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牛呼吸道合胞体病毒感染牛的肺转录组分析及抗病毒和/或环氧化酶抑制剂的治疗作用

Analysis of lung transcriptome in calves infected with Bovine Respiratory Syncytial Virus and treated with antiviral and/or cyclooxygenase inhibitor.

机构信息

Department of Pathology, Microbiology and Immunology, School of Veterinary Medicine, University of California Davis, Davis, California, United States of America.

Pediatric Emergency Medicine, Sutter Medical Center Sacramento, Sacramento, California, United States of America.

出版信息

PLoS One. 2021 Feb 18;16(2):e0246695. doi: 10.1371/journal.pone.0246695. eCollection 2021.

Abstract

Bovine Respiratory Syncytial virus (BRSV) is one of the major infectious agents in the etiology of the bovine respiratory disease complex. BRSV causes a respiratory syndrome in calves, which is associated with severe bronchiolitis. In this study we describe the effect of treatment with antiviral fusion protein inhibitor (FPI) and ibuprofen, on gene expression in lung tissue of calves infected with BRSV. Calves infected with BRSV are an excellent model of human RSV in infants: we hypothesized that FPI in combination with ibuprofen would provide the best therapeutic intervention for both species. The following experimental treatment groups of BRSV infected calves were used: 1) ibuprofen day 3-10, 2) ibuprofen day 5-10, 3) placebo, 4) FPI day 5-10, 5) FPI and ibuprofen day 5-10, 6) FPI and ibuprofen day 3-10. All calves were infected with BRSV on day 0. Daily clinical evaluation with monitoring of virus shedding by qRT-PCR was conducted. On day10 lung tissue with lesions (LL) and non-lesional (LN) was collected at necropsy, total RNA extracted, and RNA sequencing performed. Differential gene expression analysis was conducted with Gene ontology (GO) and KEGG pathway enrichment analysis. The most significant differential gene expression in BRSV infected lung tissues was observed in the comparison of LL with LN; oxidative stress and cell damage was especially noticeable. Innate and adaptive immune functions were reduced in LL. As expected, combined treatment with FPI and Ibuprofen, when started early, made the most difference in gene expression patterns in comparison with placebo, especially in pathways related to the innate and adaptive immune response in both LL and LN. Ibuprofen, when used alone, negatively affected the antiviral response and caused higher virus loads as shown by increased viral shedding. In contrast, when used with FPI Ibuprofen enhanced the specific antiviral effect of FPI, due to its ability to reduce the damaging effect of prostanoids and oxidative stress.

摘要

牛呼吸道合胞体病毒(BRSV)是牛呼吸道疾病综合征病因学中的主要传染性病原体之一。BRSV 引起犊牛呼吸道综合征,与严重的细支气管炎有关。在这项研究中,我们描述了抗病毒融合蛋白抑制剂(FPI)和布洛芬治疗对感染 BRSV 的犊牛肺组织基因表达的影响。感染 BRSV 的犊牛是婴儿人类 RSV 的极佳模型:我们假设 FPI 与布洛芬联合使用将为两种物种提供最佳的治疗干预。使用以下实验性 BRSV 感染犊牛治疗组:1)布洛芬第 3-10 天,2)布洛芬第 5-10 天,3)安慰剂,4)FPI 第 5-10 天,5)FPI 和布洛芬第 5-10 天,6)FPI 和布洛芬第 3-10 天。所有犊牛均于第 0 天感染 BRSV。通过 qRT-PCR 监测病毒脱落进行每日临床评估。在剖检时,第 10 天收集有病变(LL)和无病变(LN)的肺组织,提取总 RNA,并进行 RNA 测序。通过基因本体论(GO)和 KEGG 途径富集分析进行差异基因表达分析。在 BRSV 感染肺组织中观察到的最显着差异基因表达是在 LL 与 LN 比较中;氧化应激和细胞损伤尤为明显。LL 中的固有和适应性免疫功能降低。正如预期的那样,当早期开始时,与安慰剂相比,FPI 和布洛芬联合治疗在基因表达模式上的差异最大,尤其是在 LL 和 LN 中与固有和适应性免疫反应相关的途径。布洛芬单独使用时,会对抗病毒反应产生负面影响,并导致病毒载量增加,因为病毒脱落增加。相比之下,当与 FPI 一起使用时,布洛芬通过降低前列腺素和氧化应激的破坏性作用增强了 FPI 的特异性抗病毒作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a36/7891793/bdb61475ade7/pone.0246695.g001.jpg

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