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Malaria Parasite Survival Depends on Conserved Binding Peptides' Critical Biological Functions

机译:疟疾寄生虫的生存取决于保守的结合肽的关键生物学功能。

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Biochemical, structural and single amino acid level analysis of 49 Plasmodium falciparum protein regions (13 sporozoite and 36 merozoite proteins) has highlighted the functional role of each conserved high activity binding peptide (cHABP) in cell host-microbe interaction, involving biological functions such as gliding motility, traversal activity, binding invasion, reproduction, nutrient ion transport and the development of severe malaria. Each protein's key function in the malaria parasite's asexual lifecycle (pre-erythrocyte and erythro-cyte) is described in terms of cHABPs; their sequences were located in elegant work published by other groups regarding critical binding regions implicated in malarial parasite invasion. Such cHABPs represent the starting point for developing a logical and rational methodology for selecting an appropriate mixture of modified cHABPs to be used in a completely effective, synthetic antimalarial vaccine. Such methodology could be used for developing vaccines against diseases scourging humanity.
机译:对49个恶性疟原虫蛋白质区域(13个子孢子和36个裂殖子蛋白)的生化,结构和单氨基酸水平分析强调了每个保守的高活性结合肽(cHABP)在细胞宿主-微生物相互作用中的功能作用,包括诸如滑翔运动,穿越活动,结合入侵,繁殖,营养离子运输和严重疟疾的发展。每种蛋白质在疟原虫无性生活周期(红细胞前和红细胞)中的关键功能都用cHABPs来描述。它们的序列位于其他小组发表的关于疟疾寄生虫入侵所涉及的关键结合区的精美著作中。此类cHABPs是开发逻辑和合理方法的起点,该方法用于选择适当的修饰cHABPs混合物以用于完全有效的合成抗疟疾疫苗。这种方法可用于开发抗人类疾病的疫苗。

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