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克林沙星、CI-990(PD 131112)和PD 138312对肠球菌的体外和体内活性

In vitro and in vivo activities of clinafloxacin, CI-990 (PD 131112), and PD 138312 versus enterococci.

作者信息

Cohen M A, Yoder S L, Huband M D, Roland G E, Courtney C L

机构信息

Infectious Diseases Section/Therapeutics Department, Parke-Davis Pharmaceutical Research, Division of Warner-Lambert Company, Ann Arbor, Michigan 48105-2495, USA.

出版信息

Antimicrob Agents Chemother. 1995 Sep;39(9):2123-7. doi: 10.1128/AAC.39.9.2123.

Abstract

Certain new fluoroquinolones have high activity against enterococci. Against Enterococcus faecalis (n = 18), MICs at which 90% of the isolates were inhibited were as follows (in micrograms per milliliter): clinafloxacin, 0.125; CI-990, 0.5; and PD 138312, 0.25 (compared with 1 microgram/ml for ciprofloxacin and 2 micrograms/ml for ofloxacin). Strains producing beta-lactamase or that were vancomycin resistant or resistant to high-level gentamicin were not quinolone cross-resistant. The drugs were bactericidal and were unaffected by 50% human serum. Oral efficacies (in milligrams per kilogram of body weight for 50% protective doses) in lethal mouse infections with quinolone-susceptible strains were 4.3 to 24 for clinafloxacin, 7.2 to 39 for CI-990, 7.2 to 76 for PD 138312, and 41 to > 100 for ciprofloxacin; when the drugs were given subcutaneously, the order was similar and values ranged from 1.1 to 12.5. Clinafloxacin, CI-990, and PD 138312 may have therapeutic potential in systemic enterococcal infections in humans.

摘要

某些新型氟喹诺酮类药物对肠球菌具有高活性。对于粪肠球菌(n = 18),90%分离株被抑制时的最低抑菌浓度(MIC,单位为微克/毫升)如下:克林沙星,0.125;CI-990,0.5;以及PD 138312,0.25(相比之下,环丙沙星为1微克/毫升,氧氟沙星为2微克/毫升)。产生β-内酰胺酶、对万古霉素耐药或对高水平庆大霉素耐药的菌株对喹诺酮类药物不存在交叉耐药性。这些药物具有杀菌作用,且不受50%人血清的影响。在对喹诺酮类药物敏感菌株所致的致死性小鼠感染中,口服疗效(50%保护剂量时的毫克/千克体重):克林沙星为4.3至24,CI-990为7.2至39,PD 138312为7.2至76,环丙沙星为41至>100;当药物皮下给药时,顺序相似,数值范围为1.1至12.5。克林沙星、CI-990和PD 138312在人类全身性肠球菌感染中可能具有治疗潜力。

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