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禽冠状病毒感染中的宿主免疫反应调节:气管转录组的体外和体内分析

Host Immune Response Modulation in Avian Coronavirus Infection: Tracheal Transcriptome Profiling In Vitro and In Vivo.

作者信息

O'Dowd Kelsey, Isham Ishara M, Vatandour Safieh, Boulianne Martine, Dozois Charles M, Gagnon Carl A, Barjesteh Neda, Abdul-Careem Mohamed Faizal

机构信息

Health Research Innovation Centre, Faculty of Veterinary Medicine, University of Calgary, Calgary, AB T2N 4N1, Canada.

Department of Animal and Poultry Science, Islamic Azad University, Qaemshahr Branch, Qaem Shahr 4765161964, Iran.

出版信息

Viruses. 2024 Apr 14;16(4):605. doi: 10.3390/v16040605.

Abstract

Infectious bronchitis virus (IBV) is a highly contagious causing moderate to severe respiratory infection in chickens. Understanding the initial antiviral response in the respiratory mucosa is crucial for controlling viral spread. We aimed to characterize the impact of IBV Delmarva (DMV)/1639 and IBV Massachusetts (Mass) 41 at the primary site of infection, namely, in chicken tracheal epithelial cells (cTECs) in vitro and the trachea in vivo. We hypothesized that some elements of the induced antiviral responses are distinct in both infection models. We inoculated cTECs and infected young specific pathogen-free (SPF) chickens with IBV DMV/1639 or IBV Mass41, along with mock-inoculated controls, and studied the transcriptome using RNA-sequencing (RNA-seq) at 3 and 18 h post-infection (hpi) for cTECs and at 4 and 11 days post-infection (dpi) in the trachea. We showed that IBV DMV/1639 and IBV Mass41 replicate in cTECs in vitro and the trachea in vivo, inducing host mRNA expression profiles that are strain- and time-dependent. We demonstrated the different gene expression patterns between in vitro and in vivo tracheal IBV infection. Ultimately, characterizing host-pathogen interactions with various IBV strains reveals potential mechanisms for inducing and modulating the immune response during IBV infection in the chicken trachea.

摘要

传染性支气管炎病毒(IBV)具有高度传染性,可在鸡群中引起中度至重度呼吸道感染。了解呼吸道黏膜的初始抗病毒反应对于控制病毒传播至关重要。我们旨在表征IBV德尔马瓦(DMV)/1639株和IBV马萨诸塞州(Mass)41株在感染的主要部位,即在体外鸡气管上皮细胞(cTECs)和体内气管中的影响。我们假设在两种感染模型中,诱导的抗病毒反应的某些要素是不同的。我们用IBV DMV/1639株或IBV Mass41株接种cTECs并感染幼龄无特定病原体(SPF)鸡,同时设置 mock 接种对照,在感染后3小时和18小时(hpi)对cTECs进行RNA测序(RNA-seq)研究转录组,并在感染后4天和11天(dpi)对气管进行研究。我们发现IBV DMV/1639株和IBV Mass41株可在体外cTECs和体内气管中复制,诱导宿主mRNA表达谱呈现毒株和时间依赖性。我们证明了体外和体内气管IBV感染之间不同的基因表达模式。最终,表征宿主与各种IBV毒株之间的相互作用揭示了鸡气管IBV感染期间诱导和调节免疫反应的潜在机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1151/11053446/004e6b1773c2/viruses-16-00605-g001.jpg

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