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用于研究基孔肯雅病毒发病机制的当前小鼠模型的局限性

Limitations of Current Mouse Models for the Study of Chikungunya Virus Pathogenesis.

作者信息

Chan Yi-Hao, Lum Fok-Moon, Ng Lisa Fong Poh

机构信息

Department of Biochemistry, Yong Loo Lin School of Medicine, National University of Singapore, 21 Lower Kent Ridge Road, Singapore 117597, Singapore.

Laboratory of Microbial Immunity, Singapore Immunology Network, Agency for Science, Technology and Research (AA*STAR), 8A Biomedical Grove, #04-06 Immunos, Singapore 138648, Singapore.

出版信息

Med Sci (Basel). 2015 Aug 7;3(3):64-77. doi: 10.3390/medsci3030064.

Abstract

Chikungunya virus (CHIKV) is an arthropod-borne alphavirus that causes febrile chikungunya fever (CHIKF) in humans. This disease is debilitating and characterized by acute fever onset and chronic incapacitating polyarthralgia. CHIKF pathogenesis remains poorly defined with no approved vaccines and therapies. Recent outbreaks in the Caribbean islands have elevated concerns over the possibility of a global pandemic. Tremendous efforts have been made to develop relevant mouse models to enable the study of infection and immunity against this viral disease. Among them, the more common C57BL/6 mouse model demonstrated the ability to recapitulate the symptoms shown in infected humans, including self-limiting arthritis, myositis, and tenosynovitis. This has facilitated the unraveling of some key factors involved in disease pathogenesis of CHIKF. However, the stark differences in immune response between humans and mouse models necessitate the development of an animal model with an immune system that is more genetically similar to the human system for a better representation. In this paper, we aim to uncover the limitations of the C57BL/6 model and discuss alternative mouse models for CHIKV research.

摘要

基孔肯雅病毒(CHIKV)是一种节肢动物传播的甲病毒,可导致人类发热性基孔肯雅热(CHIKF)。这种疾病使人衰弱,其特征为急性发热起病和慢性致残性多关节痛。CHIKF的发病机制仍不清楚,尚无获批的疫苗和疗法。最近在加勒比岛屿的疫情爆发加剧了人们对全球大流行可能性的担忧。人们已付出巨大努力来开发相关小鼠模型,以便研究针对这种病毒性疾病的感染和免疫情况。其中,较为常用的C57BL/6小鼠模型显示出能够重现受感染人类所表现出的症状,包括自限性关节炎、肌炎和腱鞘炎。这有助于揭示CHIKF疾病发病机制中一些关键因素。然而,人类和小鼠模型在免疫反应上的显著差异使得有必要开发一种免疫系统在基因上更类似于人类系统的动物模型,以便更好地呈现相关情况。在本文中我们旨在揭示C57BL/6模型的局限性,并讨论用于CHIKV研究的替代小鼠模型。

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