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利用单细胞转录组学分析血腔型和前鞭毛体循环细胞周期。

Profiling the bloodstream form and procyclic form cell cycle using single-cell transcriptomics.

机构信息

Institute for Immunology and Infection Research, School of Biological Sciences, University of Edinburgh, Edinburgh, United Kingdom.

Wellcome Centre for Integrative Parasitology, School of Infection & Immunity, University of Glasgow, Glasgow, United Kingdom.

出版信息

Elife. 2023 May 11;12:e86325. doi: 10.7554/eLife.86325.

Abstract

African trypanosomes proliferate as bloodstream forms (BSFs) and procyclic forms in the mammal and tsetse fly midgut, respectively. This allows them to colonise the host environment upon infection and ensure life cycle progression. Yet, understanding of the mechanisms that regulate and drive the cell replication cycle of these forms is limited. Using single-cell transcriptomics on unsynchronised cell populations, we have obtained high resolution cell cycle regulated (CCR) transcriptomes of both procyclic and slender BSF without prior cell sorting or synchronisation. Additionally, we describe an efficient freeze-thawing protocol that allows single-cell transcriptomic analysis of cryopreserved . Computational reconstruction of the cell cycle using periodic pseudotime inference allowed the dynamic expression patterns of cycling genes to be profiled for both life cycle forms. Comparative analyses identify a core cycling transcriptome highly conserved between forms, as well as several genes where transcript levels dynamics are form specific. Comparing transcript expression patterns with protein abundance revealed that the majority of genes with periodic cycling transcript and protein levels exhibit a relative delay between peak transcript and protein expression. This work reveals novel detail of the CCR transcriptomes of both forms, which are available for further interrogation via an interactive webtool.

摘要

非洲锥虫分别以血液阶段(BSF)和前鞭毛体形式在哺乳动物和采采蝇的中肠中增殖。这使它们能够在感染时定植宿主环境并确保生命周期的进展。然而,对于调节和驱动这些形式的细胞复制周期的机制的理解是有限的。我们使用未同步细胞群体的单细胞转录组学,获得了未进行细胞分选或同步化的前鞭毛体和纤细 BSF 的高分辨率细胞周期调控(CCR)转录组。此外,我们描述了一种有效的冻融方案,允许对冷冻保存的 进行单细胞转录组分析。使用周期性拟时推断对细胞周期的计算重建允许对两种生命周期形式的循环基因的动态表达模式进行分析。比较分析确定了形式之间高度保守的核心循环转录组,以及几个转录水平动态具有形式特异性的基因。将转录表达模式与蛋白质丰度进行比较表明,具有周期性循环转录和蛋白质水平的大多数基因在峰值转录和蛋白质表达之间存在相对延迟。这项工作揭示了两种形式的 CCR 转录组的新细节,可通过交互式网络工具进一步探究。

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