BA.2.12.1, BA.4 and BA.5 escape antibodies elicited by Omicron BA.1 infection-Reference-Cited by-同舟云学术

BA.2.12.1, BA.4 and BA.5 escape antibodies elicited by Omicron BA.1 infection

Published:2022-05-02 Issue: Volume: Page:
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Author:

Xie Xiaoliang¹^ORCID,Cao Yunlong²^ORCID,Yisimayi Ayijiang²,Jian Fanchong²^ORCID,Song Weiliang³,Xiao Tianhe³,Wang Lei⁴,Du Shuo²^ORCID,wang jing^ORCID,Li Qianqian⁵,Chen Xiaosu⁶,Wang Peng³,Zhang Zhiying²^ORCID,Liu Pulan⁷,An Ran³,Hao Xiaohua⁸,Wang Yao³,Wang Jing³,Feng Rui⁹,Sun Haiyan³,Zhao Lijuan¹,Zhang Wen¹⁰,Zhao Dong¹⁰,Zheng Jiang¹,Yu Lingling¹,Li Can¹,Zhang Na¹,Wang Rui¹,Niu Xiao³,Yang Sijie³,Song Xuetao¹,Zheng Linlin¹,Li Zhiqiang¹¹,Gu Qingqing¹,Shao Fei³,Huang Weijin¹²^ORCID,ronghua Jin^ORCID,Shen Zhongyang¹³,Wang Youchun¹⁴^ORCID,Wang Xiangxi¹⁵^ORCID,Xiao Junyu²^ORCID

Affiliation:

1. Changping Laboratory

2. Peking University

3. Biomedical Pioneering Innovation Center (BIOPIC), Peking University, Beijing, P.R. China.

4. CAS Key Laboratory of Infection and Immunity, National Laboratory of Macromolecules, Institute of Biophysics, Chinese Academy of Sciences, Beijing 100101, China.

5. National Institutes for Food and Drug Control

6. Institute for Immunology, College of Life Sciences, Nankai University, Tianjin, P. R. China.

7. School of Life Sciences, Peking University

8. Beijing Ditan Hospital

9. Chinese Academy of Sciences

10. Beijing Ditan Hospital, Capital Medical University

11. Academy for Advanced Interdisciplinary Studies, Peking University

12. NIFDC

13. Organ Transplant Center, NHC Key Laboratory for Critical Care Medicine, Tianjin First Central Hospital, Nankai University, Tianjin, P. R. China.

14. National Institutes for Food and Drug Control (NIFDC) and WHO Collaborating Center for Standardization and Evaluation of Biologicals, Beijing, China

15. Institute of Biophysics

Abstract

Abstract Recent emergence of SARS-CoV-2 Omicron sublineages BA.2.12.1, BA.2.13, BA.4 and BA.5 all contain L452 mutations and show potential higher transmissibility over BA.2. The new variants’ receptor binding and immune evasion capability require immediate investigation, especially on the role of L452 substitutions. Herein, coupled with structural comparisons, we showed that BA.2 sublineages, including BA.2.12.1 and BA.2.13, exhibit increased ACE2-binding affinities compared to BA.1; while BA.4/BA.5 shows the weakest receptor-binding activity due to F486V and R493Q reversion. Importantly, compared to BA.2, BA.2.12.1 and BA.4/BA.5 exhibit stronger neutralization escape from the plasma of 3-dose vaccinees and, most strikingly, from vaccinated BA.1 convalescents. To delineate the underlying evasion mechanism, we determined the escaping mutation profiles, epitope distribution and Omicron sub-lineage neutralization efficacy of 1640 RBD-directed neutralizing antibodies (NAbs), including 614 isolated from BA.1 convalescents. Interestingly, post-vaccination BA.1 infection mainly recalls wildtype-induced humoral memory and elicits antibodies that neutralize both wild-type and BA.1. These cross-reactive NAbs are significantly enriched on non-ACE2-competing epitopes; and surprisingly, the majority are undermined by R346 and L452 substitutions, namely R346K (BA.1.1), L452M (BA.2.13), L452Q (BA.2.12.1) and L452R (BA.4/BA.5), suggesting that R346K and L452 mutations appeared under the immune pressure of Omicron convalescents. Nevertheless, BA.1 infection can also induce new clones of BA.1-specific antibodies that potently neutralize BA.1 but do not respond to wild-type SARS-CoV-2, due to the high susceptibility to N501, N440, K417 and E484. However, these NAbs are largely escaped by BA.2 sublineages and BA.4/BA.5 due to D405N and F486V, exhibiting poor neutralization breadths. As for therapeutic NAbs, LY-CoV1404 (Bamlanivimab) and COV2-2130 (Cilgavimab) can still effectively neutralize BA.2.12.1 and BA.4/BA.5, while the S371F, D405N and R408S mutations carried by BA.2/BA.4/BA.5 sublineages would undermine most broad sarbecovirus NAbs. Together, our results indicate that Omicron can evolve mutations to specifically evade humoral immunity elicited by BA.1 infection. The continuous evolution of Omicron poses great challenges to SARS-CoV-2 herd immunity and suggests that BA.1-derived vaccine boosters may not be ideal for achieving broad-spectrum protection.

Publisher

Research Square Platform LLC

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