化学和热抑制蛋白分泌对体外恶性疟原虫红细胞内发育具有阶段性特异性作用。

J Benting, I Ansorge, K Paprotka, K R Lingelbach
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引用次数: 0

摘要

人疟原虫恶性疟原虫的红细胞内阶段可引起宿主红细胞的多种生理变化。许多蛋白质由寄生虫分泌,随后在宿主细胞内的特定位置被发现。为了阐明蛋白质分泌对寄生虫存活的重要性,研究人员将被感染的红细胞(IRBC)置于真菌代谢物brefeldin A (BFA)和15℃的孵育下,这些处理抑制了蛋白质分泌和寄生虫的发育。有证据表明,BFA存在的寄生虫发育迟缓与蛋白质分泌的抑制有关。15摄氏度的孵育和BFA在环阶段可逆地阻止寄生虫的发育。在用BFA处理1.5天后,在15℃下处理约4天后,冻结环阶段失去50%发育为滋养体的能力。BFA影响滋养体发育的浓度与冻结环所需的浓度相似。与环相比,滋养体在15℃或BFA存在下的活力在24小时内完全消失。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Chemical and thermal inhibition of protein secretion have stage specific effects on the intraerythrocytic development of Plasmodium falciparum in vitro.

The intraerythrocytic stages of the human malaria parasite Plasmodium falciparum induce a variety of physiological changes of the host erythrocyte. Many proteins are secreted from the parasite and are subsequently found at specific locations within the host cell. To elucidate the importance of protein secretion for parasite survival, infected red blood cells (IRBC) were subjected to the fungal metabolite brefeldin A (BFA) and to incubation at 15 degrees C, treatments that inhibit protein secretion and parasite development. Evidence is provided that retardation of parasite development in the presence of BFA correlates with an inhibition of protein secretion. Incubation at 15 degrees C and BFA reversibly arrest parasite development at the ring stage. Arrested ring stages loose 50% of their competence to develop to trophozoites after 1.5 days of treatment with BFA and after approximately 4 days at 15 degrees C. BFA affects development of trophozoites at concentrations similar to those required to arrest rings. In contrast to rings, the viability of trophozoites cultured at 15 degrees C or in the presence of BFA is completely abolished within 24 h.

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