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Targeting protein kinases in the malaria parasite: Update of an antimalarial drug target

机译:疟原虫中的靶向蛋白激酶:抗疟药物靶标的更新

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摘要

Millions of deaths each year are attributed to malaria worldwide. Transmitted through the bite of an Anopheles mosquito, infection and subsequent death from the Plasmodium species, most notably P. falciparum, can readily spread through a susceptible population. A malaria vaccine does not exist and resistance to virtually every antimalarial drug predicts that mortality and morbidity associated with this disease will increase. With only a few antimalarial drugs currently in the pipeline, new therapeutic options and novel chemotypes are desperately needed. Hit-to-Lead diversity may successfully provide novel inhibitory scaffolds when essential enzymes are targeted, for example, the plasmodial protein kinases. Throughout the entire life cycle of the malaria parasite, protein kinases are essential for growth and development. Ongoing efforts continue to characterize these kinases, while simultaneously pursuing them as antimalarial drug targets. A collection of structural data, inhibitory profiles and target validation has set the foundation and support for targeting the malarial kinome. Pursuing protein kinases as cancer drug targets has generated a wealth of information on the inhibitory strategies that can be useful for antimalarial drug discovery. In this review, progress on selected protein kinases is described. As the search for novel antimalarials continues, an understanding of the phosphor-regulatory pathways will not only validate protein kinase targets, but also will identify novel chemotypes to thwart malaria drug resistance.
机译:全世界每年都有数百万人死于疟疾。通过疟蚊的叮咬传播,疟原虫物种(尤其是恶性疟原虫)的感染和随后的死亡很容易在易感人群中传播。疟疾疫苗不存在,对每种抗疟疾药物的抗药性都表明与该疾病相关的死亡率和发病率将增加。当前只有少数几种抗疟药正在开发中,迫切需要新的治疗选择和新的化学型。当必需酶(例如血浆蛋白激酶)被靶向时,“命中率”多样性可能会成功地提供新型的抑制性支架。在疟原虫的整个生命周期中,蛋白激酶对于生长和发育至关重要。正在进行的工作继续表征这些激酶,同时将其作为抗疟药的目标。结构数据,抑制谱和靶标验证的收集为靶向疟疾激酶组奠定了基础和支持。追求蛋白激酶作为抗癌药物的靶标已产生了大量有关抑制策略的信息,这些信息可用于发现抗疟​​疾药物。在这篇综述中,描述了所选蛋白激酶的进展。随着对新型抗疟疾药物的搜寻不断,对磷光调节途径的理解不仅将验证蛋白激酶靶点,还将鉴定出新型化学型以阻止疟疾的耐药性。

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