THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec DNA 2, , % 1.65% 1.17% 90% 9 Escherichia coli -
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1 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS sita oxacin sita oxacin STFX 50 mg 10% STFX 1, % 1,235/1, % 466/ % 511/ % 49/ % 145/ % 64/ % 49/ % 48/ % 545/602 Escherichia coli 92.7% 294/317 Enterococcus faecalis 86.0% 43/50 Pseudomonas aeruginosa 66.7% 16/24 Klebsiella pneumoniae 95.2% 20/21 Chlamydia trachomatis 88.9% 8/9 2.71% 37/1, % % 7 1 STFX 91.4% 87.2% Sita oxacin STFX STFX
2 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec DNA 2, , % 1.65% 1.17% 90% 9 Escherichia coli - Extended-Spectrum Beta-Lactamase: ESBL STFX E. coli 2,3,10 70% 11 1,452 STFX I mg 1 STFX 50 mg 10% 1 g STFX 100 mg STFX 3,558 1, FAX %
3 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS % % ICH MedDRA/J: Medical Dictionary for Regulatory Activities/J Ver Fig. 1. Distribution of the patients in the study.
4 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec Table 1. Patients demographics.
5 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS II 1. STFX 3,558 1,452 1, % % % 87 1, ,351 Fig ,351 Table % SD % 78.2% 3.3% 8.9% 30.0% 88.2% 1 50 mg % mg % 8.2% SD % SD % 48.4% 23.5% 33.5% 31.4% 86.5% 44.5% 1 50 mg % 91.0% mg % 5.2% SD % SD 1 50 mg % mg % SD , % 1,235/1,351 Table % 466/ % 511/ % 49/ % 145/ % 64/ % 352/ % 159/178 Table
6 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec Table 2. Clinical ef cacy by patient demographics.
7 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS % % 116/ % 150/ % 245/281 Table % 142/ % 446/ % 89/ % 56/61 Table % 35/ % 14/ % 75/ % 35/ % 35/ % 15/ % 125/ % 47/ % 5/ % 12/13 Table % 24/25 3 1, % 83.2% 119/143 Table % 48/ % 49/ Table 3 Escherichia coli E. coli 52.7% Enterococcus 12.0% Staphylococcus 11.3% Streptococcus 7.5% Klebsiella 5.0% Pseudomonas aeruginosa P. aeruginosa 4.0% E. coli 70.5% 10% E. coli 35.6% Enterococcus 17.2% Staphylococcus 14.6% Streptococcus 11.3% E. coli 83.3% E. coli 45.0% Enterococcus Staphylococcus 13.3% P. aeruginosa 11.7% 52.9% Chlamydia trachomatis C. trachomatis % 545/602 Table 4 E. coli 92.7% 294/317 Enterococcus faecalis E. faecalis 86.0% 43/50 P. aeruginosa 66.7% 16/24 Klebsiella pneumoniae K. pneumoniae 95.2% 20/21 C. trachomatis 88.9% 8/9 96.3% 258/ % 204/ % 17/ % 50/ % 16/17 E. coli 96.3% 182/ % 73/ % 14/ % 24/27
8 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec Table 3. Distribution of causative bacteria.
9 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS Table 4. Bacterial eradication rate.
10 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec Table 5. Bacterial eradication rate complicated cystitis.
11 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS Table 6. Incidence of adverse drug reactions ADRs.
