新出现的抗真菌药物:对呼吸道感染的影响。

Marta Feldmesser
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引用次数: 4

摘要

真菌病原体是呼吸系统疾病日益重要的原因,但抗真菌药物的数量可用于临床使用是有限的。两性霉素B脱氧胆酸盐的使用受到严重毒性的阻碍。目前可用的三唑类药物具有显著的药物相互作用;氟康唑具有有限的活性谱,而伊曲康唑直到最近才在生物利用度有限的口服制剂中可用。人们越来越认识到对这三种药物的耐药性的发展,一些丝状真菌对所有这些药物的作用都有耐药性。在过去的几年中,新的抗真菌药物和现有药物的新配方已经出现。两性霉素B脂质体制剂的使用与肾毒性和输注相关反应的发生率降低有关,但仍然很大。介绍了一种伊曲康唑静脉制剂,并开发了几种新的三唑制剂,以期确定具有增强效力,更广泛的作用谱和改善的药效学特性的制剂。其中的伏立康唑已经完成了大规模的临床试验。此外,caspofungin是一类新型药物中的第一种,即抑制细胞壁葡聚糖合成的棘白菌素(echinocandins),于2001年在美国被批准用于治疗侵袭性曲霉病。希望这些药物的可用性将对真菌呼吸道感染的发病率和死亡率产生重大影响。然而,目前,我们评估其影响的能力受到进行抗真菌治疗试验的问题性质的限制。
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New and emerging antifungal agents: impact on respiratory infections.

Fungal pathogens are increasingly important causes of respiratory disease, yet the number of antifungal agents available for clinical use is limited. Use of amphotericin B deoxycholate is hampered by severe toxicity. Triazole agents currently available have significant drug interactions; fluconazole has a limited spectrum of activity and itraconazole was, until recently, available only in oral formulations with limited bioavailability. The development of resistance to all three agents is increasingly being recognized and some filamentous fungi are resistant to the action of all of these agents. In the past few years, new antifungal agents and new formulations of existing agents have become available.The use of liposomal amphotericin B preparations is associated with reduced, but still substantial, rates of nephrotoxicity and infusion-related reactions. An intravenous formulation of itraconazole has been introduced, and several new triazole agents have been developed, with the view of identifying agents that have enhanced potency, broader spectra of action and improved pharmacodynamic properties. One of these, voriconazole, has completed large-scale clinical trials. In addition, caspofungin, the first of a new class of agents, the echinocandins, which inhibit cell wall glucan synthesis, was approved for use in the US in 2001 as salvage therapy for invasive aspergillosis. It is hoped that the availability of these agents will have a significant impact on the morbidity and mortality of fungal respiratory infections. However, at the present time, our ability to assess their impact is limited by the problematic nature of conducting trials for antifungal therapy.

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