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一个交互式单细胞网络门户可识别新冠病毒宿主反应中的基因和细胞网络。

An interactive single cell web portal identifies gene and cell networks in COVID-19 host responses.

作者信息

Jin Kang, Bardes Eric E, Mitelpunkt Alexis, Wang Jake Y, Bhatnagar Surbhi, Sengupta Soma, Krummel Daniel Pomeranz, Rothenberg Marc E, Aronow Bruce J

机构信息

Division of Biomedical Informatics, Cincinnati Children's Hospital Medical Center, Cincinnati, OH 45229, USA.

Department of Biomedical Informatics, University of Cincinnati, Cincinnati, OH 45229, USA.

出版信息

iScience. 2021 Oct 22;24(10):103115. doi: 10.1016/j.isci.2021.103115. Epub 2021 Sep 10.

Abstract

Numerous studies have provided single-cell transcriptome profiles of host responses to SARS-CoV-2 infection. Critically lacking however is a data mine that allows users to compare and explore cell profiles to gain insights and develop new hypotheses. To accomplish this, we harmonized datasets from COVID-19 and other control condition blood, bronchoalveolar lavage, and tissue samples, and derived a compendium of gene signature modules per cell type, subtype, clinical condition, and compartment. We demonstrate approaches to interacting with, exploring, and functional evaluating these modules via a new interactive web portal ToppCell (http://toppcell.cchmc.org/). As examples, we develop three hypotheses: (1) alternatively-differentiated monocyte-derived macrophages form a multicelllar signaling cascade that drives T cell recruitment and activation; (2) COVID-19-generated platelet subtypes exhibit dramatically altered potential to adhere, coagulate, and thrombose; and (3) extrafollicular B maturation is driven by a multilineage cell activation network that expresses an ensemble of genes strongly associated with risk for developing post-viral autoimmunity.

摘要

众多研究提供了宿主对SARS-CoV-2感染反应的单细胞转录组图谱。然而,至关重要的是缺乏一个数据库,该数据库能让用户比较和探索细胞图谱,以获得见解并提出新的假设。为实现这一目标,我们整合了来自新冠肺炎及其他对照条件下的血液、支气管肺泡灌洗和组织样本的数据集,并针对每种细胞类型、亚型、临床状况和区室得出了基因特征模块的汇总。我们展示了通过一个新的交互式门户网站ToppCell(http://toppcell.cchmc.org/)与这些模块进行交互、探索和功能评估的方法。例如,我们提出了三个假设:(1)交替分化的单核细胞衍生巨噬细胞形成一个多细胞信号级联,驱动T细胞招募和激活;(2)新冠肺炎产生的血小板亚型在黏附、凝血和形成血栓方面表现出显著改变的潜能;(3)滤泡外B细胞成熟由一个多谱系细胞激活网络驱动,该网络表达一组与病毒后自身免疫发展风险密切相关的基因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/59c3/9698024/37eebfb59ede/fx1.jpg

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