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阿奇霉素对小鼠IV型B族链球菌引起的全身感染和脓毒性关节炎的体内疗效:与红霉素和青霉素G的比较研究

In vivo efficacy of azithromycin in treatment of systemic infection and septic arthritis induced by type IV group B Streptococcus strains in mice: comparative study with erythromycin and penicillin G.

作者信息

Tissi L, von Hunolstein C, Mosci P, Campanelli C, Bistoni F, Orefici G

机构信息

Department of Experimental Medicine and Biochemical Sciences, University of Perugia, Italy.

出版信息

Antimicrob Agents Chemother. 1995 Sep;39(9):1938-47. doi: 10.1128/AAC.39.9.1938.

Abstract

We compared the activities of azithromycin, erythromycin, and penicillin G in a mouse model of systemic infection and septic arthritis induced by type IV group B streptococci (GBS). The in vitro and in vivo efficacy data for these drugs were analyzed relative to the pharmacokinetics of the drugs in sera, joints, and kidneys. Adult CD-1 mice were infected intravenously with 10(7) CFU of type IV GBS. Intraperitoneal drug administration was initiated with different dose regimens at different times after infection. A single dose of azithromycin (100 mg/kg) strongly reduced the incidence of articular lesions with respect to that with erythromycin or penicillin G. Treatment with azithromycin (three intraperitoneal administrations of 50 mg/kg at 12-h intervals) resulted in the complete prevention of arthritis. In contrast, erythromycin was poorly effective and penicillin G was effective only if inoculated 30 min after infection and at high doses (400,000 or 600,000 IU/kg). Furthermore, azithromycin was able to cure about 70% of the mice when administered 7, 8, and 9 days after GBS infection. Azithromycin was much more active than erythromycin and penicillin G with respect to bacterial killing in the joints and kidneys. In fact, cultures from these tissues were always negative no matter what treatment schedule was employed. The pharmacokinetics of azithromycin account for its superior in vivo efficacy against type IV GBS. A longer half-life and higher levels of this drug in serum and tissues with respect to those for erythromycin or penicillin G were achieved. The high affinity of azithromycin for the joints strongly supports its potential value for therapy of septic arthritis, which is a severe and frequent clinical manifestation of GBS infection.

摘要

我们在由IV型B组链球菌(GBS)引起的全身感染和脓毒性关节炎小鼠模型中比较了阿奇霉素、红霉素和青霉素G的活性。相对于这些药物在血清、关节和肾脏中的药代动力学,分析了这些药物的体外和体内疗效数据。成年CD-1小鼠静脉注射10(7) CFU的IV型GBS。在感染后的不同时间以不同剂量方案开始腹腔内给药。单剂量阿奇霉素(100 mg/kg)相对于红霉素或青霉素G,能显著降低关节病变的发生率。阿奇霉素治疗(每隔12小时腹腔内给药3次,每次50 mg/kg)可完全预防关节炎。相比之下,红霉素效果不佳,青霉素G仅在感染后30分钟接种且高剂量(400,000或600,000 IU/kg)时才有效。此外,在GBS感染后7、8和9天给予阿奇霉素,能够治愈约70%的小鼠。在关节和肾脏中,阿奇霉素在杀灭细菌方面比红霉素和青霉素G活性更强。事实上,无论采用何种治疗方案,这些组织的培养物始终为阴性。阿奇霉素的药代动力学解释了其对IV型GBS的体内疗效更优。与红霉素或青霉素G相比,该药物在血清和组织中的半衰期更长、水平更高。阿奇霉素对关节的高亲和力有力地支持了其在治疗脓毒性关节炎方面的潜在价值,脓毒性关节炎是GBS感染的一种严重且常见的临床表现。

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