12 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec STFX 83.1% 148/ % 26/ % 30/33 E. coli 81.3% 52/ % 13/ % 8/8 Table 5 C. trachomatis 88.9% 8/9 Neisseria gonorrhoeae STFX 6 Table 4 4 1, % Table % % mg STFX QT 1.64% 8/ % 16/ % 4/ % 6/ % 3/ % 14/ % 10/ % 13/470 Table mg % 36/1, mg % 1/96 28 III E. coli levo oxacin LVFX MIC 2 g/ml % % MIC g/ml 16 g/ml 4 7, 13 STFX E. coli 2,3,10 70%
13 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS Table 7. Incidence of ADRs by age. 11 STFX STFX 3, , % 1,235/1,351 87% 94.8% 95.5% 88.6% 14 E. coli 70.5% 83.3% E. coli 70 80% E. coli 96.3% 182/ % 14/15 E. coli E. faecalis P. aeruginosa K. pneumoniae Staphylococcus STFX E. coli 85% 83% UTI 4 18
14 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec MATSUMOTO E. coli 19 MATSUMOTO STFX 77.4% 48/62 E. coli DNA quinolone-resistance determining region: QRDR 1 2 LVFX, cipro oxacin, tosu oxacin 2,3 QRDR 3 E. coli LVFX MIC 2.0 g/ml 2.1% 4/193 STFX MIC 1.0 g/ ml 65.8% 127/ STFX 2.71% 37/1, % % % 1.65% 1.17% 9 1 STFX STFX 91.4% 87.2% Sita oxacin 1 SATO, K.; K. HOSHINO, M. TANAKA, et al.: Antimicrobial activity of DU-6859, a new potent uoroquinolone, against clinical isolates. Antimicrob. Agents Chemother. 36: , Sita oxacin 56 S-1 : 1 17, : 43 51, ,475 Jpn. J. Antibiotics 58: 17 44, ,639 Jpn. J. Antibiotics 59: , ,919 Jpn. J. Antibiotics 62: , ,866 Jpn. J. Antibiotics 65: , Sita oxacin Jpn. J. Antibiotics 63: ,
15 Dec THE JAPANESE JOURNAL OF ANTIBIOTICS sita oxacin Jpn. J. Antibiotics 64: , : , NAKASHIMA, M.; T. UEMATSU, K. KOSUGE, et al.: Pharmacokinetics and tolerance of DU-6859a, a new uoroquinolone, after single and multiple oral doses in healthy volunteers. Antimicrob. Agents Chemother. 39: , : , ,474 Jpn. J. Antibiotics 56: , mg 10% : , : , : 29 39, UTI 4 45: , MATSUMOTO, T.; R. HAMASUNA, K. ISHIKAWA, et al.: Nationwide survey of antibacterial activity against clinical isolates from urinary tract infections in Japan Int. J. Antimicrob. Agents 37: , 2011 Ef cacy and safety of sita oxacin in patients with urinary tract infections TAKUYUKI MATSUMOTO 1, HIROKI YAMAGUCHI 1, KAZUHIRO UCHINO 1, MEGUMI TAKAHASHI 1, HIROKO KODAMA 1, SATOKO HAMAJIMA 1, RIE YONEMOCHI 2, SACHIKO FUJITA 2, ATSUSHI TAKITA 3, NAOKI YAMANOUCHI 3, TOMOO SHIOZAWA 1 and YUKIHIRO OKUTANI 1 1 Post Marketing Studies Management Department, Daiichi Sankyo Company, Limited 2 Pharmacovigilance Department, Daiichi Sankyo Company, Limited 3 Clinical Data and Biostatistics Department, Daiichi Sankyo Company, Limited Sita oxacin STFX, Gracevit 50 mg, ne granules 10%, a new quinolone antibacterial agent, was approved in January 2008, and the use-results survey was carried out over the 2 years between December 2008 and November We studied the ef cacy and safety of STFX in 1,452 patients with urinary tract infections cystitis, pyelonephritis, urethritis. The total efficacy rate for urinary tract infections was 91.4% 1,235/1,351 patients. Ef cacy rates, classi ed by the type of infection, were: uncomplicated cystitis 95.9% 466/486
16 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec patients, complicated cystitis 87.2% 511/586 patients, uncomplicated pyelonephritis 96.1% 49/51 patients, complicated pyelonephritis 93.5% 145/155 patients, and urethritis 87.7% 64/73 patients. Ef cacy rates were 86.0% 49/57 patients for non-responders to cephems and 77.4% 48/62 patients for non-responders to quinolones. The eradication rate of indicated strains was 90.5% 545/602 strains. The eradication rates of major causative bacteria were; Escherichia coli 92.7% 294/317 isolates, Enterococcus faecalis 86.0% 43/50 isolates, Pseudomonas aeruginosa 66.7% 16/24 isolates, Klebsiella pneumoniae 95.2% 20/21 isolates, and Chlamydia trachomatis 88.9% 8/9 isolates. The incidence of adverse drug reactions ADRs was 2.71% 37/1,365 cases. Major ADRs were diarrhoea 0.88%, 12 cases and hepatic function disorders 0.51%, 7 cases. A serious ADR hepatic function abnormality was observed in 1 case, and the hepatic function in this patient returned to normal after treatment with STFX was discontinued. In conclusion, these results suggest that STFX is a useful antibacterial agent with an ef cacy rate of 91.4% against urinary tract infections, with a minimum ef cacy rate of 87.2% against complicated cystitis, and has no serious problems in its safety pro le.
