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Plasmodium berghei MAPK1 displays differential and dynamic subcellular localizations during liver stage development

机译:伯氏疟原虫MAPK1在肝脏发育过程中显示差异和动态亚细胞定位

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摘要

Mitogen-activated protein kinases (MAPKs) regulate key signaling events in eukaryotic cells. In the genomes of protozoan Plasmodium parasites, the causative agents of malaria, two genes encoding kinases with significant homology to other eukaryotic MAPKs have been identified (mapk1, mapk2). In this work, we show that both genes are transcribed during Plasmodium berghei liver stage development, and analyze expression and subcellular localization of the PbMAPK1 protein in liver stage parasites. Live cell imaging of transgenic parasites expressing GFP-tagged PbMAPK1 revealed a nuclear localization of PbMAPK1 in the early schizont stage mediated by nuclear localization signals in the C-terminal domain. In contrast, a distinct localization of PbMAPK1 in comma/ring-shaped structures in proximity to the parasite's nuclei and the invaginating parasite membrane was observed during the cytomere stage of parasite development as well as in immature blood stage schizonts. The PbMAPK1 localization was found to be independent of integrity of a motif putatively involved in ATP binding, integrity of the putative activation motif and the presence of a predicted coiled-coil domain in the C-terminal domain. Although PbMAPK1 knock out parasites showed normal liver stage development, the kinase may still fulfill a dual function in both schizogony and merogony of liver stage parasites regulated by its dynamic and stage-dependent subcellular localization.
机译:丝裂原激活的蛋白激酶(MAPK)调节真核细胞中的关键信号事件。在疟疾的致病原虫疟原虫的基因组中,已经确定了两个编码与其他真核MAPKs具有显着同源性的激酶的基因(mapk1,mapk2)。在这项工作中,我们显示这两个基因在伯氏疟原虫肝阶段发育过程中均被转录,并分析了肝阶段寄生虫中PbMAPK1蛋白的表达和亚细胞定位。表达GFP标签的PbMAPK1的转基因寄生虫的活细胞成像显示,在裂殖体早期,PbMAPK1的核定位由C末端域的核定位信号介导。相比之下,PbMAPK1在寄生虫发育的细胞周期以及未成熟的裂殖体中,在靠近寄生虫细胞核和侵入性寄生虫膜的逗号/环形结构中有明显的定位。发现PbMAPK1的定位与假定参与ATP结合的基序的完整性,假定的激活基序的完整性以及C末端结构域中预测的卷曲螺旋结构域的存在无关。尽管PbMAPK1敲除寄生虫显示正常的肝阶段发育,但该激酶可能仍在肝阶段寄生虫的分裂和旋律中均具有双重功能,这取决于其动态和阶段依赖性亚细胞定位。

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