Oct THE JAPANESE JOURNAL OF ANTIBIOTICS Pseudomonas aeruginosa 186 P. aeruginosa piperacillin PIPC, taz

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1 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS Pseudomonas aeruginosa 186 P. aeruginosa piperacillin PIPC, tazobactam/piperacillin TAZ/PIPC, ceftazidime CAZ, cefepime CFPM, imipenem IPM, meropenem MEPM, doripenem DRPM, aztreonam AZT, ciprofloxacin CPFX, levofloxacin LVFX, amikacin AMK colistin CL MIC 50/90 8/32, 4/32, 2/8, 2/16, 1/32, 0.5/8, 0.25/4, 8/32, 0.25/8, 0.5/16, 4/8 1/1 μg/ml2 1.1%

2 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct P. aeruginosa Pseudomonas aeruginosa 1 3 MDRP 4 MDRP 5, I Piperacillin PIPC, tazobactam/piperacillin TAZ/PIPC, ceftazidime CAZ, cefepime CFPM, imipenem/cilastatin IPM/CS, meropenem MEPM, doripenem DRPM, aztreonam AZT, ciprofloxacin

3 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS CPFX, levofloxacin LVFX, amikacin AMK, colistin CL 12 IPM/ CS IPM TAZ/PIPC TAZ 4 μg/ml PIPC MIC 3. MIC Clinical and Laboratory Standards Institute CLSI 11 CLSI MIC interpretive standard SAS release 9.2 χ II % % % MIC 50, MIC β- DRPM MIC μg/ml MEPM 0.5 μg/ml, IPM 1 μg/ml, CAZ CFPM 2 μg/ml, TAZ/PIPC 4 μg/ml, PIPC AZT 8 μg/ml MIC 90 DRPM 4 μg/ml CAZ, MEPM 8 μg/ ml, CFPM 16 μg/ml, PIPC, TAZ/PIPC, IPM, AZT 32 μg/ml CAZ 90.3% CFPM 88.2%, TAZ/ PIPC 85.5%, PIPC 85.0%, DRPM 84.4%, MEPM 78.5%, IPM 73.7%, AZT 73.1% CPFX LVFX MIC μg/ml, 0.5 μg/mlmic 90 8 μg/ml 16 μg/ml 85.0%, 79.6% AMK MIC 50 MIC 90 4 μg/ml, 8 μg/ml 97.8% CL MIC 50 MIC 90 1 μg/ml IPM 4 μg/ml MIC 49 MIC 50, MIC CL MEPM DRPM 22.4% 40.8% 50% P AMK 91.8%6% P CPFX LVFX 61.2% 53.1% P

4 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct MIC 50, MIC 90

5 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS IPM 4 μg/ml 49 MIC 50, MIC 90

6 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct PIPC TAZ/PIPC 63.3% 65.3% P CAZ CFPM 75.5% 67.3% P AZT 53.1% P % 2 3. MDRP CPFX MIC 4 μg/ml IPM MIC 16 μg/ml AMK MIC 32 μg/ml kekkaku-kansenshou11/ html CPFX, IPM, AMK % % 4 2.2% IPM, CPFX, AMK CPFX IPM, CPFX AMK, IPM AMK % 3 1.6% 3 1.6% CPFX IPM 2 3 MDRP 2 1.1% 2008 CPFX, IPM AMK 2 MDRP % P Susceptible Intermediate Resistant PIPC, TAZ/PIPC, CAZ, CFPM, IPM, MEPM, DRPM, AZT AMK 2008 CPFX 76.0% 85.0% P LVFX 73.4% 79.6% P CL 96.4% 100.0% P

Oct. 2016 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 333 33 1. MIC 50, MIC 90 4, 5, 6 2 β- TAZ/PIPC 92.6% 87.5% 81.0% CAZ 96.3%, 92.5%, 86.1% IPM 80.0% 73.4% 55.6% MEPM 85.0%, 74.7%, 70.4% LVFX 92.

7 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS MIC 50, MIC 90 4, 5, 6 2 β- TAZ/PIPC 92.6% 87.5% 81.0% CAZ 96.3%, 92.5%, 86.1% IPM 80.0% 73.4% 55.6% MEPM 85.0%, 74.7%, 70.4% LVFX 92.6% 80.0% 74.7% CL, AMK 4. MIC 50 MIC 90 7 AMK CL MIC 50, MIC 90 CFPM, MEPM, DRPM, AZT CPFX MIC MIC 90 PIPC, AMK, CL III β- PIPC, TAZ/PIPC, CAZ, CFPM, IPM, MEPM, DRPM AZT MIC 50/90 8/32, 4/32, 2/8, 2/16, 1/32, 0.5/8, 0.25/4,

8 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct MIC 50, MIC 90

9 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS MIC 50, MIC 90

10 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct MIC 50, MIC 90

11 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS /32 μg/ml DRPM MIC 50/90 CLSI CAZ, CFPM, TAZ/PIPC PIPC, TAZ/PIPC, CAZ, CFPM, IPM, MEPM, DRPM AZT MIC 50/90 8/32, 8/32, 2/8, 4/16, 2/16, 0.5/8, 0.5/4 8/32 μg/ml PIPC, TAZ/PIPC, CAZ, CFPM, IPM, MEPM MIC 50/90 8/128, 8/64, 2/32, 4/16, 2/16, 0.5/16 μg/ml TAZ/PIPC 85.5% 80.9% MEPM 78.5% 72.9% 5% IPM 4 μg/ml MIC 49 CL AMK 6% 20 50% MDRP CL 2008 CL CL MIC 50 MIC 90 1 μg/mlclsi 100% AMK CPFX, IPM MDRP MDRP