THE JAPANESE JOURNAL OF ANTIBIOTICS 67 3 June 2014 STFX mg mg mg mg mg 1
June 2014 THE JAPANESE JOURNAL OF ANTIBIOTICS 67 3 175 29 1 2 2 2 2 2 3 4 4 5 5 2 2 1 2 3 4 5 2014 4 15 STFX 50 mg 10% 2011 8 1 100 mg 1 1 2011 12 2013 5 226 1,186 1,089 1,069 2.11% 23/1,089 1.10% 12/1,089
400 46 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 Dec. 2012 LVFX 100 mg 3 / 7 150 mg 2 / 7 2 2006 2008 9 LVFX PK PD 2009 7 100 mg 1 3 500 mg 1 1 AUC/MIC
Dec. 2012 THE JAPANESE JOURNAL OF ANTIBIOTICS 65 6 399 45 2012 11 5 LVFX 500 mg 1 1 20 Chlamydia trachomatis C. trachomatismycoplasma genitalium M. genitalium LVFX 1 500 mg 1 1 7 22 22 C. trachomatis 17
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日本化学療法学会雑誌第61巻第6号
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VOL.27 S-5 CHEMOTHERAPY Table 1 Clinical evaluations of cefamandole on UTI (1) Benign prostatic hypertrophy (2) Transurethral resection of bladder tum
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Title 尿路感染症分離菌の年次的変遷と薬剤感受性の検討 ( ニューキノロン系を中心として ) 深津, 英捷 ; 本多, 靖明 ; 水本, 裕之 ; 瀧, 知弘 ; 三井, Author(s) 々村, 仁志 ; 羽田野, 幸夫 ; 平岩, 親輔 ; 吉川, 和宏 ; 山田彰 ; 瀬川, 昭夫 Ci
Title 尿路感染症分離菌の年次的変遷と薬剤感受性の検討 ( ニューキノロン系を中心として ) 深津, 英捷 ; 本多, 靖明 ; 水本, 裕之 ; 瀧, 知弘 ; 三井, Author(s) 々村, 仁志 ; 羽田野, 幸夫 ; 平岩, 親輔 ; 吉川, 和宏 ; 山田彰 ; 瀬川, 昭夫 Citation 泌尿器科紀要 (1992), 38(11): 1215-1223 Issue Date
CHEMOTHERAPY
VOL.40 S-1 coagulase negative Staphylococcus sp, methicillin- resistant Staphylococcus aureus (MRSA), Enterococcus faecalis, Escherichia coli, Citrobacter freundii, Klebsiella pneumoniae, Enterobacter
semen quality or those without WBC in semen. In the patients with azoospermia and normal FSH levels (normogonadotropic azzospermia), the antibody (IgG
CLINICAL STUDIES OF UROGENITAL INFECTIONS WITH CHLAMYDIA TRACHOMA TIS Report 2. The Epidemiology of Chlamydial Infections in Okayama District in Japan and Detection of Antibodies to Chlamydiae in the Sera
b) Gram-negative bacteria Fig. 2 Sensitivity distribution of clinical isolates : E. coli Fig. 3 Sensitivity distribution of clinical isolates : Pseudomonas Fig. 1 Sensitivity distribution of clinical isolates
CHEMOTHERAPY Proteus mirabilis GN-79 Escherichia coli No. 35 Proteus vulgaris GN-76 Pseudomonas aeruginosa No. 11 Escherichia coli ML-1410 RGN-823 Kle
VOL. 29 NO.8 CHEMOTHERAPY 865 CHEMOTHERAPY Proteus mirabilis GN-79 Escherichia coli No. 35 Proteus vulgaris GN-76 Pseudomonas aeruginosa No. 11 Escherichia coli ML-1410 RGN-823 Klebsiella pneumoniae GN-69
CHEMOTHERAPY FEB Table 1 Background of volunteers
