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Nationwide surveillance of parenteral antibiotics containing meropenem activities against clinically isolated strains in 2006
Authors:Yamaguchi Keizo  Ishii Yoshikazu  Iwata Morihiro  Watanabe Naoki  Uehara Nobuyuki  Yasujima Minoru  Kasai Takeshi  Suwabe Akira  Yamahata Kumiko  Kaku Mitsuo  Kanemitsu Keiji  Imafuku Yuji  Nishiyama Kyouko  Murakami Masami  Yomoda Sachie  Taniguchi Nobuyuki  Yamada Toshiyuki  Nomura Fumio  Watanabe Masaharu  Kanno Harushige  Aihara Masanori  Maesaki Shigefumi  Hashikita Giichi  Kondo Shigemi  Misawa Shigeki  Horiuchi Hajime  Tazawa Yoko  Nakashima Hideki  Takemura Hiromu  Okada Masahiko  Yamazaki Fusako  Horii Toshinobu  Maekawa Masato  Baba Hisashi  Ishigo Shiomi  Fujita Naohisa  Komori Toshiaki  Ichiyama Satoshi
Institution:Department of Microbiology and Infectious Diseases, Toho University School of Medicine.
Abstract:The antibacterial activity of meropenem (MEPM) and other parenteral antibiotics against clinical isolates of 876 strains of Gram-positive bacteria, 1764 strains of Gram-negative bacteria, and 198 strains of anaerobic bacteria obtained from 30 medical institutions during 2006 was measured. The results were as follows; 1. MEPM was more active than the other carbapenem antibiotics tested against Gram-negative bacteria, especially against enterobacteriaceae and Haemophilus influenzae. MEPM was also active against most of the species tested in Gram-positive and anaerobic bacteria, except for multi-drug resistant strains including methicillin-resistant Staphylococcus aureus. 2. As for Pseudomonas aeruginosa, all of the MEPM-resistant strains were resistant to imipenem (IPM). MEPM showed low cross-resistant rate both againt IPM-resistant P. aeruginosa (41.8%) and ciprofloxacin-resistant P. aeruginosa (33.3%). 3. The proportion of extended-spectrum beta-lactamase (ESBL) strains was 4.3% (6 strains) in Escherichia coli, 1.1% (1 strain) in Citrobacter freundii, 21.7% (5 strains) in Citrobacter koseri, 3.1% (4 strains) in Klebsiella pneumoniae, 3.3% (3 strains) in Enterobacter cloacae, 0.8% (1 strain) in Serratia marcescens, and 4.9% (2 strains) in Providencia spp. The proportion of metallo-beta-lactamase strains was 3.1% (10 strains) in P. aeruginosa. 4. Of all species tested, there were no species, which MIC90 of MEPM was more than 4-fold higher than those in our previous study. Therefore, there is almost no significant decrease in susceptibility of clinical isolates to meropenem. In conclusion, the results from this surveillance study suggest that MEPM retains its potent and broad antibacterial activity and therefore is a clinically useful carbapenem at present, 11 years after available for commercial use.
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