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Extracellular vesicles shed by Trypanosoma cruzi are linked to small RNA pathways, life cycle regulation, and susceptibility to infection of mammalian cells

机译:克鲁斯氏锥虫脱落的细胞外囊泡与小RNA途径,生命周期调控以及对哺乳动物细胞感染的敏感性有关

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The protozoan parasite Trypanosoma cruzi has a complex life cycle characterized by intracellular and extracellular forms alternating between invertebrate and mammals. To cope with these changing environments, T. cruzi undergoes rapid changes in gene expression, which are achieved essentially at the posttranscriptional level. At present, expanding families of small RNAs are recognized as key players in novel forms of posttranscriptional gene regulation in most eukaryotes. However, T. cruzi lacks canonical small RNA pathways. In a recent work, we reported the presence of alternate small RNA pathways in T. cruzi mainly represented by a homogeneous population of tRNA-derived small RNAs (tsRNAs). In T. cruzi epimastigotes submitted to nutrient starvation, tsRNAs colocalized with an argonaute protein distinctive of trypanosomatids (TcPIWI-tryp) and were recruited to particular cytoplasmic granules. Using epifluorescence and electronic microscopy, we observed that tsRNAs and the TcPIWI-tryp protein were recruited mainly to reservosomes and other intracellular vesicles including endosome-like vesicles and vesicular structures resembling the Golgi complex. These data suggested that, in T. cruzi, tsRNA biogenesis is probably part of endocytic/exocytic routes. We also demonstrated that epimastigotes submitted to nutrient starvation shed high levels of vesicles to the extracellular medium, which carry small tRNAs and TcPIWI-tryp proteins as cargo. At least a fraction of extracellular vesicle cargo was transferred between parasites and to mammalian susceptible cells. Our data afford experimental evidence, indicating that extracellular vesicles shed by T. cruzi promote not only life cycle transition of epimastigotes to trypomastigote forms but also infection susceptibility of mammalian cells
机译:原生动物寄生虫克氏锥虫具有复杂的生命周期,其特征在于无脊椎动物和哺乳动物之间交替的细胞内和细胞外形式。为了应对这些不断变化的环境,克鲁斯锥虫的基因表达发生了快速变化,这基本上是在转录后水平实现的。目前,在大多数真核生物中,扩大的小RNA家族被认为是转录后基因调控新形式的关键参与者。但是,克鲁氏锥虫缺乏规范的小RNA途径。在最近的工作中,我们报道了在克鲁氏锥虫中存在交替的小RNA途径,主要由同种的tRNA衍生的小RNA(tsRNA)组成。在提交给营养缺乏症的克鲁斯锥鞭毛虫中,tsRNA与锥虫的特异精子(TcPIWI-tryp)共定位,并被募集到特定的细胞质颗粒中。使用落射荧光和电子显微镜,我们观察到tsRNA和TcPIWI-tryp蛋白主要被募集到储库和其他细胞内囊泡,包括内体样囊泡和类似于高尔基体的囊泡结构。这些数据表明,在克鲁氏锥虫中,tsRNA生物发生可能是内吞/外切途径的一部分。我们还证明,提交给营养饥饿的淫羊tig科动物将高水平的囊泡流到细胞外培养基中,这些细胞携带着小的tRNA和TcPIWI-tryp蛋白作为货物。至少一部分细胞外囊泡货物在寄生虫之间转移至哺乳动物易感细胞。我们的数据提供了实验证据,表明克鲁氏梭菌脱落的细胞外囊泡不仅促进了表鞭毛虫向锥鞭毛虫形式的生命周期转变,而且还促进了哺乳动物细胞的感染敏感性

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