CHEMOTHERAPY FEB. 1985 Table 1 Background of volunteers Table 3 Reproducibility of saisomicln In the EIA and the RIA Fig.1 Comparison of the EIA with the RIA or bioassay of sisomicin Table 4 Blood levels
EVALUATION OF NOCTURNAL PENILE TUMESCENCE (NPT) IN THE DIFFERENTIAL DIAGNOSIS OF IMPOTENCE Masaharu Aoki, Yoshiaki Kumamoto, Kazutomi Mohri and Kazunori Ohno Department of Urology, Sapporo Medical College
VOL. 17 NO. 7 CHEMOTHERAPY 1305 1) W. BRumFirr et al. : Clinical and laboratory studies with carbenicillin. Lancet 1: 1289~ 1293, 1967 2) E. T. KNUDSEN et al. : A new semisynthetic penicillin active against
Table 1 Classification of female patients with vealcal irritating symptom by their signs Urination pain with other vesical irritability or not Table 2 Serum levels of DL-8280 after a single oral administration
VOL.47 NO.5 Table 1. Susceptibility distribution of Ĉ- lactams against clinical isolates of MRSA MRSA: rnethicillin- resistant Staphylococcus aureus
MAY 1999 VOL.47 NO.5 Table 1. Susceptibility distribution of ƒà- lactams against clinical isolates of MRSA MRSA: rnethicillin- resistant Staphylococcus aureus (oxacillin MIC: 4ƒÊg/ ml) FMOX: flomoxef,
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β β β β β Streptococcus pneumoniaehaemophilus influenzaemoraxella catarrhalismycoplasma pneumoniaechlamydia pneumoniae β Key wordsβ mys nilc laci ngis Table. Assessmentschedule Parameters Patientcharacteristics
Table 1 Patients with various renal function * Ccr, Creatinine clearance ml/min per 1. 48 m2 ** C.V.D., Cerebral vascular disease ; C.R F., Chronic renal failure ; H.D., Hemoclialysis ; D., Dialyzer ;
THE JAPANESE JOURNAL OF ANTIBIOTICS 63 13 243 ( 37 ) 2007 12 2008 5 19 863 methicillin-susceptible Staphylococcus aureus (MSSA) Escherichia coli levof
242 ( 36 ) THE JAPANESE JOURNAL OF ANTIBIOTICS 63 _ 3 prulifloxacin * ** ** CMC * ** 2010 2 22 Prulifloxacin ulifloxacin (UFX) 3 1 2003 12 2004 5 19 534 2 2005 12 2006 5 19 805 3 THE JAPANESE JOURNAL OF
Dec. THE JAPANESE JOURNAL OF ANTIBIOTICS XXXVII (45)
Dec. THE JAPANESE JOURNAL OF ANTIBIOTICS XXXVII-12 2305(45) 2306(46) THE JAPANESE JOURNAL OF ANTIBIOTICS XXXVII-12 Dec. Dec. THE JAPANESE JOURNAL OF ANTIBIOTICS XXXVII-12 2307(47) 2308(48) THE JAPANESE
VOL.30 NO.12 CHEMOTHERAPY Fig. 1 Effect of temperature on the growth curve of A. calcoaceticus A. calcoaceticits Ac 54 A. calcoacetictts Ac 164 Fig. 2 Effect of medium ph on the growth curve of A. calcoaceticus
CHEMOTHERAPY OCT. 1994 Tazobactam Piperacillin Fig. I. Chemical structures of tazobactam and piperacillin. Table 1. Media used for preculture and MIC determination BHIB: Brain heart infusion broth (Difco),
