Community-associated methicillin-resistant Staphylococcus aureus isolates causing healthcare-associated infections (1).We noted a marked increase in healthcare-associated (HA) 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. ) infections caused by isolates phenotypically consistent with community-associated (CA)-MRSA strains. To study this trend, we retrospectively examined all HA-MRSA isolates from patients in our institution during 1999-2004. An isolate was considered an SCCmecIV phenotype if it had antimicrobial antimicrobial /an·ti·mi·cro·bi·al/ (-mi-kro´be-al) 1. killing microorganisms or suppressing their multiplication or growth. 2. an agent with such effects. drug susceptibilities consistent with typical CA-MRSA CA-MRSA Community Acquired Methicillin-Resistant Staphylococcus Aureus isolates. Our phenotypic definition was validated in a limited subset of isolates by SCCmec genotype genotype (jēn`ətīp'): see genetics. genotype Genetic makeup of an organism. The genotype determines the hereditary potentials and limitations of an individual. , pulsed-field gel electrophoresis gel electrophoresis n. Electrophoresis performed in a gel composed of agarose, polyacrylamide, or starch. , and multilocus sequence typing Multilocus sequence typing (MLST) is a technique in molecular biology for the typing of multiple loci. The procedure characterizes isolates of bacterial species using the DNA sequences of internal fragments of multiple (usually seven) housekeeping genes. . Among 352 patients with HA-MRSA isolates, SCCmecIV phenotype increased from 17% in 1999 to 56% in 2003 (p<0.0001). Antimicrobial drug-susceptibility phenotype and genotype were consistent in 21 (91%) of 23 isolates. In a multivariate model, the SCCmec type IV phenotype was independently associated with wound culture source, later year of collection, and MRSA isolated earlier during hospitalization. In conclusion, MRSA isolates phenotypically similar to CA strains have become the predominant isolates associated with HA-MRSA in our hospital. ********** Methicillin-resistant Staphylococcus aureus (MRSA) is the most frequently identified antimicrobial drug-resistant pathogen in US hospitals (1). The epidemiology of infections caused by MRSA is rapidly changing. In the past 10 years, infections caused by this organism have emerged in the community. The 2 MRSA clones in the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. most closely associated with community outbreaks, USA400 (MW2 strain, ST1 lineage) and USA300, often contain pvl genes and, more frequently, have been associated with skin and soft tissue infections (2,3). Outbreaks of community-associated (CA)-MRSA infections have been reported in correctional facilities, among athletic teams, among military recruits, in newborn nurseries, and among men who have sex with men Men who have sex with men (MSM) is a term used mostly in the United States to classify men who engage in sex with other men, regardless of whether they self-identify as gay, bisexual, or heterosexual. (4-7). CA-MRSA infections now appear to be endemic in many urban regions and cause most CA-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. infections (5,6,8-10). CA-MRSA isolates were first recognized by distinct resistance profiles of antimicrobial drugs that lacked resistance to older antimicrobial drugs (11-13). Several groups have noted these distinct susceptibility patterns appearing in isolates from hospitalized patients. Denis Denis, king of Portugal: see Diniz. et al. noted that since 1995, MRSA isolates in Belgian hospitals were losing resistance to older antimicrobial drugs such as gentamicin gentamicin /gen·ta·mi·cin/ (jen?tah-mi´sin) an aminoglycoside antibiotic complex isolated from bacteria of the genus Micromonospora, and clindamycin (14). A Spanish hospital experienced a decrease in gentamicin-resistant MRSA isolates (from 97% in 1998 to 20% in 2002) and a simultaneous increase in MRSA isolates carrying the SCCmec type IV cassette (from 0% prevalence in 2000 to 23% prevalence in 2002) (15). A French group noted a similar finding in their hospitals over an 11-year period and found a correlation between isolates that contained SCCmec type IV and susceptibility profiles to [greater than or equal to] 3 antimicrobial drugs (16). However, these investigations did not distinguish between cultures obtained from patients hospitalized with CA infection and those with hospital-associated (HA) infections. Thus, it is unclear whether these trends in decreased antimicrobial drug resistance and increased number of MRSA isolates that contained SCCmec type IV were due to increased hospitalization of patients with CA-MRSA infections or to an increased prevalence of isolates containing SCCmec type IV among HA-MRSA isolates. Some MRSA strains associated with CA infection have been noted to cause HA infections. Outbreaks of HA infections caused by isolates containing SCCmec type IV have been reported from Australia and the United States. Affected populations have included postpartum postpartum /post·par·tum/ (post-pahr´tum) occurring after childbirth, with reference to the mother. post·par·tum adj. Of or occurring in the period shortly after childbirth. women and patients undergoing prosthetic pros·thet·ic adj. 1. Serving as or relating to a prosthesis. 