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咪康唑治疗球孢子菌病。II. 人体治疗与药理学研究

Miconazole in coccidiodomycosis. II. Therapeutic and pharmacologic studies in man.

作者信息

Stevens D A, Levine H B, Deresinski S C

出版信息

Am J Med. 1976 Feb;60(2):191-202. doi: 10.1016/0002-9343(76)90428-9.

Abstract

Fourteen patients with chronic coccidioidomycosis, many of whom had complicating concurrent diseases and/or had failed to respond to amphotericin therapy, were treated with intravenous miconazole, a synthetic imidazole drug previously shown to be effective in experimental murine coccidioidomycosis. Up to 3.6 g/day was given for up to three months. 7inimal inhibitory concentrations of mycelial and endospore phases of all clinical isolates of C. immitis were less than 2.0 mug/ml. Peak concentrations in the blood of up to 7.5 mug/ml (by assay against C. immitis in vitro) were achieved. Doses above 9 mg/kg or 350 mg/m2 were more efficacious in producing blood levels over 1 mug/ml. Serum protein binding, determined by several methods, was approximately 90 per cent. The disappearance of bioactive drug from blood after infusion has a rapid initial phase (t1/2 approximately 30 minutes) and a final plateau (t1/2 approximately 20 hours). Eight patients had objective evidence of response, three had slight or equivocal responses, two could not be evaluated, and one was a treatment failure. Side effects were generally uncommon, minor and transient except for phlebitis. Infusion into central venous catheters appears to circumvent this problem. Miconazole is a potentially useful drug in the treatment of coccidioidomycosis.

摘要

14例慢性球孢子菌病患者,其中许多人合并有其他疾病和/或对两性霉素治疗无反应,接受了静脉注射咪康唑治疗,咪康唑是一种合成咪唑类药物,此前已证明其在实验性小鼠球孢子菌病中有效。剂量高达每日3.6g,持续三个月。所有粗球孢子菌临床分离株的菌丝体和内生孢子期的最低抑菌浓度均低于2.0μg/ml。血液中的峰值浓度(通过体外针对粗球孢子菌的测定)达到7.5μg/ml。剂量高于9mg/kg或350mg/m2在产生超过1μg/ml的血药浓度方面更有效。通过几种方法测定的血清蛋白结合率约为90%。输注后生物活性药物从血液中的消失有一个快速的初始阶段(t1/2约为30分钟)和一个最终的平台期(t1/2约为20小时)。8例患者有客观的反应证据,3例有轻微或不明确的反应,2例无法评估,1例治疗失败。除静脉炎外,副作用一般不常见、轻微且短暂。通过中心静脉导管输注似乎可以避免这个问题。咪康唑在治疗球孢子菌病方面是一种潜在有用的药物。

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