Author:
Yang Sijie,Yu Yuanling,Jian Fanchong,Song Weiliang,Yisimayi Ayijiang,Chen Xiaosu,Xu Yanli,Wang Peng,Wang Jing,Yu Lingling,Niu Xiao,Wang Jing,Xiao Tianhe,An Ran,Wang Yao,Gu Qingqing,Shao Fei,Jin Ronghua,Shen Zhongyang,Wang Youchun,Cao Yunlong
Abstract
AbstractThe recently identified SARS-CoV-2 variant, BA.2.86, which carries a substantial number of Spike mutations, has raised a global alarm. An immediate assessment of its antigenic properties and infectivity is necessary. Here, we reveal the distinct antigenicity of BA.2.86 compared with previous variants including XBB.1.5. BA.2.86 significantly evades convalescent plasma from XBB breakthrough infection (BTI) and reinfections. Key mutations that mediate the enhanced resistance include N450D, K356T, L452W, A484K, V483del, and V445H on the RBD, while BA.2.86’s NTD mutations and E554K on SD1 also largely contribute. However, we found that BA.2.86 pseudovirus exhibits compromised efficiency of infecting HEK293T-hACE2 cells compared to XBB.1.5 and EG.5, which may be caused by K356T, V483del, and E554K, and could potentially limit BA.2.86’s transmissibility. In sum, it appears that BA.2.86 has traded its infectivity for higher immune evasion during long-term host-viral evolution. Close attention should be paid to monitoring additional mutations that could improve BA.2.86’s infectivity.
Publisher
Cold Spring Harbor Laboratory
Cited by
13 articles.
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