2. Of or relating to prosthetics. prosthetic serving as a substitute; pertaining to prostheses or to prosthetics. joint replacement (17-19). Another recent report demonstrated that CA strains had emerged as a substantial cause of HA bloodstream infections (20). However, these reports are anecdotal, and data examining temporal trends are lacking. At our institution, which is located in an area in which CA-MRSA infections are endemic, we have noted a large increase in HA infections caused by MRSA isolates that, by assessment of antibiotic susceptibility patterns, appear to carry the SCCmec type IV element (e.g., susceptible to gentamicin, clindamycin, and trimethoprim-sulfamethoxazole) (6,10,21). The aim of this study was to quantify this trend over a 6-year period. Methods Population To find patients with HA-MRSA infections, we identified all cultures obtained [greater than or equal to] 72 hours after hospitalization that grew MRSA, from January 1, 1999, through December 31, 2004, at Harbor-UCLA Medical Center Harbor-UCLA Medical Center is a hospital located within the city of Torrance, California, USA. The hospital was founded in 1946, and is funded by Los Angeles County Harbor-UCLA serves as the Level I Trauma Center for the South Bay area. , a tertiary-care, urban, county hospital in Los Angeles Los Angeles (lôs ăn`jələs, lŏs, ăn`jəlēz'), city (1990 pop. 3,485,398), seat of Los Angeles co., S Calif.; inc. 1850. County. At this hospital, surveillance cultures for MRSA colonization are not routinely performed; therefore, cultures positive for MRSA are likely to reflect infection rather than colonization. For a given patient, we examined only data from the first positive culture and excluded patients who had positive cultures both [greater than or equal to] 72 hours and <72 hours after admission. If a patient had been hospitalized more than once during the study period, only data from the first hospitalization were retained. A standardized instrument was used to abstract data from the medical record of each patient. Information obtained included demographics, admission date and time, hospital location, antimicrobial drug susceptibility of the MRSA isolate, and time, date, and source of the MRSA culture. We obtained only MRSA blood isolates for molecular typing because the clinical microbiology Clinical microbiology The adaptation of microbiological techniques to the study of the etiological agents of infectious disease. Clinical microbiologists determine the nature of infectious disease and test the ability of various antibiotics to inhibit or kill laboratory discards all other types of isolates after identification is complete. In vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. susceptibilities were reported as minimal inhibitory concentrations and performed with the VITEK system (bioMerieux, Durham, NC, USA), according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. the protocols of the Clinical and Laboratory Standards Institute (CLSI CLSI Clinical and Laboratory Standards Institute (Wayne, PA) CLSI Cisco Link Services Interface ). The investigation protocol was reviewed and approved by the Institutional Review Board of Harbor-UCLA Medical Center. Molecular Characterization of Strains Molecular typing was performed at the University of Chicago by investigators who were blinded to the clinical details and antibiograms of the isolates. SCCmec Typing PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) was performed to detect mecA by using the primer pair mecAF/mecAR (22). SCCmec elements were distinguished by the molecular architecture of the ccr and mecA complexes (21,23,24). PCR typing of SCCmec types I-IV was performed under the conditions previously described (24,25). SCCmec type II (ccrAB complex type 2 and mec complex class A), SCCmec type III Type III may stand for:
al·lo·type n. 4 (ccr complex 4) was assessed in a separate reaction that used the primer pair ccrA4F and ccrB4R (27). Screening for the ccrC gene (ccr complex 5) was performed with a forward primer ([gamma]F) in combination with the reverse primer [gamma]R described by Ito et al. (28). Prototype strains used for SCCmec typing were 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) 10442 (SCCmec I), N315 (SCCmec II), 85/2082 (SCCmec III), MW2 (SCCmec IV), and WIS (SCCmec V). The control strain used for detection of ccrAB4 was S. epidermidis strain ATCC ATCC American Type Culture Collection, see there 12228, which contains ccrAB4 in the non-mec-containing SCCcomposite island (24). MLST MLST Multi Locus Sequence Typing MLST Medical Logistics Support Team MLST Mini Losi Super Truck (1/18th scale radio control vehicle) MLST was performed by PCR amplification and sequencing of 7 housekeeping genes by using the primer pairs designed by Enright et al (29). Denville Taq-Pro Complete (Denville Scientific, Metuchen, NJ, USA) or the Taq DNA Polymerase DNA polymerase /DNA po·lym·er·ase/ (pah-lim´er-as) any of various enzymes catalyzing the template-directed incorporation of deoxyribonucleotides into a DNA chain, particularly one using a DNA template. (Promega, Madison, WI, USA) was used for the PCR reactions. PCR products were evaluated on an agarose agarose more highly purified form of agar with similar uses to agar and widely used in the separation of nucleic acid fragments. gel and purified by using Millipore 96-well Montage montage (mŏntäzh`, Fr. môNtäzh`), the art and technique of motion-picture editing in which contrasting shots or sequences are used to effect emotional or intellectual responses. (Billerica, MA, USA) plates according to manufacturer's instructions. The purified templates were sequenced at the University of Chicago Core Sequencing Facility and evaluated with the use of Vector NTI NTI NewTech Infosystems (software company, Irvine, California) NTI Nuclear Threat Initiative NTI National Transit Institute (New Brunswick, New Jersey) NTI Nunavut Tunngavik Incorporated software (Invitrogen, Carlsbad, CA, USA). Each sequence was submitted to the MLST database website (www.mlst.net) for assignment of the allelic al·lele n. One member of a pair or series of genes that occupy a specific position on a specific chromosome. [German Allel, short for Allelomorph, allelomorph, from English profile and sequence type (ST). Screening for pvl Genes Isolates were screened for the lukF-PV and lukS-PV genes encoding the components of the PVL toxin by PCR amplification of a 433-bp product that includes a portion of both the lukS-PV and lukF-PV ORFs by using the primer pair luk-PV-1/ luk-PV-2 (final concentration 0.2 [micro]M) designed by Lina et al. (30). The thermocycler conditions have been described (27). Case Definition and Data Analysis A standardized definition of