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如果它能转录,我们就能对其进行测序:利用RNA测序挖掘宿主-病原体-环境相互作用的复杂性。

If it transcribes, we can sequence it: mining the complexities of host-pathogen-environment interactions using RNA-seq.

作者信息

Colgan Aoife M, Cameron Andrew Ds, Kröger Carsten

机构信息

Department of Microbiology, School of Genetics and Microbiology, Moyne Institute of Preventive Medicine, Trinity College Dublin, Dublin, Ireland.

Department of Biology, University of Regina, Regina, Saskatchewan, Canada.

出版信息

Curr Opin Microbiol. 2017 Apr;36:37-46. doi: 10.1016/j.mib.2017.01.010. Epub 2017 Feb 10.

Abstract

Host-pathogen interactions are exceedingly complex because they involve multiple host tissues, often occur in the context of normal microflora, and can span diverse microenvironments. Although decades of gene expression studies have provided detailed insights into infection processes, technical challenges have restricted experiments to single pathogenic species or host tissues. RNA-sequencing (RNA-seq) has revolutionized the study of gene expression because in addition to quantifying transcriptional output, it allows detection and characterization of all transcripts in a genome. Here, we review how refined approaches to RNA-seq are used to map the transcriptional networks that control host-pathogen interactions. These enhanced techniques include dRNA-seq and term-seq for the fine-scale mapping of transcriptional start and termination sites, and dual RNA-seq for simultaneous sequencing of host and bacterial pathogen transcriptomes. Dual RNA-seq experiments are currently limited to in vitro infection systems that do not fully reflect the complexities of the in vivo environment, thus a challenge is to develop in vivo model systems and experimental approaches that address the biological heterogeneity of host environments, followed by the integration of RNA-seq with other genome-scale datasets to identify the transcriptional networks that mediate host-pathogen interactions.

摘要

宿主与病原体的相互作用极其复杂,因为它们涉及多个宿主组织,通常发生在正常微生物群落的背景下,并且可以跨越不同的微环境。尽管数十年来的基因表达研究为感染过程提供了详细的见解,但技术挑战限制了实验只能针对单一致病物种或宿主组织。RNA测序(RNA-seq)彻底改变了基因表达研究,因为除了量化转录输出外,它还能检测和表征基因组中的所有转录本。在这里,我们综述了如何利用RNA-seq的改进方法来绘制控制宿主与病原体相互作用的转录网络。这些增强技术包括用于转录起始和终止位点精细定位的dRNA-seq和term-seq,以及用于同时对宿主和细菌病原体转录组进行测序的双RNA-seq。双RNA-seq实验目前仅限于不能完全反映体内环境复杂性的体外感染系统,因此一个挑战是开发体内模型系统和实验方法,以解决宿主环境的生物异质性问题,随后将RNA-seq与其他基因组规模数据集整合,以识别介导宿主与病原体相互作用的转录网络。

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