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首页> 外文期刊>Cellular microbiology >RON12, a novel Plasmodium-specific rhoptry neck protein important for parasite proliferation
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RON12, a novel Plasmodium-specific rhoptry neck protein important for parasite proliferation

机译:RON12,一种新的针对疟原虫的疟原虫特异性疟原虫特异性颈突蛋白

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摘要

Apicomplexan parasites invade host cells by a conserved mechanism:parasite proteins are secreted from apical organelles, anchored in the host cell plasma membrane, and then interact with integral membrane proteins on the zoite surface to form the moving junction (MJ). The junction moves from the anterior to the posterior of the parasite resulting in parasite internalization into the host cell within a parasitophorous vacuole (PV). Conserved as well as coccidia-unique rhoptry neck proteins (RONs) have been described, some of which associate with the MJ. Here we report a novel RON, which we call RON12. RON12 is found only in Plasmodium and is highly conserved across the genus. RON12 lacks a membrane anchor and is a major soluble component of the nascent PV. The bulk of RON12 secretion happens late during invasion (after parasite internalization) allowing accumulation in the fully formed PV with a small proportion of RON12 also apparent occasionally in structures resembling the MJ. RON12, unlike most other RONs is not essential, but deletion of the gene does affect parasite proliferation. The data suggest that although the overall mechanism of invasion by Apicomplexan parasites is conserved, additional components depending on the parasite-host cell combination are required.
机译:顶叶复合体寄生虫以保守的机制侵入宿主细胞:寄生蛋白从顶端细胞器中分泌出来,锚定在宿主细胞质膜中,然后与动物分子表面的整合膜蛋白相互作用,形成活动连接(MJ)。该连接从寄生虫的前部移动到后部,导致寄生虫内化进入寄生虫液泡(PV)内的宿主细胞。已经描述了保守的以及球菌独特的变态颈蛋白(RON),其中一些与MJ有关。在这里,我们报告一种新颖的RON,我们称之为RON12。 RON12仅在疟原虫中发现,并且在整个属中高度保守。 RON12没有膜锚,是新生PV的主要可溶性成分。 RON12的大部分分泌发生在入侵后期(寄生虫内在化之后),从而允许在完全形成的PV中积聚,其中少量RON12也偶尔出现在类似于MJ的结构中。与大多数其他RON不同,RON12不是必需的,但该基因的缺失确实会影响寄生虫的增殖。数据表明,尽管保守了顶复体寄生虫入侵的总体机制,但仍需要依赖于寄生虫-宿主细胞组合的其他成分。

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