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亚胺培南治疗实验性金黄色葡萄球菌和粪肠球菌心内膜炎

Imipenem therapy of experimental Staphylococcus aureus and Streptococcus faecalis endocarditis.

作者信息

Scheld W M, Keeley J M

出版信息

J Antimicrob Chemother. 1983 Dec;12 Suppl D:65-78. doi: 10.1093/jac/12.suppl_d.65.

Abstract

Imipenem was very active in vitro against 36 Staphylococcus aureus isolates from cases of infective endocarditis; the MBC90 was 0.06 mg/l (four- to eight-fold more active than nafcillin). The in-vitro activity of imipenem against 22 Streptococcus faecalis isolates from proven endocarditis cases was similar to that of penicillin G (MBC90 = 8 mg/l). Imipenem was compared with nafcillin and with penicillin plus gentamicin in the therapy of experimental endocarditis induced in rabbits by Staph. aureus and Str. faecalis, respectively. The dosages were chosen to simulate closely serum antibiotic concentrations found in humans receiving standard parenteral regimens. Imipenem was more rapidly bactericidal than nafcillin in experimental staphylococcal endocarditis. The mean +/- S.D. Staph. aureus concentrations within aortic valve vegetations (log10 cfu/g) after 5 days of therapy were as follows: imipenem = 1.39 +/- 0.61 versus nafcillin 2.39 +/- 0.36 (P less than 0.02). Both the imipenem and nafcillin regimens resulted in 'sterile' vegetations in congruent to 50% of rabbits with experimental staphylococcal endocarditis after 5 days of therapy (P greater than 0.05). Imipenem was also equivalent to penicillin plus gentamicin in the therapy of experimental enterococcal endocarditis for 5 days, as assessed by the mean cfu/g vegetation and the percentage of vegetations rendered sterile. However, 7 days of therapy cured experimental enterococcal endocarditis in 72% of rabbits receiving penicillin plus gentamicin versus 20% for imipenem alone (P less than 0.05). Imipenem deserves further evaluation in the therapy of infective endocarditis, both in experimental animal models of infection and in humans. This agent may prove useful in the therapy of staphylococcal endocarditis in a variety of difficult clinical situations. Therapy of enterococcal endocarditis with imipenem alone is not advisable, pending further data.

摘要

亚胺培南对36株来自感染性心内膜炎病例的金黄色葡萄球菌分离株在体外具有很强的活性;90%最低杀菌浓度(MBC90)为0.06mg/L(活性比萘夫西林高4至8倍)。亚胺培南对22株来自确诊心内膜炎病例的粪肠球菌分离株的体外活性与青霉素G相似(MBC90 = 8mg/L)。分别在由金黄色葡萄球菌和粪肠球菌诱导的兔实验性心内膜炎治疗中,将亚胺培南与萘夫西林以及青霉素加庆大霉素进行了比较。所选择的剂量旨在紧密模拟接受标准胃肠外给药方案的人类血清中的抗生素浓度。在实验性葡萄球菌心内膜炎中,亚胺培南比萘夫西林杀菌更快。治疗5天后主动脉瓣赘生物内金黄色葡萄球菌的平均±标准差浓度(log10 cfu/g)如下:亚胺培南 = 1.39 ± 0.61,而萘夫西林为2.39 ± 0.36(P < 0.02)。治疗5天后,亚胺培南和萘夫西林治疗方案在约50%的实验性葡萄球菌心内膜炎兔中均产生了“无菌”赘生物(P > 0.05)。根据赘生物的平均cfu/g以及变为无菌的赘生物百分比评估,在实验性肠球菌心内膜炎治疗5天时,亚胺培南也等同于青霉素加庆大霉素。然而,治疗7天时,接受青霉素加庆大霉素的兔中72%的实验性肠球菌心内膜炎被治愈,而单独使用亚胺培南的治愈率为20%(P < 0.05)。亚胺培南在感染性心内膜炎的治疗中,无论是在感染的实验动物模型还是在人类中,都值得进一步评估。这种药物在各种困难的临床情况下可能被证明对葡萄球菌心内膜炎的治疗有用。在获得更多数据之前,不建议单独使用亚胺培南治疗肠球菌心内膜炎。

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