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转录组分析揭示代谢转换和表面重塑是……阶段转变的关键过程。 (注:原文中“in”后面似乎缺失了具体内容)

Transcriptomic analysis reveals metabolic switches and surface remodeling as key processes for stage transition in .

作者信息

Berná Luisa, Chiribao Maria Laura, Greif Gonzalo, Rodriguez Matias, Alvarez-Valin Fernando, Robello Carlos

机构信息

Unidad de Biología Molecular, Institut Pasteur de Montevideo, Montevideo, Uruguay.

Departamento de Bioquímica, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay.

出版信息

PeerJ. 2017 Mar 8;5:e3017. doi: 10.7717/peerj.3017. eCollection 2017.

Abstract

American trypanosomiasis is a chronic and endemic disease which affects millions of people. , its causative agent, has a life cycle that involves complex morphological and functional transitions, as well as a variety of environmental conditions. This requires a tight regulation of gene expression, which is achieved mainly by post-transcriptional regulation. In this work we conducted an RNAseq analysis of the three major life cycle stages of : amastigotes, epimastigotes and trypomastigotes. This analysis allowed us to delineate specific transcriptomic profiling for each stage, and also to identify those biological processes of major relevance in each state. Stage specific expression profiling evidenced the plasticity of to adapt quickly to different conditions, with particular focus on membrane remodeling and metabolic shifts along the life cycle. Epimastigotes, which replicate in the gut of insect vectors, showed higher expression of genes related to energy metabolism, mainly Krebs cycle, respiratory chain and oxidative phosphorylation related genes, and anabolism related genes associated to nucleotide and steroid biosynthesis; also, a general down-regulation of surface glycoprotein coding genes was seen at this stage. Trypomastigotes, living extracellularly in the bloodstream of mammals, express a plethora of surface proteins and signaling genes involved in invasion and evasion of immune response. Amastigotes mostly express membrane transporters and genes involved in regulation of cell cycle, and also express a specific subset of surface glycoprotein coding genes. In addition, these results allowed us to improve the annotation of the Dm28c genome, identifying new ORFs and set the stage for construction of networks of co-expression, which can give clues about coded proteins of unknown functions.

摘要

美洲锥虫病是一种影响数百万人的慢性地方病。其病原体具有一个涉及复杂形态和功能转变以及多种环境条件的生命周期。这需要对基因表达进行严格调控,而这主要通过转录后调控来实现。在这项工作中,我们对该病原体的三个主要生命周期阶段:无鞭毛体、前鞭毛体和锥鞭毛体进行了RNA测序分析。该分析使我们能够描绘每个阶段的特定转录组图谱,并识别每个状态下主要相关的生物学过程。阶段特异性表达谱证明了该病原体具有快速适应不同条件的可塑性,尤其关注整个生命周期中的膜重塑和代谢转变。在前鞭毛体阶段,它在昆虫媒介的肠道中进行复制,与能量代谢相关的基因表达较高,主要是与三羧酸循环、呼吸链和氧化磷酸化相关的基因,以及与核苷酸和类固醇生物合成相关的合成代谢基因;此外,在这个阶段还观察到表面糖蛋白编码基因普遍下调。锥鞭毛体生活在哺乳动物血液的细胞外,表达大量参与免疫反应侵袭和逃避的表面蛋白和信号基因。无鞭毛体主要表达膜转运蛋白和参与细胞周期调控的基因,也表达特定子集的表面糖蛋白编码基因。此外,这些结果使我们能够改进Dm28c基因组的注释,识别新的开放阅读框,并为构建共表达网络奠定基础,这可以为未知功能的编码蛋白提供线索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/471a/5345387/04955ad1b9b5/peerj-05-3017-g001.jpg

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