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An upstream open reading frame (uORF) signals for cellular localization of the virulence factor implicated in pregnancy associated malaria

机译:上游开放阅读框(uORF)信号指示与妊娠相关的疟疾有关的毒力因子的细胞定位

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摘要

Plasmodium falciparum, the causative agent of the deadliest form of human malaria, alternates expression of variable antigens, encoded by members of a multi-copy gene family named var. In var2csa, the var gene implicated in pregnancy-associated malaria, translational repression is regulated by a unique upstream open reading frame (uORF) found only in its 5′ UTR. Here, we report that this translated uORF significantly alters both transcription and posttranslational protein trafficking. The parasite can alter a protein's destination without any modifications to the protein itself, but instead by an element within the 5′ UTR of the transcript. This uORF-dependent localization was confirmed by single molecule STORM imaging, followed by fusion of the uORF to a reporter gene which changes its cellular localization from cytoplasmic to ER-associated. These data point towards a novel regulatory role of uORF in protein trafficking, with important implications for the pathology of pregnancy-associated malaria.
机译:恶性疟原虫是人类疟疾最致命的病因,它交替表达可变抗原,可变抗原由多拷贝基因家族var编码。在var2csa(与怀孕相关的疟疾有关的var基因)中,翻译抑制受唯一在其5'UTR中发现的独特上游开放阅读框(uORF)调控。在这里,我们报告说,这种翻译的uORF会显着改变转录和翻译后蛋白质的运输。寄生虫可以改变蛋白质的目的地,而无需对蛋白质本身进行任何修饰,而是通过转录物的5'UTR中的一个元素。通过单分子STORM成像确认了uORF依赖的定位,然后将uORF与报告基因融合,从而将其细胞定位从胞质变为与ER相关。这些数据表明uORF在蛋白质运输中的新型调节作用,对与妊娠相关的疟疾的病理学具有重要意义。

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