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BMY-28142对大肠杆菌和B组链球菌所致实验性菌血症和脑膜炎的疗效

Efficacy of BMY-28142 in experimental bacteremia and meningitis caused by Escherichia coli and group B streptococci.

作者信息

Kim K S, Bayer A S

出版信息

Antimicrob Agents Chemother. 1985 Jul;28(1):51-4. doi: 10.1128/AAC.28.1.51.

Abstract

We evaluated the activity of BMY-28142 against a K1 E. coli strain and a type III group B streptococcal strain in vitro and in vivo and compared the results with those of cefotaxime and penicillin G, respectively. In vitro, the MICs and MBCs of BMY-28142 were close to those of cefotaxime (less than or equal to 2-fold difference) for E. coli and fourfold less than those of penicillin G for group B streptococci. In vivo studies with an experimental bacteremia and meningitis model in newborn rats revealed that the mean penetration of BMY-28142 into the cerebrospinal fluid was 15% that of concomitant levels in serum and that significantly greater bactericidal titers were achieved in blood and cerebrospinal fluid for both test organisms with BMY-28142 than with cefotaxime and penicillin G. However, the overall efficacy of BMY-28142 was similar to that of cefotaxime for the E. coli infection and that of penicillin G for the group B streptococcal infection. This was shown by similar rates of bacterial clearance from blood and cerebrospinal fluid and similar mortality rates. These findings indicate that the activity of BMY-28142 is bactericidal in vitro and in vivo against E. coli and group B streptococci, suggesting that this agent may be a suitable alternative for the therapy of E. coli and group B streptococcal bacteremia and meningitis.

摘要

我们在体外和体内评估了BMY-28142对一株K1大肠杆菌菌株和一株III型B组链球菌菌株的活性,并分别将结果与头孢噻肟和青霉素G的结果进行了比较。在体外,BMY-28142对大肠杆菌的MIC和MBC与头孢噻肟相近(差异小于或等于2倍),对B组链球菌的MIC和MBC比青霉素G低四倍。在新生大鼠的实验性菌血症和脑膜炎模型的体内研究中发现,BMY-28142进入脑脊液的平均渗透率是血清中相应水平的15%,并且对于两种受试微生物,BMY-28142在血液和脑脊液中达到的杀菌效价比头孢噻肟和青霉素G显著更高。然而,BMY-28142对大肠杆菌感染的总体疗效与头孢噻肟相似,对B组链球菌感染的总体疗效与青霉素G相似。这通过血液和脑脊液中细菌清除率相似以及死亡率相似得以体现。这些发现表明,BMY-28142在体外和体内对大肠杆菌和B组链球菌具有杀菌活性,提示该药物可能是治疗大肠杆菌和B组链球菌菌血症及脑膜炎的合适替代药物。

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