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In silico analysis of calcium binding pocket of perforin like protein 1: insights into the regulation of pore formation

机译:在计算机模拟中分析穿孔素样蛋白的钙结合口袋1:洞察孔形成的调节

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摘要

Plasmodium falciparum perforin like proteins (PfPLPs) are an important arsenal for the entry and exit of malaria parasites. These proteins bind and oligomerize on the membrane in calcium dependent manner and form an open pore. The calcium dependent pore forming activity of PLPs is usually conferred by their C2 like C-terminal domain. Here, we have tried to elucidate the calcium binding residues in the C-terminal domain of PfPLPl, a member of P. falciparum PLPs, playing a crucial role in calcium dependent egress of blood stage parasites. Through our in silico study, we have found that the C-terminal domain of all PfPLPs is rich in (3-pleated sheets and is structurally similar to C2 domain of human perforin. Furthermore, homology search based on 3-D structure of PfPLPl confirmed that it is structurally homologous to the calcium binding C2 domain of many proteins. On further elucidation of the calcium-binding pocket of the C2 like domain of PfPLPl showed that it binds to two calcium molecules. The calcium-binding pocket could be a target of novel chemotherapeutics for studying functional role of PfPLPs in parasite biology as well as for limiting blood stage growth of malaria parasite.
机译:恶性疟原虫穿孔素样蛋白(PfPLP)是疟疾寄生虫进入和退出的重要武器库。这些蛋白质以钙依赖性方式结合并寡聚在膜上并形成开孔。 PLP的钙依赖性孔形成活性通常由其C2样C末端结构域赋予。在这里,我们试图阐明恶性疟原虫PLP成员PfPLP1 C末端结构域中的钙结合残基,在血钙期寄生虫的钙依赖性出口中起关键作用。通过我们的计算机研究,我们发现所有PfPLP的C末端结构域都富含(3折叠的薄片,在结构上类似于人穿孔素的C2结构域。此外,基于PfPLP1的3-D结构进行的同源性搜索得到证实它在结构上与许多蛋白质的钙结合C2结构域同源。进一步阐明PfPLP1的C2样结构域的钙结合口袋表明它与两个钙分子结合。用于研究PfPLP在寄生虫生物学中的功能以及限制疟原虫血液阶段生长的新型化学疗法。

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