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《间日疟原虫唾液腺子孢子转录组和组蛋白表观基因组揭示了在复发疟疾中紧密的调控控制和肝脏阶段分化的机制》

Transcriptome and histone epigenome of Plasmodium vivax salivary-gland sporozoites point to tight regulatory control and mechanisms for liver-stage differentiation in relapsing malaria.

出版信息

Int J Parasitol. 2019 Jun;49(7):501-513. doi: 10.1016/j.ijpara.2019.02.007. Epub 2019 May 7.

Abstract

Plasmodium vivax is the key obstacle to malaria elimination in Asia and Latin America, largely attributed to its ability to form resilient hypnozoites (sleeper cells) in the host liver that escape treatment and cause relapsing infections. The decision to form hypnozoites is made early in the liver infection and may already be set in sporozoites prior to invasion. To better understand these early stages of infection, we undertook a comprehensive transcriptomic and histone epigenetic characterization of P. vivax sporozoites. Through comparisons with recently published proteomic data for the P. vivax sporozoite, our study found that although highly transcribed, transcripts associated with functions needed for early infection of the vertebrate host are not detectable as proteins and may be regulated through translational repression. We identified differential transcription between the sporozoite and published transcriptomes of asexual blood stages and mixed versus hypnozoite-enriched liver stages. These comparisons point to multiple layers of transcriptional, post-transcriptional and post-translational control that appear active in sporozoites and to a lesser extent hypnozoites, but are largely absent in replicating liver schizonts or mixed blood stages. We also characterised histone epigenetic modifications in the P. vivax sporozoite and explored their role in regulating transcription. Collectively, these data support the hypothesis that the sporozoite is a tightly programmed stage to infect the human host and identify mechanisms for hypnozoite formation that may be further explored in liver stage models.

摘要

间日疟原虫是亚洲和拉丁美洲消除疟疾的主要障碍,这主要归因于它在宿主肝脏中形成具有弹性的休眠子(休眠细胞)的能力,这些休眠子能够逃避治疗并导致复发感染。形成休眠子的决定是在肝脏感染早期做出的,并且可能在入侵前就在子孢子中确定了。为了更好地理解感染的早期阶段,我们对间日疟原虫子孢子进行了全面的转录组学和组蛋白表观遗传特征分析。通过与最近发表的间日疟原虫子孢子蛋白质组数据进行比较,我们的研究发现,尽管转录水平很高,但与脊椎动物宿主早期感染相关的功能所需的转录本不能作为蛋白质检测到,并且可能通过翻译抑制来调节。我们发现子孢子与无性血期和混合期与休眠子富集期的已发表转录本之间存在差异转录。这些比较表明,在子孢子中存在多个转录、转录后和翻译后调控层,在休眠子中也存在一定程度的调控,但在复制的肝裂殖体或混合血期则基本不存在。我们还对间日疟原虫子孢子中的组蛋白表观遗传修饰进行了特征描述,并探讨了它们在调节转录中的作用。总的来说,这些数据支持了子孢子是一个紧密编程的阶段,可以感染人类宿主的假说,并确定了形成休眠子的机制,这些机制可能在肝期模型中进一步探索。

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