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Functional Analysis of Protein Kinase CK2 of the Human Malaria Parasite Plasmodium falciparum

机译:人疟原虫恶性疟原虫蛋白激酶CK2的功能分析

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摘要

Protein kinase CK2 (casein kinase 2) is a eukaryotic serine/threonine protein kinase with multiple substrates and roles in diverse cellular processes, including differentiation, proliferation, and translation. The mammalian holoenzyme consists of two catalytic alpha or alpha′ subunits and two regulatory beta subunits. We report the identification and characterization of a Plasmodium falciparum CK2α orthologue, PfCK2α, and two PfCK2β orthologues, PfCK2β1 and PfCK2β2. Recombinant PfCK2α possesses protein kinase activity, exhibits similar substrate and cosubstrate preferences to those of CK2α subunits from other organisms, and interacts with both of the PfCK2β subunits in vitro. Gene disruption experiments show that the presence of PfCK2α is crucial to asexual blood stage parasites and thereby validate the enzyme as a possible drug target. PfCK2α is amenable to inhibitor screening, and we report differential susceptibility between the human and P. falciparum CK2α enzymes to a small molecule inhibitor. Taken together, our data identify PfCK2α as a potential target for antimalarial chemotherapeutic intervention.
机译:蛋白激酶CK2(酪蛋白激酶2)是一种真核生物丝氨酸/苏氨酸蛋白激酶,具有多种底物,并在多种细胞过程中起作用,包括分化,增殖和翻译。哺乳动物全酶由两个催化性α或α'亚基和两个调节性β亚基组成。我们报告鉴定和特征的恶性疟原虫CK2α直向同源物,PfCK2α,和两个PfCK2β直向同源物,PfCK2β1和PfCK2β2。重组PfCK2α具有蛋白激酶活性,与来自其他生物体的CK2α亚基表现出相似的底物和共底物偏好,并且在体外与两个PfCK2β亚基相互作用。基因破坏实验表明,PfCK2α的存在对无性血液阶段寄生虫至关重要,因此可以验证该酶是否可能成为药物靶标。 PfCK2α适用于抑制剂筛选,我们报道了人和恶性疟原虫CK2α酶对小分子抑制剂的敏感性不同。两者合计,我们的数据确定PfCK2α为抗疟疾化学治疗干预的潜在目标。

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