Desynchronizing Plasmodium Cell Cycle Increases Chloroquine Protection at Suboptimal Doses

P. Bagnaresi, R. Markus, C. T. Hotta, T. Pozzan, Celia R. S. Garcia
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引用次数: 14

Abstract

We have previously shown that in vivo and in vitro the hormone melatonin is responsible for the synchronous development of Plasmodia. Melatonin can also mobilize calcium from internal stores in these parasites and this response is abolished by luzindole, a melatonin antagonist. We here demonstrate that in vivo alteration of parasite synchronous de- velopment, using luzindole, partially improves survival of infected mice and dramatically increases the antimalarial ac- tivity of chloroquine. The data presented may lead to a conceptually new paradigm for malaria infection therapy and pro- vide novel evidence suggesting that the malaria parasite uses the cell cycle synchrony as one of the strategies to evade the host immune system.
不同步的疟原虫细胞周期在次优剂量下增加氯喹的保护作用
我们以前已经表明,体内和体外激素褪黑素负责疟原虫的同步发展。褪黑素还可以调动这些寄生虫体内储存的钙,而这种反应被褪黑素拮抗剂——卢津多尔所消除。我们在此证明,在体内改变寄生虫的同步发育,使用luzindole,部分改善感染小鼠的生存,并显着增加氯喹的抗疟活性。这些数据可能为疟疾感染治疗提供一个概念上的新范式,并提供新的证据,表明疟疾寄生虫利用细胞周期同步性作为逃避宿主免疫系统的策略之一。
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