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解析猪圆环病毒 2 型的临床结果与宿主组织反应的体内衍生转录组特征。

Dissecting clinical outcome of porcine circovirus type 2 with in vivo derived transcriptomic signatures of host tissue responses.

机构信息

Laboratory of Virology, Faculty of Veterinary Medicine, Ghent University, Merelbeke, Belgium.

Ann Romney Center for Neurologic Diseases, Department of Neurology, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

BMC Genomics. 2018 Nov 20;19(1):831. doi: 10.1186/s12864-018-5217-5.

Abstract

BACKGROUND

Porcine Circovirus Type 2 (PCV2) is a pathogen that has the ability to cause often devastating disease manifestations in pig populations with major economic implications. How PCV2 establishes subclinical persistence and why certain individuals progress to lethal lymphoid depletion remain to be elucidated.

RESULTS

Here we present PorSignDB, a gene signature database describing in vivo porcine tissue physiology that we generated from a large compendium of in vivo transcriptional profiles and that we subsequently leveraged for deciphering the distinct physiological states underlying PCV2-affected lymph nodes. This systems genomics approach indicated that subclinical PCV2 infections suppress a myeloid leukocyte mediated immune response. However, in contrast an inflammatory myeloid cell activation is promoted in PCV2 patients with clinical manifestations. Functional genomics further uncovered STAT3 as a druggable PCV2 host factor candidate. Moreover, IL-2 supplementation of primary lymphocytes enabled ex vivo study of PCV2 replication in its target cell, the lymphoblast.

CONCLUSION

Our systematic dissection of the mechanistic basis of PCV2 reveals that subclinical and clinical PCV2 display two diametrically opposed immunotranscriptomic recalibrations that represent distinct physiological states in vivo, which suggests a paradigm shift in this field. Finally, our PorSignDB signature database is publicly available as a community resource ( http://www.vetvirology.ugent.be/PorSignDB/ , included in Gene Sets from Community Contributors http://software.broadinstitute.org/gsea/msigdb/contributed_genesets.jsp ) and provides systems biologists with a valuable tool for catalyzing studies of human and veterinary disease. Finally, a primary porcine lymphoblast cell culture system paves the way for unraveling the impact of host genetics on PCV2 replication.

摘要

背景

猪圆环病毒 2 型(PCV2)是一种病原体,能够在猪群中引起常毁灭性的疾病表现,对经济有重大影响。PCV2 如何建立亚临床持续性,以及为什么某些个体进展为致命的淋巴耗竭,仍有待阐明。

结果

这里我们介绍了 PorSignDB,这是一个基因特征数据库,描述了我们从大量体内转录谱综合数据中生成的体内猪组织生理学,我们随后利用该数据库来破译 PCV2 感染的淋巴结所潜在的不同生理状态。这种系统基因组学方法表明,亚临床 PCV2 感染抑制了骨髓白细胞介导的免疫反应。然而,相反的是,在有临床表现的 PCV2 患者中,炎症性骨髓细胞激活被促进。功能基因组学进一步揭示了 STAT3 作为一个可药物治疗的 PCV2 宿主因子候选物。此外,IL-2 补充原代淋巴细胞使 PCV2 在其靶细胞淋巴母细胞中的复制能够在体外进行研究。

结论

我们对 PCV2 机制基础的系统剖析表明,亚临床和临床 PCV2 显示出两种截然相反的免疫转录组重新校准,这代表了体内的不同生理状态,这表明该领域的范式转变。最后,我们的 PorSignDB 特征数据库作为一个公共资源(http://www.vetvirology.ugent.be/PorSignDB/,包含在社区贡献者基因集 http://software.broadinstitute.org/gsea/msigdb/contributed_genesets.jsp 中)可供系统生物学家使用,为他们研究人类和兽医疾病提供了有价值的工具。最后,一个原代猪淋巴母细胞培养系统为揭示宿主遗传对 PCV2 复制的影响铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e9a/6247532/5e763430e742/12864_2018_5217_Fig1_HTML.jpg

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