12 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct

13 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS CAZ, TAZ/PIPC 96.3%, 92.6% IPM, MEPM 55.6%, 70.4% β- 7 MEPM DRPM MIC MSD MSD MSD Meiji Seika MSD Meiji Seika

14 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 5 Oct : 33 41, GÓMEZ, M. I. & A. PRINCE: Opportunistic infections in lung disease: Pseudomonas infections in cystic fibrosis. Curr. Opin. Pharmacol. 7: , OSIH, R. B.; J. C. MCGREGOR, S. E. RICH, et al.: Impact of empiric antibiotic therapy on outcomes in patients with Pseudomonas aeruginosa bacteremia. Antimicrob. Agents Chemother. 51: , TSUJI, A.; I. KOBAYASHI, T. OGURI, et al.: An epidemiological study of the susceptibility and frequency of multiple-drug-resistant strains of Pseudomonas aeruginosa isolated at medical institutes nationwide in Japan. J. Infect. Chemother. 11: 64 70, SEKIGUCHI, J.; T. ASAGI, T. MIYOSHI-AKIYAMA, et al.: Multidrug-resistant Pseudomonas aeruginosa strain that caused an outbreak in a neurosurgery ward and its aac 6 -Iae gene cassette encoding a novel aminoglycoside acetyltransferase. Antimicrob. Agents Chemother. 49: , KIRIKAE, T.; Y. MIZUGUCHI & Y. ARAKAWA: Investigation of isolation rates of Pseudomonas aeruginosa with and without multidrug resistance in medical facilities and clinical laboratories in Japan. J. Antimicrob. Chemother. 61: , Jpn. J. Antibiotics 58: , : , ,919 Jpn. J. Antibiotics 62: , Jpn. J. Antibiotics 59: , CLSI: Methods for dilution antimicrobial susceptibility tests for bacteria that grow aerobically; Approved standard-ninth edition. M07-A9. CLSI 32: CLSI: Performance standards for antimicrobial susceptibility testing; twenty-third informational supplement. M100-S23. CLSI 33: Jpn. J. Antibiotics 65: 15 26, Haemophilus influenzae Jpn. J. Antibiotics 65: , Jpn. J. Antibiotics 65: 1 14, β- Jpn. J. Antibiotics 66: , Jpn. J. Antibiotics 66: , tazobactam/piperacillin 61: , : 17 22, 2004

15 Oct THE JAPANESE JOURNAL OF ANTIBIOTICS Sensitivity surveillance of Pseudomonas aeruginosa isolates for several antibacterial agents in Chubu area Chubu Anti-biogram Study Group Research Laboratories, Toyama Chemical Co., Ltd., Development Division, Toyama Chemical Co., Ltd. AI KAKUMOTO, HAYATO OKADE, SHINGO MIZUNAGA and NOBUHIKO NOMURA Research Laboratories, Toyama Chemical Co., Ltd. JUNICHI MITSUYAMA Development Division, Toyama Chemical Co., Ltd. KAZUKIYO YAMAOKA Gifu University of Medical Science YUKO ASANO Department of Clinical Laboratory Medicine, Ogaki Municipal Hospital YOKO MATSUKAWA Clinical Laboratories, Gifu Prefectural Tajimi Hospital HIROYUKI SUEMATSU and HARUKI SAWAMURA Department of Infection Control and Prevention, Aichi Medical University Hospital SHIGENORI MATSUBARA Matsubara Otorhinolaryngology Clinic NAOHIRO SHIBATA Department of Infectious Diseases, Tohno Kousei Hospital KUNITOMO WATANABE Division of Anaerobe Research, Life Science Research Center, Gifu University YOSHIHIRO YAMAMOTO Department of Clinical Infectious Diseases, Toyama University Hospital HIROMICHI IWASAKI Division of Infection Control and Prevention, University of Fukui Hospital YUKA YAMAGISHI and HIROSHIGE MIKAMO Department of Clinical Infectious Diseases, Aichi Medical University We investigated the susceptibility to antibacterial agents of 186 clinical isolates of Pseudomonas aeruginosa isolated from medical facilities in Gifu, Aichi, Toyama, and Fukui prefectures from October 2013 to February MIC 50/90 of piperacillin PIPC, tazobactam/piperacillin TAZ/PIPC, ceftazidime CAZ, cefepime CFPM, imipenem IPM, meropenem MEPM, doripenem DRPM, aztreonam AZT, ciprofloxacin CPFX, levofloxacin LVFX, amikacin AMK and colistin CL against P. aeruginosa was 8/32, 4/32, 2/8, 2/16, 1/32, 0.5/8, 0.25/4, 8/32, 0.25/8, 0.5/16, 4/8 and 1/1 μg/ml respectively. Two strains of multidrug resistant P. aeruginosa were isolated 1.1% They were isolated from the respiratory tract, intra-abdominal, and urinary infection. The susceptible ratio against P. aeruginosa derived from intra-abdominal infection for carbapenem was lower than those from respiratory tract and urinary infection. The susceptible ratio against P. aeruginosa derived from urinary infection for penicillin, cephem, monobactam, and fluoroquinolone was lower than those from respiratory and intra-abdominal infection. It is meaningful to pay attention to the susceptibility to antibacterial agents in each clinical specimen from infected organ.

日本化学療法学会雑誌第64巻第4号

日本化学療法学会雑誌第64巻第4号 β β Moraxella catarrhalisescherichia colicitrobacter Klebsiella pneumoniaeenterobacter cloacaeserratia marcescens Proteus Providencia Pseudomonas aeruginosaacinetobacter Bacteroides fragilis β β E. colik.