CA-MRSA infection was created 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 ) Active Bacterial Core Surveillance sites (31). Using this definition, we defined HA-MRSA infections as those MRSA infections that did not meet the definition of CA-MRSA infections. Specifically, we defined an MRSA isolate as HA associated if the original entry criteria of hospitalization for [greater than or equal to] 72 hours before culture acquisition was met and if in the year before the present hospitalization, the patient had had any 1 of the following: hospitalization, surgery, residency in a long-term care facility long-term care facility n. See skilled nursing facility. , and hemodialysis or peritoneal dialysis peritoneal dialysis n. The removal of soluble substances and water from the body by transfer across the peritoneum, utilizing a solution which is intermittently introduced into and removed from the peritoneal cavity. , or at the present admission had 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. percutaneous devices or catheters. A CA infection was defined as a culture-confirmed MRSA infection without any of the above criteria. However, if the patient did not meet any of the above criteria, had an infection at the time of admission, and the culture of the infection on admission was taken [greater than or equal to] 72 hours after admission, then the infection was considered CA. An example of this situation would be a deep tissue infection microbiologically diagnosed from a surgical biopsy specimen 4 days after the patient's admission. To validate our definition of HA-associated infection, we reviewed 105 (30%) randomly selected charts of the patients with MRSA infections identified [greater than or equal to] 72 hours after hospitalization. The purpose of this validation was to confirm that these cultures did not reflect CA infections that were diagnosed late (>72 hours) in the hospital course. Of note, in the CDC definition, an infection is considered HA if it occurs >48 hours after admission. Yet, we chose [greater than or equal to] 72 hours as a cut-off cut-off Anesthesiology The point at which elongation of the carbon chain of the 1-alkanol family of anesthetics results in a precipitous drop in the anesthetic potential of these agents–eg, at > 12 carbons in length, there is little anesthetic activity, to more conservatively capture HA infections, i.e., to minimize the miscategorization of CA infections as HA infections. We then defined MRSA strains as having the SCCmec type IV phenotype if the isolates were resistant to 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. and susceptible to gentamicin, clindamycin, and trimethoprim-sulfamethoxazole. All other isolates were considered to be phenotypically non-SCCmec type IV. Characteristics were compared between patients infected with the non-SCCmec type IV phenotype isolates and those infected with SCCmec type IV phenotype isolates by using a [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. ] or t test, as appropriate. No adjustments were made for multiple comparisons. Temporal trends in the proportion of the SCCmec type IV phenotype were compared with the Cochran-Armitage test of trends. A multivariate analysis multivariate analysis, n a statistical approach used to evaluate multiple variables. multivariate analysis, n a set of techniques used when variation in several variables has to be studied simultaneously. that predicted phenotypically SCCmec type IV isolates was performed by using an unconditional logistic regression In statistics, logistic regression is a regression model for binomially distributed response/dependent variables. It is useful for modeling the probability of an event occurring as a function of other factors. model and a backward model selection method. A p value of [less than or equal to] 0.05 was defined as statistically significant. Data analysis was done with SAS (1) (SAS Institute Inc., Cary, NC, www.sas.com) A software company that specializes in data warehousing and decision support software based on the SAS System. Founded in 1976, SAS is one of the world's largest privately held software companies. See SAS System. software version 8.2 (SAS Institute SAS Institute Inc., headquartered in Cary, North Carolina, USA, has been a major producer of software since it was founded in 1976 by Anthony Barr, James Goodnight, John Sall and Jane Helwig. Inc., Cary, NC, USA). Results Population Characteristics We identified 352 patients who had HA-MRSA cultures; 229 (65%) were men, and the median age was 50 years (mean 49.5 years). In the subset of medical records reviewed for validation of HA or CA status, none of the patients' infections (0/105) fit our definition of a CA infection. The SCCmec type IV phenotype was identified in 128 (36%) of these 352 patients. Compared with the non-SCCmec type IV phenotype, patients with the SCCmec type IV phenotype were younger (median age 48 vs. 54 years, p = 0.02) and had the defining culture taken earlier in the hospitalization (median 8 vs. 15 days, p = 0.01). Finding an isolate with the SCCmec type IV phenotype was more likely if the culture source was from a wound, blood, or source other than sputum sputum /spu·tum/ (spu´tum) [L.] expectoration; matter ejected from the trachea, bronchi, and lungs through the mouth. sputum cruen´tum bloody sputum. (odds ratio [OR] 2.9, 95% confidence interval confidence interval, n a statistical device used to determine the range within which an acceptable datum would fall. Confidence intervals are usually expressed in percentages, typically 95% or 99%. [CI] 1.7-5.0, p<0.0001; OR 2.6, 95% CI 1.2-5.7, p = 0.02; and OR 1.2, 95% CI 0.6-2.3, p = 0.69) (Table 1). Validation of the SCCmec Phenotype Definition Of the 352 cultures, 35 were recovered from blood and were potentially available for genetic analysis. We were able to subculture subculture /sub·cul·ture/ (sub´kul-chur) a culture of bacteria derived from another culture. sub·cul·ture n. 24 of the blood isolates. We could not perform