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全基因组功能分析揭示了驱动蛋白在疟原虫生活史的哺乳动物和蚊子阶段的关键作用。

Genome-wide functional analysis reveals key roles for kinesins in the mammalian and mosquito stages of the malaria parasite life cycle.

机构信息

University of Nottingham, School of Life Sciences, Nottingham, United Kingdom.

University of Geneva, Faculty of Medicine, Geneva, Switzerland.

出版信息

PLoS Biol. 2022 Jul 28;20(7):e3001704. doi: 10.1371/journal.pbio.3001704. eCollection 2022 Jul.

Abstract

Kinesins are microtubule (MT)-based motors important in cell division, motility, polarity, and intracellular transport in many eukaryotes. However, they are poorly studied in the divergent eukaryotic pathogens Plasmodium spp., the causative agents of malaria, which manifest atypical aspects of cell division and plasticity of morphology throughout the life cycle in both mammalian and mosquito hosts. Here, we describe a genome-wide screen of Plasmodium kinesins, revealing diverse subcellular locations and functions in spindle assembly, axoneme formation, and cell morphology. Surprisingly, only kinesin-13 is essential for growth in the mammalian host while the other 8 kinesins are required during the proliferative and invasive stages of parasite transmission through the mosquito vector. In-depth analyses of kinesin-13 and kinesin-20 revealed functions in MT dynamics during apical cell polarity formation, spindle assembly, and axoneme biogenesis. These findings help us to understand the importance of MT motors and may be exploited to discover new therapeutic interventions against malaria.

摘要

驱动蛋白是微管(MT)依赖性马达,在许多真核生物的细胞分裂、运动、极性和细胞内运输中起着重要作用。然而,在疟原虫等分化的真核病原体中,它们的研究甚少,疟原虫是疟疾的病原体,在哺乳动物和蚊子宿主的整个生命周期中表现出细胞分裂和形态可塑性的非典型方面。在这里,我们描述了一个对疟原虫驱动蛋白的全基因组筛选,揭示了它们在纺锤体组装、轴丝形成和细胞形态方面的多样化亚细胞定位和功能。令人惊讶的是,只有驱动蛋白-13 对在哺乳动物宿主中的生长是必需的,而其他 8 种驱动蛋白在疟原虫通过蚊子媒介传播的增殖和侵袭阶段是必需的。对驱动蛋白-13 和驱动蛋白-20 的深入分析揭示了它们在顶端细胞极性形成、纺锤体组装和轴丝发生过程中对 MT 动力学的作用。这些发现有助于我们理解 MT 马达的重要性,并可能被用来发现新的抗疟疾治疗干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6040/9333250/bec07d94df0e/pbio.3001704.g001.jpg

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