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CHEMOTHERAPY MAY. 1988 CHEMOTHERAPY Fig. 1 Chemical structure CHEMOTHERAPY MAY. 1988 VOL.36 5-1 CHEMOTHERAPY CHEMOTHERAPY MAY. 1988 VOL.36 S-1 CHEMOTHERAPY CHEMOTHERAPY MAY. 1988 VOL.36 S-1 CHEMOTHERAPY
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µ µ Key words Streptococcus pneu- moniae S. pneumoniae µ µ I γ H H C HN F F O N O CO H H C SO H H O Fig.. ChemicalstructureofGRNX. γ γ II Haemophilus influenzae Pseudomonas aeruginosa Streptococcus intermedius
CHEMOTHERAPY APR Fig. 2 The inactivation of aminoglycoside antibiotics by PC-904 Fig. 3 Serum concentration of PC-904 (1) Fig. 4 Urinary recover
VOL.26 S-2 CHEMOTHERAPY Gentamicin (GM), Dibekacin (DKB), Tobramycin Fig. 1 Protein concentration and protein binding rate Table 2 Protein binding rate of PC-904 in serum of healthy adults, and patients
03-b-„FŒ{›xŒ¾-4.02
518( 30 ) THE JAPANESE JOURNAL OF ANTIBIOTICS 58 6 Dec. 25 2003 1. * * Dec. THE JAPANESE JOURNAL OF ANTIBIOTICS 58 6 519( 31 ) 9 5 2003 8 2004 7 14 565 701 258 (36.8%) 443 (63.2%) Staphylococcus aureus
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moxifloxacin in vitro moxifloxacin in vitro 17 9 6 17 11 21 moxifloxacinmflx in vitro cefdinir CFDNclavulanic acidamoxicillincvaampcclarithromycincamclindamycincldm levofloxacinlvfx 1MFLX Clostridium clostridiiformeclostridium
Fig. 1 Chemical structure of norfioxacin (AM-715)
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Fig. 1 Clinical findings and extent of inflammation area in female urethrocystitis Fig. 2 Classification and distribution of female patients with blad
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CHEMOTHERAPY DEC phvlococcus aureus Staphylococcus Enterococcus faecalis Escherichia Klebsiella pneumoniae Serratia marcescens Pseudomonas cepac
CHEMOTHERAPY DEC. 1988 phvlococcus aureus Staphylococcus Enterococcus faecalis Escherichia Klebsiella pneumoniae Serratia marcescens Pseudomonas cepacia 1 Bacteroides bivius Propionibacterium granulosum
Table 1 Antibacterial spectra of CPM and other antimicrobials against anaerobes Fig. 1 In vitro activity of CPM and other antibiotics against B. fragilis (136 strains) Fig. 2 In vitro activity of CPM and
CHEMOTHERAPY 52 MAY d a a. Normal S. aureus d Đg/ml, 2h; e b b Đg/ml, Abnormal e. division lh; Abnormal thickening division cross f c. 1
Levloxacin V.:1 Z iiiir fa L CHEMOTHERAPY 52 MAY d a a. Normal S. aureus d. 0.39 Đg/ml, 2h; e b b. 0.10 Đg/ml, Abnormal e. division lh; Abnormal thickening division cross f c. 1992 0.39 Đg/ml, and Fig.