SCCmec typing on 1 of the 24 growing isolates. The 23 remaining isolates were representative of each year of the 6-year period except 1999, when no isolates could be recovered. Twelve isolates carried the SCCmec type IV element, and 9 also carried the pvl genes (Table 2). Eleven isolates carried the SCCmee type II element; none carried pvl. The clinical definition of the SCCmec IV phenotype was fulfilled by 11 (92%) of the 12 isolates that carried the SCCmec IV element. The exception was an isolate that contained SCCmec IV that was resistant to gentamicin, clindamycin, and trimethoprim-sulfamethoxozole. The definition of the non-SCCmec IV phenotype was fulfilled by 10 (91%) of 11 isolates carrying the SCCmec II element. Phenotypic case definition of SCCmec type was highly correlated with the genotype confirmation of the SCCmec type phenotype (p<0.0001 by Fisher exact test). Trend and Multivariate Analysis of the SCCmec type IV Phenotype The proportion of MRSA isolates with the SCCmec type IV phenotype increased from 17% in 1999 to 56% in 2003 (p<0.0001, Figure). The proportion of isolates that were of the SCCmec type IV phenotype in 2004 (52%) was little changed from 2003 (Figure). In the multivariate model, independent predictors for having an SCCmec type IV phenotype isolate were wound source of culture (referent group was sputum source, OR 2.6, 95% CI 1.5-4.6, p = 0.001), culture obtained in less time after admission, (OR 0.88 per week, 95% CI 0.8-0.98, p = 0.02), and year of culture acquisition (p<0.0001) (Table 1). [FIGURE OMITTED] Discussion In many urban centers worldwide, infections due to MRSA account for a large proportion of CA-S. aureus infections; in some communities MRSA accounts for more than half of CA-S. aureus infections (6,8-10,32). There have been reports of strains frequently associated with community outbreaks causing HA infections, but they have been mostly limited to case reports or case series (17-19). To our knowledge, ours is the first investigation quantifying the rise of MRSA isolates typical of CA disease to become the predominant strain of HA-MRSA (i.e., accounting for >50% of MRSA strains) within the hospital setting. Remarkably, at our institution the number of HA-MRSA isolates that have a CA phenotype, which previously was uncommon, now is >50%. Our analysis found 3 significant risk factors for an SCCmec type IV phenotype MRSA culture. First, patients with MRSA cultures from a wound source were more likely to have the SCCmec type IV phenotype. This finding may be understandable, given that the most common clinical syndrome described with CA-MRSA infections has been skin and soft tissue infections (10,33). In addition, 75% of CA-MRSA isolates that were genotyped carried the pvl gene, which has a strong association with skin and soft tissue infections (33). A second risk factor for the SCCmec type IV phenotype was a shorter length of hospital stay before MRSA culture. This association may be due to the increased severity of illness and coexisting conditions in patients with a longer hospital stay, factors that have been commonly associated with the traditional (non-SCCmec type IV) HA-MRSA infections. However, measures of severity of illness and coexisting conditions were not captured in this investigation. A third risk factor was a later year of culture collection; the likelihood of SCCmec type IV phenotype peaked in 2003. The rise of these isolates in our hospital may be from CA-MRSA isolates brought in from colonized Colonized This occurs when a microorganism is found on or in a person without causing a disease. Mentioned in: Isolation persons from the community. CA-MRSA infections in Los Angeles County have rapidly become common and now exceed the frequency of those caused by CA-methicillin-susceptible S. aureus (34). Alternatively, the rise of SCCmec type IV isolates may be a result of spread throughout our hospital by the usual means of dissemination in a healthcare setting (e.g., hands of healthcare workers, contaminated contaminated, v 1. made radioactive by the addition of small quantities of radioactive material. 2. made contaminated by adding infective or radiographic materials. 3. an infective surface or object. environment) (35) or possibly by a combination of factors. Exactly why the SCCmec type IV strains are successful in hospital settings such as ours and others (20) is unknown. Some evidence indicates that SCCmec type IV strains may be more "fit" than SCCmec types II/III that contain HA-MRSA isolates. Compared with methicillin-susceptible S. aureus, isolates containing SCCmec type II/III replicate more slowly in vitro (36). Okuma et al. found that CA-MRSA isolates that contain SCCmec type IV replicate more rapidly than these traditional HA-MRSA strains and argued that CA-MRSA may have enhanced ecologic fitness compared with SCCmec type II/III isolates, perhaps due simply to a shorter doubling time doubling time Oncology A parameter used to determine tumor aggressiveness, which serves to prognosticate, measure therapeutic success, and quantify tumor kinetics and growth rate. Cf Gompertzian growth curve. (37). Given the vulnerable population within the hospital setting, it is unclear how infections with isolates that contain SCCmec type IV will differ in symptoms and severity from those caused by traditional HA-MRSA isolates. On the basis of our study and other somewhat similar reports (20), concern is rising that USA300 strains may overtake the traditional HA-MRSA strains in many hospital and healthcare settings. Our investigation had some limitations. First, the analysis was retrospective and thus it was not possible to prospectively identify patients with HA infections and compare them with patients with CA infections. Although, by means of a chart review of a subset of patients who were selected by the criteria of a MRSA culture obtained [greater than or equal to] 72 hrs after admission, none of these infections fulfilled the CDC definition of a CA-MRSA infection (31). A second limitation was that