Envelope domain III E 324 , E 351 , and E 380 mutations lever adaptive evolution of DENV-1 genotype I

生物 非同义代换 病毒学 登革热病毒 病毒 传染性 毒力 病毒准种 基因型 病毒进化 遗传学 基因 丙型肝炎病毒 基因组
作者
Tao Jiang,Chenxiao Huang,Qianqian Ruan,Xiaorong Huang,Chumin Liang,Zhiqiang Chen,Xi Yu,Yihao Peng,Zhongfan Liu,Gong Cheng,Jianfeng Dai,Jiufeng Sun
出处
期刊:Journal of Virology [American Society for Microbiology]
标识
DOI:10.1128/jvi.01183-24
摘要

ABSTRACT Dengue virus (DENV) gains genetic mutations during continuous transmission and evolution, making the virus more adaptive and virulent. The clade of DENV-1 genotype I has expanded and become the predominant genotype in Asia and the Pacific areas, but the underlying mechanisms are unclear. A combined analysis of nonsynonymous mutations in domain III of the envelope protein and their biological effects on virus pathogenesis and transmission was evaluated. Phylogenetic analyses found three nonsynonymous mutations (V324I, V351L, and V380I) in domain III of the envelope protein, which emerged in 1970s–1990s and stably inherited and expanded in contemporary strains after 2000. We generated reverse-mutated viruses (I324V, L351V, and I380V) based on an infectious clone of an epidemic DENV-1 strain (NIID02–20), and the results suggested that the infectivity of the contemporary epidemic virus (wild type, WT) has increased compared to the reverse mutant viruses in mammalian hosts but not mosquito vectors. The WT virus showed a higher binding affinity to host cells and increased virion stability. In addition, weaker immunogenicity and higher resistance to neutralizing antibodies of the WT virus indicated a trend of immune escape. The data suggested that nonsynonymous mutations of the E protein (V324I, V351L, and V380I) promote infectivity and immune evasion of DENV-1 genotype I, which may facilitate its onward transmission on a global scale. IMPORTANCE We provide evidence that minor sequence variation among dengue virus (DENV) strains can result in increased adaptability and virulence, impacting both the biology of the virus and the antiviral immune response. The genetic mutations of DENV-1 gained during continuous transmission and evolution will offer new clues for the design of novel vaccines against flaviviruses.

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