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洞穴花蜜蝠(Eonycteris spelaea)对病毒感染体内反应的单细胞转录组分析。

Single-cell transcriptome analysis of the in vivo response to viral infection in the cave nectar bat Eonycteris spelaea.

作者信息

Gamage Akshamal M, Chan Wharton O Y, Zhu Feng, Lim Yan Ting, Long Sandy, Ahn Matae, Tan Chee Wah, Hiang Foo Randy Jee, Sia Wan Rong, Lim Xiao Fang, He Haopeng, Zhai Weiwei, Anderson Danielle E, Sobota Radoslaw Mikolaj, Dutertre Charles-Antoine, Wang Lin-Fa

机构信息

Programme in Emerging Infectious Diseases, Duke-NUS Medical School, Singapore, Singapore.

Functional Proteomics Laboratory, SingMass National Laboratory, Institute of Molecular and Cell Biology, Agency for Science, Technology and Research (A∗STAR), Singapore, Singapore.

出版信息

Immunity. 2022 Nov 8;55(11):2187-2205.e5. doi: 10.1016/j.immuni.2022.10.008.

Abstract

Bats are reservoir hosts of many zoonotic viruses with pandemic potential. We utilized single-cell transcriptome sequencing (scRNA-seq) to analyze the immune response in bat lungs upon in vivo infection with a double-stranded RNA virus, Pteropine orthoreovirus PRV3M. Bat neutrophils were distinguished by high basal IDO1 expression. NK cells and T cells were the most abundant immune cells in lung tissue. Three distinct CD8 effector T cell populations could be delineated by differential expression of KLRB1, GFRA2, and DPP4. Select NK and T clusters increased expression of genes involved in T cell activation and effector function early after viral infection. Alveolar macrophages and classical monocytes drove antiviral interferon signaling. Infection expanded a CSF1R population expressing collagen-like genes, which became the predominant myeloid cell type post-infection. This work uncovers features relevant to viral disease tolerance in bats, lays a foundation for future experimental work, and serves as a resource for comparative immunology studies.

摘要

蝙蝠是许多具有大流行潜力的人畜共患病毒的储存宿主。我们利用单细胞转录组测序(scRNA-seq)分析了蝙蝠肺部在体内感染双链RNA病毒——翼手目正呼肠孤病毒PRV3M后的免疫反应。蝙蝠中性粒细胞的特征是基础IDO1表达较高。自然杀伤(NK)细胞和T细胞是肺组织中最丰富的免疫细胞。通过KLRB1、GFRA2和DPP4的差异表达可以区分出三个不同的CD8效应T细胞群体。在病毒感染后早期,特定的NK和T细胞簇增加了参与T细胞活化和效应功能的基因表达。肺泡巨噬细胞和经典单核细胞驱动抗病毒干扰素信号传导。感染使一个表达胶原样基因的CSF1R群体扩大,该群体在感染后成为主要的髓样细胞类型。这项工作揭示了与蝙蝠病毒疾病耐受性相关的特征,为未来的实验工作奠定了基础,并为比较免疫学研究提供了资源。

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