our case definition was based on phenotypic criteria because nonbloodstream isolates had been discarded and the SCCmec type could not be validated. Traditionally, most HA-MRSA isolates in the United States carry SCCmec type II (and to a lesser extent, SCCmec type III) that encodes resistance to [beta]-lactam antimicrobial agents Antimicrobial agents Chemical compounds biosynthetically or synthetically produced which either destroy or usefully suppress the growth or metabolism of a variety of microscopic or submicroscopic forms of life. bleomycin bleomycin /ble·o·my·cin/ (ble-o-mi´sin) a polypeptide antibiotic mixture obtained from cultures of Streptomyces verticellus; used as the sulfate salt as an antineoplastic. ble·o·my·cin n. , macrolide-lincosamide-streptogamin B, aminoglycosides, and spectinomycin spectinomycin /spec·ti·no·my·cin/ (spek?ti-no-mi´sin) an antibiotic derived from Streptomyces spectabilis, used as the hydrochloride salt in the treatment of gonorrhea. (38). Gentamicin resistance occurs in most strains that carry the SCCmec type II element but is conferred by the aac6'-aph2" gene elsewhere on the chromosome and is frequently carried by transposon transposon /trans·po·son/ (trans-po´zon) a small mobile genetic (DNA) element that moves around the genome or to other genomes within the same cell, usually by copying itself to a second site but sometimes by splicing itself out of its Tn4001 (11,16). Therefore, to select for isolates that did not confer a phenotype typical of healthcare-associated or non-SCCmec type IV-containing isolates, the SCCmec type IV phenotype was defined as isolates that were resistant to oxacillin and susceptible to gentamicin, clindamycin, and trimethoprim-sulfamethoxazole. Some banked isolates did not grow, and in 1 isolate we could not detect an SCCmec element. Of note, stored isolates may lose their SCCmec elements over time (39), which may explain our findings. Nevertheless, over the 6-year observation period of our investigation, among isolates, the phenotype and genotype definition of SCCmec type were in agreement for >90% of isolates. Thus, we were able to validate our case definition of an HA-MRSA isolate with SCCmec type IV phenotype using both chart review and SCCmec typing. A third limitation of our investigation was that we were able to recover only bloodstream isolates, a subset of strains that are small and potentially nonrepresentattive. Whether the relationship of phenotype to genotype is similar for bloodstream and nonbloodstream infections is unclear. A fourth limitation is that all of the patients were from 1 institution and, therefore, may only reflect local trends. However, as previously mentioned, reports of isolates associated with the CA-MRSA infections causing HA infections are growing (17-20). In summary, we found that over a 5-year span, MRSA with a CA-MRSA phenotype has become the most common cause of HA-MRSA infections in our institution. This finding has important implications for MRSA epidemiology, infection control practices, and empiric antimicrobial drug selection. Acknowledgments We are indebted to Danny Kim and Jie Peng for performing SCCmec typing, MLST typing, and PCR to detect the Panton-Valentine leukocidin Panton-Valentine leukocidin a nonhemolytic toxin produced by Staphylococcus aureus which kills segmented neutrophils and macrophages. genes. We thank Roger Detels for his continued support and guidance. In addition, we acknowledge Kevin Bui, Gunter Rieg, and Grace Tagudar for their important contributions to this investigation. C.L.M. reports having received grant support from Pfizer Pharmaceuticals. L.G.M. reports having received lecture and consulting fees from Pfizer Pharmaceuticals. C.L.M.'s effort was supported by a grant from the National Institute of Allergy and Infectious Diseases infectious diseases: see communicable diseases. (T32 AI07481-09). R.S.D.'s and S.B.V's efforts were supported by a grant from NIAID NIAID National Institute of Allergy and Infectious Diseases. (AI40481-01A1), the Centers for Disease Control and Prevention (RO1 CCR523379), and the Grant Health Care Foundation. L.G.M.'s effort was supported by grants from CDC(RO1/CCR923419) and the National Institutes of Health (K23AI0183). References (1.) Centers for Disease Control and Prevention. National Nosocomial Infections Nosocomial infections Infections that were not present before the patient came to a hospital, but were acquired by a patient while in the hospital. Mentioned in: Enterobacterial Infections, Staphylococcal Infections Surveillance System (NNIS NNIS National Nosocomial Infection Surveillance System ) report, data summary from January 1992 through June 2003, issued August 2003. Am J Infect Control. 2003;31:481-98. (2.) Deresinski S. Methicillin-resistant Staphylococcus aureus: an evolutionary, epidemiologic, and therapeutic odyssey. Clin Infect Dis. 2005;40:562-73. (3.) Chambers HF. Community-associated MRSA--resistance and virulence converge. N Engl J Med. 2005;352:1485-7. (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.) Outbreaks of community-associated methicillin-resistant Staphylococcus aureus skin infections--Los Angeles County, California, 2002-2003. 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;52:88. (6.) Bancroft E, Kilgore G, Jones A, Yasuda L, Lee NE, Ruane P, et al. Four outbreaks of community-associated methicillin-resistant Staphylococcus aureus in Los Angeles County. Presented at the 41st Annual Meeting of the Infectious Diseases Society of America The Infectious Diseases Society of America (IDSA) is a medical association representing physicians, scientists and other health care professionals who specialize in infectious diseases. ; 2003 Oct 9-13; San Diego, California “San Diego” redirects here. For other uses, see San Diego (disambiguation). San Diego is a coastal Southern California city located in the southwestern corner of the continental United States. As of 2006, the city has a population of 1,256,951. . Alexandria (VA): Infectious Diseases Society of America; 2003. (7.) Ellis MW, Hospenthal DR, Dooley DP, Gray PJ, Murray CK. Natural history of community-acquired methicillin-resistant Staphylococcus aureus colonization and infection in soldiers. Clin Infect Dis. 2004;39:971-9. (8.) Eady EA, Cove JH. 