In-Silico detection of chokepoints enzymes in four plasmodium species

S. Fatumo, Cs Yah
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引用次数: 4

Abstract

Of the over 156 species of Plasmodium that infect vertebrates, only four infect man: Plasmodium falciparum, Plasmodium vivax, Plasmodium ovale and Plasmodium malariae. Other species infect other animals including birds, reptiles and rodents. The rodent malaria parasites are Plasmodium berghei, Plasmodium yoelii, Plasmodium chabaudi and Plasmodium vinckei. Since research has shown a high similarity in sequence and properties between human and rodent, we sought to study the likely similar enzymatic pathways between the parasites that infect these two organisms that may be used as drug targets. The paper therefore, employed a computational biochemical approach to identify some choke points in the four selected species of Plasmodium: two (2) that infect humans and two (2) that infect rodents. These include- P. falciparum, P. vivax, P. berghei and P. chanbaudi respectively. In general, we identified an average of 178 chokepoint enzymes in these Plasmodium species which were common to all of them. Since there were several chokepoints enzymes common to all the species; we hypothesize that the chokepoints which are only common to a particular species could be possible drug targets to the individual parasites.
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四种疟原虫呛点酶的计算机检测
在感染脊椎动物的超过156种疟原虫中,只有4种会感染人类:恶性疟原虫、间日疟原虫、卵形疟原虫和疟疾疟原虫。其他物种会感染其他动物,包括鸟类、爬行动物和啮齿动物。啮齿动物的疟疾寄生虫有伯氏疟原虫、约氏疟原虫、沙氏疟原虫和长春疟原虫。由于研究表明人类和啮齿动物在序列和特性上高度相似,我们试图研究感染这两种生物的寄生虫之间可能相似的酶促途径,这些酶促途径可能用作药物靶点。因此,本文采用计算生化方法来确定四种选定的疟原虫的一些瓶颈:两种感染人类,两种感染啮齿动物。它们分别包括恶性疟原虫、间日疟原虫、伯氏疟原虫和昌伯氏疟原虫。总的来说,我们在这些疟原虫物种中平均鉴定出178种共同的瓶颈酶。由于存在一些所有物种共有的瓶颈酶;我们假设仅在特定物种中常见的阻塞点可能是单个寄生虫的可能药物靶点。
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