CHEMOTHERAPY Methicillin-resistant S.aureus(MRSA) coccus epidermidis 105 Streptococcus pyogenes E.faecali senterococcus avium Enterococcus faecium Str
cefaclor(ccl),cefuroxime(cxm),cefixime (CFIX),cefteram(CFTM),cefdinir(CFDN) pneumoniae,streptococcus pyogenes Moraxella catarrhalis,haemophilus influenzae,escherichia coli, Klebsiella pneumoniae,proteus
日本化学療法学会雑誌第65巻第4号
Mycoplasma pneumoniae M. pneumoniae M. pneumoniae M. pneumoniae M. pneumoniae M. pneumoniae Key words Mycoplasma pneumoniae Mycoplasma pneumoniae M. pneumoniae I M. pneumoniae M. pneumoniae M. pneumoniae
Feb THE JAPANESE JOURNAL OF ANTIBIOTICS ,4 2,4 2,4 2,3,4 2,3,4 2,3, ,3, Garenoxacin GRNX Levofloxacin LV
Feb. 2016 THE JAPANESE JOURNAL OF ANTIBIOTICS 69 1 27 27 1,4 2,4 2,4 2,3,4 2,3,4 2,3,4 2 1 2,3,4 1 2 3 4 2015 10 21 9 Garenoxacin GRNX Levofloxacin LVFX Sitafloxacin STFX Moxifloxacin MFLX Pharmacokinetics-Pharmacodynamics
VOL.30 NO.10 CHEMOTHERAPY 1123 Fig,1 Group B case 6 hepatolithiasis,e.k.66 y.0.,f.45kg Postoperative wound infection Fig.2 Group B case 15 gastric cancer,k.k.60 y.o.,m. Postoperative peritonitis Fig.3
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.
日本化学療法学会雑誌第65巻第3号
μ Key words Chlamydia trachomatis C. trachomatis I Table1.Observation items, categories and scores Observation item Category Score Body temperature () Lower abdominal pain Uterine corpus tenderness Condition
Table 1. Concentration of ritipenem in plasma, gallbladder tissue and bile after ritipenem acoxil administration (200 mg t.i.d., 3 days) N.D.: not det
Table 1. Concentration of ritipenem in plasma, gallbladder tissue and bile after ritipenem acoxil administration (200 mg t.i.d., 3 days) N.D.: not detected *: time after last administration Table 2. Concentration
VOL.39 S-3
VOL.39 S-3 CHEMOTHERAPY SEPT.1991 Table 1. Background of characteristics and allocation of 5 healthy male volunteers in a multiple-dose study on panipenem/betamipron Day 1 Fig. 1. Schedule of multiple-dose
Streptococcus pneumoniae,streptococcus pyogenes,streptococcus agalactiae,neisseria gonorrhoeae,h.influenzae,moraxella subgenus Branhamella catarrharis
Streptococcus pneumoniae,streptococcus pyogenes,streptococcus agalactiae,neisseria gonorrhoeae,h.influenzae,moraxella subgenus Branhamella catarrharis, E.coil,Klebsiella pneumoniae,klebsiella oxytoca,proteus
Staphylococcus epidermidis Streptococcus pneumoniae Staphylococcus epidermidis Streptococcus pneumontae S. epidermidis Table 1. Summary of the organis
Staphylococcus aureus S. aureus (MRSA) vancomycin (VCM), arbekacin (ABK) Streptococcus pneumoniae cefuzonam (CZON), cefpirome (CPR) S. pneumoniae Enterococcus faecalis ampicillin (ABPC), imipenem (IPM)
CHEMOTHERAPY AUG. 1982 VOL. 30 NO. 8 CHEMOTHERAPY Fig.1 Relation between various-closis of cefazolin and detection rate of organisms in heart blood of dying mice with E. coli and P. aeruginosa infection