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. resistance revisited: community-acquired methicillin methicillin /meth·i·cil·lin/ (meth?i-sil´in) a semisynthetic penicillin highly resistant to inactivation by penicillinase; used as the sodium salt. meth·i·cil·lin n. 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. aureus--an emerging problem for the management of skin and soft tissue infections. Curr Opin Infect Dis. 2003; 16:103-24. (9.) 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. (10.) Moran GJ, Amii RN, Abrahamian FM, Talan DA. Methicillin-resistant Staphylococcus aureus in community-acquired skin infections. Emerg Infect Dis. 2005; 11:928-30. (11.) Lelievre H, Lina G, Jones ME, Olive C, Forey F, Koussel-Delvallez M, et al. Emergence and spread in French hospitals of methicillin-resistant Staphylococcus aureus with increasing susceptibility to gentamicin and other antibiotics. J Clin Microbiol. 1999;37:3452-7. (12.) Seal JB, Moreira B, Bethel Bethel, in the Bible Bethel (bĕth`əl) [Heb.,=house of God]. 1 Ancient city of central Palestine, the modern Baytin, the West Bank, N of Jerusalem. CD, Daum RS. Antimicrobial resistance in Staphylococcus aureus at the University of Chicago Hospitals The University of Chicago Hospitals form a major center for medical care and research in the Hyde Park neighborhood of Chicago, Illinois. They are affiliated with and run by the University of Chicago, and serve as teaching hospitals for students of the institution's Pritzker : a 15-year longitudinal assessment in a large university-based hospital. Infect Control Hosp Epidemiol. 2003;24:403-8. (13.) Weber JT. Community-associated methicillin-resistant Staphylococcus aureus. Clin Infect Dis. 2005;41(Suppl 4):S269-72. (14.) Denis O, Deplano A, Nonhoff C, De Ryck R, de Mendonca R, Roltiers S, et al. National surveillance of methicillin-resistant Staphylococcus aureus in Belgian hospitals indicates rapid diversification of epidemic clones. Antimicrob Agents Chemother. 2004;48:3625-9. (15.) Perez-Roth E, Lorenzo-Diaz F, Batista N, Moreno A, Mendez-Alvarez S. Tracking methicillin-resistant Staphylococcus aureus clones during a 5-year period (1998 to 2002) in a Spanish hospital. J Clin Microbiol. 2004;42:4649-56. (16.) Donnio PY, Preney L, Gautier-Lerestif AL, Avril JL, Lafforgue N. Changes in staphylococcal cassette chromosome type and antibiotic resistance antibiotic resistance, n the ability of certain strains of microorganisms to develop resistance to antibiotics. antibiotic resistance profile in methicillin-resistant Staphylococcus aureus isolates from a French hospital over an 11 year period. J Antimicrob Chemother. 2004;53:808-13. (17.) Kourbatova EV, Halvosa JS, King MD, Ray SM, White N, Blumberg HM. Emergence of community-associated methicillin-resistant Staphylococcus aureus USA 300 clone as a cause of health care-associated infections among patients with prosthetic joint infections. Am J Infect Control. 2005;33:385-91. (18.) O'Brien FG, Pearman JW, Gracey M, Riley TV, Grubb WB. Community strain of methicillin-resistant Staphylococcus aureus involved in a hospital outbreak. J Clin Microbiol. 1999;37:2858-62. (19.) Saiman L, O'Keefe M, Graham PL Ill, Wu F, Said-Salim B, Kreiswirth B, et al. Hospital transmission of community-acquired methicillin-resistant Staphylococcus aureus among postpartum women. Clin Infect Dis. 2003;37:1313-9. (20.) Seybold U, Kourbatova EV, Johnson JG, Halvosa SJ, Wang YF, King MD,. et al. Emergence of community-associated methicillin-resistant Staphylococcus aureus USA300 genotype as a major cause of health care-associated blood stream infections. Clin Infect Dis. 2006;42:647-56. (21.) Ito T, Katayama Y, Asada K, Mori N, Tsutsumimoto K, Tiensasitom C, et al. Structural comparison of three types of staphylococcal cassette chromosome mec integrated in the chromosome in methicillin-resistant Staphylococcus aureus. Antimicrob Agents Chemother. 2001;45:1323-36. (22.) Herold BC, Immergluck LC, Maranan MC, Lauderdale DS, Gaskin gaskin the muscular portion of the hindleg between the stifle and hock, corresponding to the human calf. The term is used in horses and sometimes dogs. RE, Boyle-Vavra S, et al. Community-acquired methicillin-resistant Staphylococcus aureus in children with no identified predisposing risk. JAMA JAMA abbr. Journal of the American Medical Association . 1998;279:593-8. (23.) Mongkolrattanothai K, Boyle S, Kahana MD, Daum RS. Severe Staphylococcus aurgus infections caused by clonally related community-acquired methicillin-susceptible and methicillin-resistant isolates. Clin Infect Dis. 2003;37:1050-8. (24.) Mongkolrattanothai K, Boyle S, Murphy TV, Daum RS. Novel non-mecA-containing staphylococcal chromosomal cassette composite island containing pbp4 and tagF genes in a commensal commensal /com·men·sal/ (kom-men´sil) 1. living on or within another organism, and deriving benefit without harming or benefiting the host. 2. a parasite that causes no harm to the host. staphylococcal species: a possible reservoir for antibiotic resistance islands in Staphylococcus aureus. Antimicrob Agents Chemother. 2004:48: 1823-36. (25.) Ma XX, Ito T, Tiensasitorn C, Jamklang M, Chongtrakool P, Boyle-Vavra S, et al. Novel type of staphylococcal cassette chromosome mec identified in community-acquired methicillin-resistant Staphylococcus aureus strains. Antimicrob Agents Chemother. 2002;46:1147-52. (26.) Suzuki E, Kuwahara-Arai K, Richardson JF, Hiramatsu K. Distribution of mec regulator genes in methicillin-resistant Staphylococcus clinical strains. Antimicrob Agents Chemother. 1993;37:1219-26. (27.) Boyle-Vavra S, Ereshefsky B, Wang CC, Daum RS. Successful multiresistant community-associated methicillin-resistant Staphylococcus aureus lineage from Taipei, Taiwan, that carries either the novel staphylococcal chromosome cassette mec (SCCmec) type VT or SCCmec type IV. J Clin Microbiol. 