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Recent advances in development of amphotericin B formulations for the treatment of visceral leishmaniasis

机译:两性霉素B制剂治疗内脏利什曼病的最新进展

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PURPOSE OF REVIEW: Amphotericin B (AmpB) is considered the first-line treatment for visceral leishmaniasis in areas in which resistance to antimony is prevalent. This review describes recent advances in clinically available and novel drug delivery systems of AmpB to treat visceral leishmaniasis. RECENT FINDINGS: Over the past two decades, lipid-based AmpB formulations developed to tackle the toxicity of AmpB have been used clinically for the treatment of visceral leishmaniasis. Liposomal AmpB (AmBisome) has been the most successful lipid formulation, and recent clinical studies on visceral leishmaniasis have shown the potential of single-dose AmBisome treatment as well as its use in short course combinations with other antileishmanial drugs. Current research is focussed on the development of more stable and affordable nonlipid formulations of AmpB. Although a diverse range of nonlipid-based AmpB formulations have been evaluated, none have yet reached the clinic. SUMMARY: Liposomal AmpB (AmBisome) has become a standard treatment, by intravenous infusion, for visceral leishmaniasis and the basis for new short course treatments. There have been extensive efforts to develop new AmpB formulations on the basis of polymers, lipids or physical aggregates of AmpB to replace the costly lipid-based formulations. However, no nonlipid-based AmpB delivery systems have yet reached the clinic.
机译:审查目的:两性霉素B(AmpB)被认为是在对锑耐药的地区普遍存在的内脏利什曼病的一线治疗药物。这篇综述描述了可用于内脏利什曼病的AmpB的临床可用和新型药物递送系统的最新进展。最新发现:在过去的二十年中,为解决AmpB的毒性而开发的基于脂质的AmpB制剂已在临床上用于治疗内脏利什曼病。脂质体AmpB(AmBisome)是最成功的脂质制剂,最近关于内脏利什曼病的临床研究表明,单剂量AmBisome的治疗潜力以及与其他抗衰老药物短期组合使用的可能性。当前的研究集中在开发更稳定和负担得起的AmpB非脂质制剂。尽管已经评估了多种基于非脂质的AmpB制剂,但尚未进入临床。简介:脂质体AmpB(AmBisome)已通过静脉内输注成为内脏利什曼病的标准治疗方法,也是新的短期治疗方法的基础。在基于AmpB的聚合物,脂质或物理聚集体的基础上,已经进行了广泛的努力来开发新的AmpB制剂,以取代昂贵的基于脂质的制剂。但是,尚未有基于非脂质的AmpB递送系统进入临床。

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