl12, t622, t064, t068, t121, t1881.
[double dagger] spa types t002, t045, t242, t548, t539.
[section] spa types t018, t019, t084, t128, t160, t216, 1937, 11887.
Table 2. Microbiologic characteristics of samples taken from
patients with SSTIs, Baltimore Veterans Affairs Medical Center
Emergency Care Service, 2001-2005 *
Year Had SSTI, SSTI was SSTI was SSTI was
no. cultured, cultured cultured
no. (%) and grew and grew
MRSA, MSSA, no.
no. (%) (%)
FY01 496 98 4 10
FY02 574 120 10 12
FY03 567 99 11 7
FY04 981 292 96 37
FY05 1,070 410 172 52(13)
* SSTIs, skin and soft tissue infections, MRSA, methicillin-resistant
Staphylococcus aureus; MSSA, methicillin-susceptible S. aureus.
|
|
||||||||||||||||||
Printer friendly
Cite/link
Email
Feedback
Reader Opinion