2005;43:4719-30. (28.) Ito T, Ma XX, Takeuchi F, Okuma K, Yuzawa H, Hiramatsu K. Novel type V staphylococcal cassette chromosome mec driven by a novel cassette chromosome recombinase re·com·bi·nase n. An enzyme that catalyzes genetic recombination. recombinase a function of the recA protein in Escherichia coli , ccrC. Antimicrob Agents Chemother. 2004;48:2637-51. (29.) Enright MC, Day NP, Davies CE, Peacock SJ, Spratt BG. Multilocus sequence typing for characterization of methicillin-resistant and methicillin-susceptible clones of Staphylococcus aureus. J Clin Microbiol. 2000;38:1008-15. (30.) Lina G, Piemont Y, Godail-Gamot F, Bes M, Peter MO, Gauduchon V, et al. Involvement of Panton-Valentine leukocidin-producing Staphylococcus aureus in primary skin infections and pneumonia. Clin Infect Dis. 1999;29:1128-32. (31.) Minnesota Department of Health. Community-associated methicillin-resistant Staphylococcus aureus in Minnesota. Disease Control Newsletter. 2004;32:61-72. (32.) Centers for Disease Control and Prevention. Four pediatric pediatric /pe·di·at·ric/ (pe?de-at´rik) pertaining to the health of children. pe·di·at·ric adj. Of or relating to pediatrics. deaths from community-acquired methicillin-resistant Staphylococcus aureus--Minnesota and North Dakota North Dakota, state in the N central United States. It is bordered by Minnesota, across the Red River of the North (E), South Dakota (S), Montana (W), and the Canadian provinces of Saskatchewan and Manitoba (N). , 1997-1999. JAMA. 1999;282:1123-5. (33.) Diep BA, Sensabaugh GF, Somboona NS, Carleton HA, Perdreau-Remington F. Widespread skin and soft-tissue infections due to two methicillin-resistant Staphylococcus aureus strains harboring the genes for Panton-Valentine leucocidin. J Clin Microbiol. 2004;42:2080-4. (34.) 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. (35.) Mulligan mul·li·gan n. A golf shot not tallied against the score, granted in informal play after a poor shot especially from the tee. [Probably from the name Mulligan.] Noun 1. ME, Murray-Leisure KA, Ribner BS, Standiford HC, John JF, Korvick JA, et al. Methicillin-resistant Staphylococcus aureus: a consensus review of the microbiology, pathogenesis, and epidemiology with implications for prevention and management. Am J Med. 1993;94:313-28. (36.) Cribier B, Prevost G, Couppie P, Finck-Barbancon V, Grosshans E, Piemont Y. Staphylococcus aureus leukocidin: a new virulence factor Virulence factors are molecules produced by a pathogen that specifically influence their host's function to allow the pathogen to thrive. Factors that are used in general life processes, such as metabolism or bacterial cell structural components, may be vital to the pathogen's in cutaneous cutaneous /cu·ta·ne·ous/ (ku-ta´ne-us) pertaining to the skin. cu·ta·ne·ous adj. Of, relating to, or affecting the skin. Cutaneous Pertaining to the skin. infections? An epidemiological and experimental study. Dermatology. 1992;185:175-80. (37.) Okuma K, Iwakawa K, Turnidge JD, Grubb WB, Bell JM, O'Brien FG, et al. Dissemination of new methicillin-resistant Staphylococcus aureus clones in the community. J Clin Microbiol. 2002;40:4289-94. (38.) Kuroda M, Ohta T, Uchiyama I, Baba T, Yuzawa H, Kobayashi I, et al. Whole genome sequencing of methicillin-resistant Staphylococcus aureus. Lancet. 2001;357:1225-40. (39.) van Griethuysen A, van Loo The French Van Loo family (of Flemish origin) included a number of notable painters:
Address for correspondence: Loren G. Miller, Harbor-UCLA Medical Center, Division of Infectious Disease Infectious disease A pathological condition spread among biological species. Infectious diseases, although varied in their effects, are always associated with viruses, bacteria, fungi, protozoa, multicellular parasites and aberrant proteins known as prions. , 1000 W Carson St, Box 466, Torrance, CA 90509, USA: email: lgmiller@ucla.edu. (1) Findings from this investigation were presented in part at the 45th Annual International 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. , Washington, DC, USA, December 2005. Cynthia L. Maree, * Robert S. Daum, ([dagger]) Susan Boyle-Vavra, ([dagger]) Kelli Matayoshi, ([double dagger double dagger n. A reference mark (  ) used in printing and writing. Also called diesis.Noun 1. ]) (2) and Loren G. Miller * ([double dagger]) * David Geffen School of Medicine at the University of California, Los Angeles UCLA comprises the College of Letters and Science (the primary undergraduate college), seven professional schools, and five professional Health Science schools. Since 2001, UCLA has enrolled over 33,000 total students, and that number is steadily rising. , California, USA; ([dagger]) University of Chicago, Chicago, Illinois, USA; and ([double dagger]) Los Angeles Biomedical bi·o·med·i·cal adj. 1. Of or relating to biomedicine. 2. Of, relating to, or involving biological, medical, and physical sciences. Institute at Harbor-UCLA Medical Center, Torrance, California, USA (2) Current affiliation: University of Southern California The U.S. News & World Report ranked USC 27th among all universities in the United States in its 2008 ranking of "America's Best Colleges", also designating it as one of the "most selective universities" for admitting 8,634 of the almost 34,000 who applied for freshman admission School of Pharmacy, Los Angeles, California Dr Maree is a clinical and research fellow in Infectious Diseases at UCLA Medical Center UCLA Medical Center is a hospital located on the campus of the University of California, Los Angeles in Los Angeles, California. It is rated as one of the top three hospitals in the United States and is the top hospital on the West Coast according to US News & World Report. . She is currently studying community-associated MRSA infections and completing her PhD in epidemiology at the University of California, Los Angeles, School of Public Health.
