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全身用抗真菌药。其临床药理学与治疗应用综述。

Systemically administered antifungal agents. A review of their clinical pharmacology and therapeutic applications.

作者信息

Lyman C A, Walsh T J

机构信息

Pediatric Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland.

出版信息

Drugs. 1992 Jul;44(1):9-35. doi: 10.2165/00003495-199244010-00002.

DOI:10.2165/00003495-199244010-00002
PMID:1379913
Abstract

Systemic antifungal agents express great diversity in their pharmacokinetic profiles, mechanisms of action, and toxicities. Understanding the diverse pharmacokinetic properties of systemic antifungals is critical to their appropriate application. Amphotericin B, drug of choice for most invasive mycoses, has unique pharmacokinetic properties, binding initially to serum lipoproteins and redistributing from blood to tissues. Dosing recommendations are based on the specific infection and the status of the host. Lipid formulations of amphotericin B may be able to attenuate some of its toxicities. Flucytosine is a water-soluble, fluorinated pyrimidine that possesses excellent bioavailability. It is administered only in combination with amphotericin B because of frequent development of secondary drug resistance, and is associated with dose-dependent bone marrow suppression. The antifungal azoles are relatively well tolerated, have broad spectrum antifungal activity, and are fungistatic in vitro. Ketoconazole and itraconazole are highly bound to plasma proteins, are extensively metabolised by the liver, and are relatively insoluble in aqueous solution. By comparison, fluconazole is only weakly bound to serum proteins, is relatively stable to metabolic conversion, and is water soluble. Fluconazole penetrates the cerebrospinal fluid well and is approved for primary and suppressive therapy of cryptococcal meningitis in AIDS patients. The echinocandins have a narrow spectrum of antifungal activity, being effective only against Candida spp.

摘要

全身性抗真菌药物在药代动力学特征、作用机制和毒性方面表现出极大的多样性。了解全身性抗真菌药物多样的药代动力学特性对于其合理应用至关重要。两性霉素B是大多数侵袭性真菌病的首选药物,具有独特的药代动力学特性,最初与血清脂蛋白结合,然后从血液重新分布到组织中。给药建议基于特定感染和宿主状态。两性霉素B的脂质制剂可能能够减轻其一些毒性。氟胞嘧啶是一种水溶性氟化嘧啶,具有出色的生物利用度。由于频繁出现继发性耐药,它仅与两性霉素B联合使用,并且与剂量依赖性骨髓抑制有关。抗真菌唑类药物耐受性相对较好,具有广谱抗真菌活性,在体外具有抑菌作用。酮康唑和伊曲康唑与血浆蛋白高度结合,在肝脏中广泛代谢,并且在水溶液中相对不溶。相比之下,氟康唑仅与血清蛋白弱结合,对代谢转化相对稳定,并且是水溶性的。氟康唑能很好地穿透脑脊液,被批准用于艾滋病患者隐球菌性脑膜炎的初始和抑制治疗。棘白菌素类抗真菌活性谱较窄,仅对念珠菌属有效。

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