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Injectable anti-malarials revisited: discovery and development of new agents to protect against malaria

机译:再次探讨可注射的抗疟药:发现和开发预防疟疾的新药物

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Abstract Over the last 15?years, the majority of malaria drug discovery and development efforts have focused on new molecules and regimens to treat patients with uncomplicated or severe disease. In addition, a number of new molecular scaffolds have been discovered which block the replication of the parasite in the liver, offering the possibility of new tools for oral prophylaxis or chemoprotection, potentially with once-weekly dosing. However, an intervention which requires less frequent administration than this would be a key tool for the control and elimination of malaria. Recent progress in HIV drug discovery has shown that small molecules can be formulated for injections as native molecules or pro-drugs which provide protection for at least 2?months. Advances in antibody engineering offer an alternative approach whereby a single injection could potentially provide protection for several months. Building on earlier profiles for uncomplicated and severe malaria, a target product profile is proposed here for an injectable medicine providing long-term protection from this disease. As with all of such profiles, factors such as efficacy, cost, safety and tolerability are key, but with the changing disease landscape in Africa, new clinical and regulatory approaches are required to develop prophylactic/chemoprotective medicines. An overall framework for these approaches is suggested here.
机译:摘要在过去的15年中,大多数疟疾药物的发现和开发工作都集中在新的分子和方案上,以治疗未发生复杂或严重疾病的患者。另外,已经发现了许多新的分子支架,它们阻断了寄生虫在肝脏中的复制,为口服预防或化学保护的新工具提供了可能,可能每周一次。但是,需要比这少频繁的干预将是控制和消除疟疾的关键工具。 HIV药物发现的最新进展表明,可以将小分子配制成天然分子或前药,以提供至少2个月的保护。抗体工程学的进步提供了一种替代方法,通过这种方法,单次注射可能可以提供数月的保护。基于较简单的关于严重并发症和严重疟疾的资料,在此提出了一种可注射药物的目标产品资料,该药可长期预防该病。与所有这些概况一样,诸如功效,成本,安全性和耐受性等因素是关键,但是随着非洲疾病形势的变化,开发预防/化学保护药物需要新的临床和管理方法。本文提出了这些方法的总体框架。

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