Protozoan parasites represent major public health challenges. Many aspects of their cell biology are distinct from their animal hosts, providing potential therapeutic targets. Toxoplasma gondii is a protozoan parasite that contains a divergent regulator of chromosome condensation 1 (TgRCC1) that is required for virulence and efficient nuclear trafficking. RCC1 proteins function as a guanine exchange factor for Ras-related nuclear protein (Ran), an abundant GTPase responsible for the majority of nucleocytoplasmic transport. Here we show that while there are dramatic differences from well-conserved RCC1 proteins, TgRCC1 associates with chromatin, interacts with Ran and complements a mammalian temperature-sensitive RCC1 mutant cell line. During the investigation of TgRCC1, we observed several unprecedented phenotypes for TgRan, despite a high level of sequence conservation. The cellular distribution of TgRan is found throughout the parasite cell, whereas Ran in late branching eukaryotes is predominantly nuclear. Additionally, T. gondii tolerates at least low-level expression of dominant lethal Ran mutants. Wild type parasites expressing dominant negative TgRan grew similarly to wild type in standard tissue culture conditions, but were attenuated in serum-starved host cells and mice. These growth characteristics paralleled the TgRCC1 mutant and highlight the importance of the nuclear transport pathway for virulence of eukaryotic pathogens.

译文

原生动物寄生虫是主要的公共卫生挑战。他们的细胞生物学的许多方面与他们的动物宿主不同,提供了潜在的治疗靶标。弓形虫是一种原生动物寄生虫,含有一种不同的染色体凝聚调节剂1 (TgRCC1),这是毒力和有效核贩运所必需的。RCC1蛋白是Ras相关核蛋白 (Ran) 的鸟嘌呤交换因子,Ras相关核蛋白是一种丰富的GTPase,负责大部分核质转运。在这里,我们表明,尽管保守的RCC1蛋白存在显着差异,但TgRCC1与染色质缔合,与Ran相互作用并补充哺乳动物温度敏感的RCC1突变细胞系。在TgRCC1的研究过程中,尽管序列保守性很高,但我们观察到了TgRan的几种前所未有的表型。在整个寄生虫细胞中发现了TgRan的细胞分布,而在晚期分支真核生物中Ran主要是核的。此外,弓形虫至少可以耐受显性致死Ran突变体的低水平表达。在标准组织培养条件下,表达显性负TgRan的野生型寄生虫的生长与野生型相似,但在血清饥饿的宿主细胞和小鼠中减弱。这些生长特征与TgRCC1突变体平行,并强调了核转运途径对真核病原体毒力的重要性。

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