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疟原虫基因组在红细胞周期中的三维建模揭示了基因组结构与基因表达之间的紧密联系。

Three-dimensional modeling of the P. falciparum genome during the erythrocytic cycle reveals a strong connection between genome architecture and gene expression.

机构信息

Department of Genome Sciences, University of Washington, Seattle, Washington 98195, USA;

Department of Cell Biology and Neuroscience, University of California, Riverside, California 92521, USA;

出版信息

Genome Res. 2014 Jun;24(6):974-88. doi: 10.1101/gr.169417.113. Epub 2014 Mar 26.

Abstract

The development of the human malaria parasite Plasmodium falciparum is controlled by coordinated changes in gene expression throughout its complex life cycle, but the corresponding regulatory mechanisms are incompletely understood. To study the relationship between genome architecture and gene regulation in Plasmodium, we assayed the genome architecture of P. falciparum at three time points during its erythrocytic (asexual) cycle. Using chromosome conformation capture coupled with next-generation sequencing technology (Hi-C), we obtained high-resolution chromosomal contact maps, which we then used to construct a consensus three-dimensional genome structure for each time point. We observed strong clustering of centromeres, telomeres, ribosomal DNA, and virulence genes, resulting in a complex architecture that cannot be explained by a simple volume exclusion model. Internal virulence gene clusters exhibit domain-like structures in contact maps, suggesting that they play an important role in the genome architecture. Midway during the erythrocytic cycle, at the highly transcriptionally active trophozoite stage, the genome adopts a more open chromatin structure with increased chromosomal intermingling. In addition, we observed reduced expression of genes located in spatial proximity to the repressive subtelomeric center, and colocalization of distinct groups of parasite-specific genes with coordinated expression profiles. Overall, our results are indicative of a strong association between the P. falciparum spatial genome organization and gene expression. Understanding the molecular processes involved in genome conformation dynamics could contribute to the discovery of novel antimalarial strategies.

摘要

人类疟疾寄生虫疟原虫(Plasmodium falciparum)的发育受到其复杂生命周期中基因表达的协调变化的控制,但相应的调节机制尚不完全清楚。为了研究疟原虫的基因组结构与基因调控之间的关系,我们在其红细胞(无性)周期的三个时间点检测了疟原虫的基因组结构。我们使用染色体构象捕获与下一代测序技术(Hi-C),获得了高分辨率的染色体接触图谱,然后利用这些图谱构建了每个时间点的共识三维基因组结构。我们观察到着丝粒、端粒、核糖体 DNA 和毒力基因强烈聚集,导致了一种复杂的结构,无法用简单的体积排除模型来解释。内部毒力基因簇在接触图谱中表现出类似结构域的结构,表明它们在基因组结构中起着重要作用。在红细胞周期的中途,即高度转录活跃的滋养体阶段,基因组呈现出更开放的染色质结构,染色体之间的混杂增加。此外,我们观察到位于抑制性端粒中心附近的基因表达降低,以及不同的寄生虫特异性基因群与协调表达谱的共定位。总的来说,我们的结果表明疟原虫的空间基因组组织与基因表达之间存在很强的关联。了解涉及基因组构象动力学的分子过程可能有助于发现新的抗疟策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f305/4032861/a0a13294c0d4/974fig1.jpg

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