New Protein Settings to Support in vivo Antimalarial Activity in Plasmodium berghei Infected Mice after Garlic-Arteether Therapy

V. Govindan, P. K. Murthy
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Abstract

Many malaria endemic nations are pursuing malaria elimination and these technical challenges require the development of integrated approaches, among which safe and effective malaria vaccines could be a crucial tool.  Due to non-availability of malaria vaccine, the control efforts rely heavily on treatment with new antimalarial agents preferably acting on newer targets.  In this study, the protected serum proteomics after garlic and arteether combination treatment of P.berghei infected mice has been analyzed by western blotting. One of the identified host parasites specific proteins, peptidyl-prolyl-cis-trans isomerase A (PPIA) is known to catalyze the interconversion of the cis and trans and mediate certain protein folding events both in in vitro and in vivo conditions. This study hypothesizes that, overexpressed PPIA might lead to misfold of the parasite protein which are needed for parasite multiplication and in turn lead to the parasite death or in the protection of combination drug treated samples.
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在大蒜-青蒿素治疗后,支持伯氏疟原虫感染小鼠体内抗疟活性的新蛋白设置
许多疟疾流行国家正在努力消除疟疾,这些技术挑战要求制定综合办法,其中安全有效的疟疾疫苗可能是一个关键工具。由于没有疟疾疫苗,控制工作在很大程度上依赖于使用新的抗疟药进行治疗,最好是针对较新的目标。本研究采用western blotting方法分析了大蒜和蒿醚联合治疗伯氏螺旋体感染小鼠后血清保护蛋白组学的变化。作为宿主寄生虫的特异性蛋白之一,肽酰脯氨酸顺式反式异构酶A (PPIA)在体外和体内均可催化顺式和反式的相互转化,并介导某些蛋白质折叠事件。本研究推测,过表达的PPIA可能导致寄生虫繁殖所需的寄生虫蛋白错误折叠,从而导致寄生虫死亡或对联合药物处理的样品有保护作用。
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