Table 1. Patients with healthcare-associated MRSA isolates,
1999-2004, and predictors of SCCmec type IV phenotype *
Patients with
HA-MRSA,
Characteristic isolates, % (no.)
Total (352)
Sex
F 35 (123)
M 65 (229)
Age, y
Mean 50 [+ or -] 19 SD
Median (range) 50 (<1-97)
Time from admission to specimen collection, d
Mean 19 [+ or -] 21 SD
Median (range) 12 (4-184)
Culture specimen source
Blood 10 (35)
Sputum 34 (188)
Wound 38 (133)
Other 19 (66)
Year culture specimen collected
1999 52 (15)
2000 57 (16)
2001 65 (19)
2002 47 (13)
2003 63 (18)
2004 68 (19)
SCCmec phenotype, % (no.)
Characteristic Type IV Type II/III
Total 36 (128) 64 (224)
Sex
F 36 (44) 64 (79)
M 37 (84) 63 (145)
Age, y
Mean 47 [+ or -] 1.7 SE 51 [+ or -] 1.3 SE
Median (range) 48 (<1-87) 54 (<1-97)
Time from admission to specimen collection, d
Mean 15 [+ or -] 1.9 SE 21 [+ or -] 1.4 SE
Median (range) 8 (4-174) 15 (4-184)
Culture specimen source
Blood 46 (16) 54 (19)
Sputum 25 (29) 75 (89)
Wound 49 (65) 51 (68)
Other 27 (18) 73 (48)
Year culture specimen collected
1999 17 (9) 83 (43)
2000 19 (11) 81 (46)
2001 28 (18) 72 (47)
2002 43 (20) 57 (27)
2003 56 (35) 44 (28)
2004 52 (35) 48 (33)
Predictors of SCCmec type IV phenotype
Bivariate anaylsis
Odds ratio
Characteristic (95% CI) p value
Total
Sex
F 0.87
M
Age, y
Mean 0.02#
Median (range)
Time from admission to specimen collection, d
Mean 0.01#
Median (range)
Culture specimen source
Blood 2.6 (1.2-5.7) 0.02#
Sputum Reference
Wound 2.9 (1.7-5.0) <0.0001#
Other 1.2 (0.6-2.3) 0.69
Year culture specimen collected
1999 Reference <0.0001
([double dagger])
2000 1.1 (0.4-3.0)
2001 1.8 (0.7-4.5)
2002 3.5 (1.4-8.9]
2003 6.0 (2.4-14.3)
2004 5.1 (2.1-12)
Predictors of SCCmec type IV phenotype
Multivariate analysis
Odds ratio
Characteristic (95% CI) p value
Total
Sex
F >0.05
M
Age, y
Mean >0.05
Median (range)
Time from admission to specimen collection, d
Mean 0.88 (0.8-0.98) 0.02#
([dagger])
Median (range)
Culture specimen source
Blood 2.2 (0.97-5.0) 0.058
Sputum Reference
Wound 2.6 (1.5-4.6) 0.001#
Other 1.1 (0.5-2.2) 0.82
Year culture specimen collected
1999 Reference <0.0001
2000 NS ([section])
2001 1.8 (0.9-3.7)
2002 3.2 (1.5-6.9)
2003 5.2 (2.5-10.5)
2004 4.4 (2.2-8.8)
* MRSA, methicillin-resistant Staphylococcus aureus; HA, healthcare
associated, CI, confidence interval, SD, standard deviation; SE,
standard error; NS, not significant; # boldface indicates
significance.
([dagger]) Multivariate analysis results reflect time in weeks.
([double dagger]) Measured with the Cochran-Armitage test of trends.
([section]) Was not a significant predictor in the multivariate model.
Table 2. Summary of genetic testing for 24 healthcare-associated
MRSA blood isolates * ([dagger])
mecR1
No. isolates SCCmec mecl (PB)
8 IV -- --
1 IV -- --
2 IV -- --
1 ([section]) IV -- -
5 II + +
4 II + +
1 II + +
1 ([section]) II + +
1 ([paragraph]) -- -- --
No. isolates pvl MLST Clindamycin
8 + 8 S
1 + 1 S
2 -- 8 S
1 ([section]) -- 8 R
5 -- 5 R
4 -- 5 R
1 -- 8 R
1 ([section]) -- 5 S
1 ([paragraph]) -- 5 R
SCCmec type
phenotype
([double
No. isolates Gentamicin TMP-SMX dagger])
8 S S IV
1 S S IV
2 S S IV
1 ([section]) R R II
5 R S II
4 S S II
1 S S II
1 ([section]) S S IV
1 ([paragraph]) S S I
* MRSA, methicillin-resistant Staphylococcus aureus; PB,
penicillin-binding region; MLST, multilocus sequence typing; R,
resistant; S, susceptible; TMP-SMX, trimethoprim-sulfamethoxazole.
([dagger]) All isolates were associated with mecA and ccr2 genes.
([double dagger]) Phenotype: as defined by the study case definition,
according to antimicrobial drug susceptibilities (see Methods).
([section]) SCCmec phenotype did not match genotype.
([paragraph]) SCCmec was not located for this isolate.
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