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Proteases as antimalarial targets: strategies for genetic, chemical, and therapeutic validation

机译:蛋白酶作为抗疟疾靶标:遗传,化学和治疗验证的策略

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摘要

Malaria is a devastating parasitic disease affecting half of the world's population. The rapid emergence of resistance against new antimalarial drugs, including artemisinin-based therapies, has made the development of drugs with novel mechanisms of action extremely urgent. Proteases are enzymes proven to be well suited for target-based drug development due to our knowledge of their enzymatic mechanisms and active site structures. More importantly, Plasmodium proteases have been shown to be involved in a variety of pathways that are essential for parasite survival. However, pharmacological rather than target-based approaches have dominated the field of antimalarial drug development, in part due to the challenge of robustly validating Plasmodium targets at the genetic level. Fortunately, over the last few years there has been significant progress in the development of efficient genetic methods to modify the parasite, including several conditional approaches. This progress is finally allowing us not only to validate essential genes genetically, but also to study their molecular functions. In this review, I present our current understanding of the biological role proteases play in the malaria parasite life cycle. I also discuss how the recent advances in Plasmodium genetics, the improvement of protease-oriented chemical biology approaches, and the development of malaria-focused pharmacological assays, can be combined to achieve a robust biological, chemical and therapeutic validation of Plasmodium proteases as viable drug targets.
机译:疟疾是一种影响世界上一半人口的孕寄生疾病。对新的抗疟疾药物的抗性快速出现,包括蒿属素的疗法,使得具有新的行动机制极为紧急地发展毒品。由于我们对其酶促机制和有源部位结构的了解,蛋白酶被证明是非常适合于目标的药物开发。更重要的是,已显示疟原虫蛋白酶参与寄生物存活至关重要的各种途径。然而,药理而不是基于目标的方法已经主导了抗疟药领域,部分原因是由于遗传水平的挑战验证疟原虫靶标的挑战。幸运的是,在过去的几年里,在改变寄生虫的有效遗传方法的发展方面存在显着进展,包括几种条件方法。这一进步终于允许我们不仅验证基因上的基因,而且还研究其分子功能。在这篇综述中,我目前对生物学作用蛋白酶在疟疾寄生虫生命周期中发挥的理解。我还讨论了疟原虫遗传学中最近的进展,改善蛋白酶导向的化学生物学方法以及以疟疾为中心的药理学测定的发展,可以组合以实现疟原虫蛋白酶作为可行性药物的稳健生物学,化学和治疗验证目标。

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