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严重急性呼吸综合征冠状病毒2(SARS-CoV-2)可导致老年罗伯罗夫斯基仓鼠出现慢性肺部炎症和呼吸功能受损。

SARS-CoV-2 causes chronic lung inflammation and impaired respiratory capacity in aged Roborovski dwarf hamsters.

作者信息

Karimi Amirhossein, Lieber Carolin M, Sakamoto Kaori, Plemper Richard K

机构信息

Center for Translational Antiviral Research, Georgia State University Institute for Biomedical Sciences, Atlanta, Georgia, USA.

Department of Population Health and Pathobiology, College of Veterinary Medicine, North Carolina State University, Raleigh, North Carolina, USA.

出版信息

J Virol. 2025 Aug 11:e0075525. doi: 10.1128/jvi.00755-25.

Abstract

Roborovski dwarf hamsters are permissive for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and progress to acute viral pneumonia with profound lung tissue injury, recapitulating hallmarks of severe coronavirus disease 2019 (COVID-19) in vulnerable patient groups such as older adults. In this study, we established dwarf hamster whole-body plethysmography and assessed disease severity and propensity for long-term compromise of lung recovery from severe COVID-19-like disease in young, adult, and aged animals. Aged dwarf hamsters infected intranasally with variant of concern (VOC) omicron BA.4 experienced more severe clinical signs, carried a higher lung virus load, and had a greater risk of succumbing to infection. Resting airway hypersensitivity was transiently increased in aged, but not young, dwarf hamsters 3-4 days post-infection. Pharmacologically induced respiratory distress revealed compromised lung capacity in animals of both age groups at peak disease. Aged animals showed impaired respiratory function for 45 days, mounted a weaker antiviral response, and developed chronic pneumonia with lasting tissue damage. Treatment of acute disease with approved antivirals, paxlovid-like nirmatrelvir + ritonavir or molnupiravir, prevented long-term respiratory sequelae in aged animals. Nirmatrelvir + ritonavir fully suppressed transient respiratory distress and mediated complete survival of aged animals. This study shows a high positive correlation between host age and SARS-CoV-2 disease severity in dwarf hamsters, establishes a model for chronic pneumonia with impaired respiratory capacity in at-risk hosts, and demonstrates the benefit of antiviral therapy of acute disease for long-term respiratory health.IMPORTANCEIn the COVID-19 pandemic, the frequency of chronic respiratory insufficiency after acute SARS-CoV-2 infection was positively linked to patient age. Roborovski dwarf hamsters recapitulate hallmarks of life-threatening COVID-19 in at-risk patients. In this study, we monitored disease progression and lung function in young and aged dwarf hamsters infected with a VOC omicron isolate and assessed the effect of antiviral treatment on long-term lung function. We established a strong correlation between host age and SARS-CoV-2 disease severity in dwarf hamsters, identified a high propensity of aged animals to develop chronic lung inflammation, and demonstrated a long-term loss of respiratory capacity in the subset of aged animals that survived the acute infection. Antiviral treatment suppressed the development of late sequelae and preserved lung function. These results have important implications for effective SARS-CoV-2 management in aged hosts at high risk of developing severe viral pneumonia with long-term impaired lung function.

摘要

罗伯罗夫斯基侏儒仓鼠对严重急性呼吸综合征冠状病毒2(SARS-CoV-2)感染敏感,会发展为急性病毒性肺炎并伴有严重的肺组织损伤,重现了老年等易感患者群体中2019冠状病毒病(COVID-19)的特征。在本研究中,我们建立了侏儒仓鼠全身体积描记法,并评估了幼年、成年和老年动物从严重COVID-19样疾病中恢复时的疾病严重程度和肺恢复长期受损的倾向。经鼻感染变异株(VOC)奥密克戎BA.4的老年侏儒仓鼠出现更严重的临床症状,肺部病毒载量更高,感染致死风险更大。感染后3-4天,老年侏儒仓鼠静息气道高反应性短暂增加,而幼年侏儒仓鼠则未出现。药物诱导的呼吸窘迫显示,在疾病高峰期,两个年龄组的动物肺功能均受损。老年动物的呼吸功能在45天内受损,抗病毒反应较弱,并发展为伴有持续组织损伤的慢性肺炎。用已批准的抗病毒药物(如帕罗韦德样的奈玛特韦+利托那韦或莫努匹拉韦)治疗急性疾病,可预防老年动物出现长期呼吸后遗症。奈玛特韦+利托那韦完全抑制了短暂的呼吸窘迫,并使老年动物完全存活。本研究表明,在侏儒仓鼠中,宿主年龄与SARS-CoV-2疾病严重程度之间存在高度正相关,建立了高危宿主呼吸功能受损的慢性肺炎模型,并证明了急性疾病抗病毒治疗对长期呼吸健康的益处。

重要性

在COVID-19大流行中,急性SARS-CoV-2感染后慢性呼吸功能不全的发生率与患者年龄呈正相关。罗伯罗夫斯基侏儒仓鼠重现了高危患者中危及生命的COVID-19的特征。在本研究中,我们监测了感染VOC奥密克戎毒株的幼年和老年侏儒仓鼠的疾病进展和肺功能,并评估了抗病毒治疗对长期肺功能的影响。我们在侏儒仓鼠中建立了宿主年龄与SARS-CoV-2疾病严重程度之间的强相关性,确定了老年动物发生慢性肺部炎症的高倾向,并证明了在急性感染中存活的老年动物亚组存在长期呼吸功能丧失。抗病毒治疗抑制了晚期后遗症的发展并保留了肺功能。这些结果对于有效管理有发展为严重病毒性肺炎并伴有长期肺功能受损高风险的老年宿主中的SARS-CoV-2具有重要意义。

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