来自2.3.4.4b分支的反向遗传学衍生牛H5N1病毒在BALB/c小鼠中比旧的1分支H5N1病毒表现出更强的全身感染性和致病性。
Reverse genetics-derived cattle H5N1 virus from Clade 2.3.4.4b shows enhanced systemic infectivity and pathogenicity than an older Clade 1 H5N1 virus in BALB/c mice.
作者信息
Xiao Na, Oong Xiang Yong, Chen Yanxia, Li Can, Chung Howard Chun-Ho, Wang Pui, Ye Zhanhong, Lam Alvin Hiu-Chung, Cai Jianpiao, Song Wenchen, Lee Andrew Chak-Yiu, Chu Hin, Kok Kin-Hang, Chan Jasper Fuk-Woo, Yuan Shuofeng, Chen Honglin, Yuen Kwok-Yung, Zhang Anna Jin-Xia
机构信息
State Key Laboratory of Emerging Infectious Diseases, Carol Yu Centre for Infection, Department of Microbiology, School of Clinical Medicine, Li Ka Shing Faculty of Medicine, The University of Hong Kong, Pokfulam, Hong Kong Special Administrative Region, People's Republic of China.
Centre for Virology, Vaccinology and Therapeutics, Hong Kong Science and Technology Park, Hong Kong Special Administrative Region, Shatin, People's Republic of China.
出版信息
Emerg Microbes Infect. 2025 Dec;14(1):2475836. doi: 10.1080/22221751.2025.2475836. Epub 2025 Mar 17.
The newly emerged avian influenza A H5N1 Clade 2.3.4.4b can infect dairy cows and shed live virus in their milk. Sporadic cattle-to-human infections have been reported, highlighting the urgent need to understand its pathogenesis in mammals. Using both non-lactating and lactating BALB/c mice, we examined the viral tissue tropism, histopathological damages, and host immune responses upon intranasal inoculation with a reverse-genetic virus constructed based on A/dairy cattle/Texas/24-008749-003/2024 (Cattle-H5N1) and comparing with an older reference Clade 1 virus, A/Vietnam/1194/2004 virus (VNM1194-H5N1). Cattle-H5N1 was highly lethal in mice (mLD = 1.48PFU) with broad tissue tropism and produced higher titer in respiratory tissue and multiple extrapulmonary organs than VNM1194-H5N1. In the lungs, Cattle-H5N1 infection of airway epithelium, type II pneumocytes and CD45 immune cells were at a higher frequency than those of VNM1194-H5N1-infected mice, resulting in severe epithelial destruction and diffuse alveolar damage accompanied by elevated lung and serum pro-inflammatory cytokine/chemokines. Although both H5N1 viruses showed lactating mammary gland tropism, the gland tissue was more severely damaged after Cattle-H5N1 infection with abundant viral antigens expression in glandular cells, associated fat and lymphoid tissues. Furthermore, more suckling mice co-housed with Cattle-H5N1 infected lactating mice were virus-positive (7/30 pups) than VNM1194-H5N1. Brains were heavily infected by Cattle-H5N1, and neurological signs such as body-rolling/spinning, trembling and/or limb paralysis were seen only in Cattle-H5N1 infected mice. The spleen was more severely damaged by Cattle-H5N1 infection, which showed massive viral antigen expression accompanied by severe apoptosis and splenic atrophy, concluding that Cattle-H5N1 is more virulent in mice than VNM1194-H5N1.
新出现的甲型禽流感H5N1进化分支2.3.4.4b可感染奶牛并在其乳汁中排出活病毒。已报告了偶发的牛传人感染病例,凸显了迫切需要了解其在哺乳动物中的发病机制。我们使用非泌乳和泌乳的BALB/c小鼠,通过鼻内接种基于A/奶牛/得克萨斯州/24 - 008749 - 003/2024(牛-H5N1)构建的反向遗传病毒,并与一种较旧的参考进化分支1病毒A/越南/1194/2004病毒(VNM1194-H5N1)进行比较,研究了病毒的组织嗜性、组织病理学损伤和宿主免疫反应。牛-H5N1对小鼠具有高度致死性(半数致死剂量mLD = 1.48PFU),具有广泛的组织嗜性,并且在呼吸道组织和多个肺外器官中产生的病毒滴度高于VNM1194-H5N1。在肺部,牛-H5N1感染气道上皮细胞、II型肺泡上皮细胞和CD45免疫细胞的频率高于VNM1194-H5N1感染的小鼠,导致严重的上皮破坏和弥漫性肺泡损伤,同时伴有肺和血清促炎细胞因子/趋化因子升高。尽管两种H5N1病毒均表现出对泌乳乳腺的嗜性,但牛-H5N1感染后乳腺组织受损更严重,腺细胞、相关脂肪和淋巴组织中有丰富的病毒抗原表达。此外,与感染牛-H5N1的泌乳小鼠同笼饲养的更多乳鼠呈病毒阳性(7/30只幼崽),高于VNM1194-H5N1。牛-H5N1严重感染脑部,仅在感染牛-H5N1的小鼠中出现身体翻滚/旋转、颤抖和/或肢体麻痹等神经症状。牛-H5N1感染使脾脏受损更严重,表现为大量病毒抗原表达,伴有严重的细胞凋亡和脾萎缩,结论是牛-H5N1在小鼠中比VNM1194-H5N1更具致病性。
Zotero 插件