| Literature DB >> 19552801 |
Floriana Campanile1, Dafne Bongiorno, Sonia Borbone, Stefania Stefani.
Abstract
The aim of our study was to trace the dynamic changes of hospital-associated methicillin-resistant Staphylococcus aureus (HA-MRSA) lineages in Italy, comparing the genotypic backgrounds of contemporary isolates over a period of 17 years, with those of a sample of early MRSA strains from 1980. In total, 301 non-repetitive MRSA clinical isolates, recovered from 19 Italian hospitals between 1990 and 2007 were selected and analyzed for their antibiotic resistance, typed by PFGE and SCCmec, grouped into clonal-types and further characterized using Multi Locus Sequence Typing (MLST). A sample of fifteen early MRSA strains from 1980 was also used for comparison. The most interesting feature was the recent increase of ST228-MRSA-I (formerly the Italian clone; PFGE E) over the period 2000-2007 (57%), when compared to the period 1990-1999 (29%), and its stability to date, associated with a decrease of the highly epidemic ST247-MRSA-IA (formerly the Iberian clone; PFGE A), (23% from 1990 to 1999, 6% from 2000 to 2007). ST1-MRSA-I (1 out of 2 strains carrying ccrA2B2), ST8-MRSA-I (4 strains), ST15-MRSA-I (1 out of 4 carrying ccrA2B2) and ST30-MRSA-I (2 out of 5 carrying no ccrAB-types and ccrC) were the predominant earliest STs among the MRSA strains in 1980. A temporal shift in the susceptibility levels to glycopeptides was observed: strains with vancomycin MIC of >or= 2 mg/L increased from 19.4% to 35.5%. In conclusion, we describe the alternation of MRSA clones that occurred in hospitals from 1990 to 2007 and the increase of the glycopeptide MIC levels, reflecting a worldwide trend. We document the detection of ST1, ST8, ST15 and ST30 in the 1980 isolates; we hypothesize their possible latency and their appearance as the current CA-MRSA clones.Entities:
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Year: 2009 PMID: 19552801 PMCID: PMC2708121 DOI: 10.1186/1476-0711-8-22
Source DB: PubMed Journal: Ann Clin Microbiol Antimicrob ISSN: 1476-0711 Impact factor: 3.944
Figure 1Description of MRSA clones. a) Distribution of the MRSA clones in periods A (1990–1999) and B (2000–2007); b) Description of the molecular backgrounds (ST, SCCmec and CC) of main clones isolated in Italy, correlated to their previous names; c) Graphical representation of alternation of MRSA clones in Italy during the 27-year period of study. *Italian and Southern Germany clones belong to the same ST228-MRSA-I, but they differ for their PFGE profile. **UK EMRSA-15 was often reported in literature as gentamicin-susceptible MRSA (GS-MRSA) clone. (ST: Sequence-Type; SCCmec: Staphylococcal Cassette Chromosome mec; CC: Clonal-Complex).
Antibiotic-resistance (%) of various antibiotics against 301 MRSA strains, compared with a sample of Italian isolates from 1980.
| S | R | S | R | S | R | |
| Gentamicin | 73.3 | 26.6 | 1.9 | 98.1 | 22** | 88 |
| Erythromycin | 86.6 | 13.3 | 16.9 | 83.1 | 16.3 | 83.7 |
| Clindamycin | 86.6 | 13.3 | 15 | 85 | 35 | 75 |
| Tetracycline | 73.3 | 26.6 | 33.1 | 67 | 82.2° | 17.8 |
| Ciprofloxacin | 80 | 20 | 3 | 97 | 3.5 | 96.5 |
| Rifampin | 73.3 | 26.6 | 33.7 | 66.3* | 79 | 21 |
| Cotrimoxazole | 86.6 | 13.3 | 58.1*** | 42 | 91.5 | 8.5 |
* Rifampin resistance is characteristic of CC8 (ST247 and 239)
** Including the gentamicin-susceptible clone
*** Cotrimoxazole resistance is a marker of ST 239
° The tetracycline susceptible Italian clone increased in this period
Figure 2MIC distributions of the major anti Gram-positive drugs against MRSA strains. MIC50 and MIC90 in bold and underlined; MIC50 only in bold; MIC90 in grey.
Number of MRSA strains with glycopeptide MICs of ≤ 0.5, 1, and ≥ 2 mg/L in ST247-MRSA-IA, ST239-MRSA-IIIA and ST228-MRSA-I isolated in periods A and B
| ≤ 0.5 | 1 | ≥ 2 | ≤ 0.5 | 1 | ≥ 2 | |
| 51 (52) | 28 (28.5) | 19 (19.4) | 19 (20.4) | 41 (44.1) | 33 (35.5) | |
| 49 (50) | 25 (25.5) | 22 (22.4) | 20 (21.5) | 30 (32.2) | 43 (46.2) | |
° P < 0.001