Sensitivity of SARS-CoV-2 B.1.1.7 to mRNA vaccine-elicited antibodies

被引:0
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作者
Dami A. Collier
Anna De Marco
Isabella A. T. M. Ferreira
Bo Meng
Rawlings P. Datir
Alexandra C. Walls
Steven A. Kemp
Jessica Bassi
Dora Pinto
Chiara Silacci-Fregni
Siro Bianchi
M. Alejandra Tortorici
John Bowen
Katja Culap
Stefano Jaconi
Elisabetta Cameroni
Gyorgy Snell
Matteo S. Pizzuto
Alessandra Franzetti Pellanda
Christian Garzoni
Agostino Riva
Anne Elmer
Nathalie Kingston
Barbara Graves
Laura E. McCoy
Kenneth G. C. Smith
John R. Bradley
Nigel Temperton
Lourdes Ceron-Gutierrez
Gabriela Barcenas-Morales
William Harvey
Herbert W. Virgin
Antonio Lanzavecchia
Luca Piccoli
Rainer Doffinger
Mark Wills
David Veesler
Davide Corti
Ravindra K. Gupta
机构
[1] Cambridge Institute of Therapeutic Immunology & Infectious Disease,Department of Medicine
[2] University of Cambridge,Division of Infection and Immunity
[3] University College London,Department of Biochemistry
[4] Humabs Biomed SA,Clinic of Internal Medicine and Infectious Diseases
[5] a subsidiary of Vir Biotechnology,Division of Infectious Diseases, Luigi Sacco Hospital
[6] University of Washington,Department of Clinical Biochemistry and Immunology
[7] Vir Biotechnology,Institute of Biodiversity
[8] Clinica Luganese Moncucco,Department of Haematology
[9] University of Milan,Department of Infectious Diseases
[10] NIHR Cambridge Clinical Research Facility,Department of Biomedicine
[11] NIHR Bioresource,Botnar Research Centre for Child Health (BRCCH)
[12] University of Kent,Cambridge Clinical Research Centre, NIHR Clinical Research Facility
[13] Addenbrooke’s Hospital,MRC Toxicology Unit, School of Biological Sciences
[14] Laboratorio de Inmunologia,Department of Medicine
[15] UNAM,Department of Biochemistry
[16] University of Glasgow,Cancer Research UK, Cambridge Institute
[17] University of Cambridge,Department of Obstetrics & Gynaecology
[18] University of KwaZulu Natal,Centre for Enzyme Innovation
[19] Africa Health Research Institute,Institute of Microbiology and Infection
[20] Cambridge University Hospitals NHS Trust,Department of Surgery
[21] University Basel and University Hospital Basel,Biochemistry and Molecular Genetics
[22] University Basel & ETH Zurich,Cambridge and Peterborough Foundation Trust
[23] Cambridge University Hospitals NHS Foundation Trust,Australian National Phenome Centre
[24] Addenbrooke’s Hospital,Centre for Molecular Medicine and Innovative Therapeutics
[25] Heart and Lung Research Institute,Centre of Computational and Systems Medicine
[26] Royal Papworth Hospital NHS Foundation Trust,Department of Public Health and Primary Care, School of Clinical Medicine
[27] Addenbrooke’s Hospital,Nuffield Department of Medicine
[28] University of Cambridge,Deparment of Virology
[29] Cardiff University,Department of Pathogen Genomics
[30] Cambridge Institute for Medical Research,Department of Medicine
[31] Department of Veterinary Medicine,Genomics Innovation Department
[32] University of Cambridge,Department of Infectious Diseases
[33] University of Cambridge,Department of Microbiology
[34] The Rosie Maternity Hospital,Department of Medicine
[35] University of Portsmouth (PORT),School of Medicine, Department of Medicine
[36] University of Birmingham,School of Health Sciences, Department of Medicine
[37] Addenbrooke’s Hospital,Department of Clinical Infection & Diagnostics Research
[38] University of Colorado School of Medicine,Department of Medicine
[39] Fulbourn Hospital,Deep Seq Department, School of Life Sciences
[40] Murdoch University,Department of Medicine
[41] Health Futures Institute,Hub for Biotechnology in the Built Environment
[42] Murdoch University,Department of Medicine
[43] Health Futures Institute,Centre for Genomic Pathogen Surveillance
[44] Murdoch University,Clinical Microbiology and Public Health Laboratory
[45] University of Cambridge,School of Pharmacy and Biomedical Sciences
[46] Public Health Wales NHS Trust,Department of Medicine
[47] University of Oxford,Department of Medicine
[48] King’s College London,Department of Medicine
[49] Wellcome Sanger Institute,Department of Medicine
[50] University of Brighton,Department of Medicine
来源
Nature | 2021年 / 593卷
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摘要
Transmission of SARS-CoV-2 is uncontrolled in many parts of the world; control is compounded in some areas by the higher transmission potential of the B.1.1.7 variant1, which has now been reported in 94 countries. It is unclear whether the response of the virus to vaccines against SARS-CoV-2 on the basis of the prototypic strain will be affected by the mutations found in B.1.1.7. Here we assess the immune responses of individuals after vaccination with the mRNA-based vaccine BNT162b22. We measured neutralizing antibody responses after the first and second immunizations using pseudoviruses that expressed the wild-type spike protein or a mutated spike protein that contained the eight amino acid changes found in the B.1.1.7 variant. The sera from individuals who received the vaccine exhibited a broad range of neutralizing titres against the wild-type pseudoviruses that were modestly reduced against the B.1.1.7 variant. This reduction was also evident in sera from some patients who had recovered from COVID-19. Decreased neutralization of the B.1.1.7 variant was also observed for monoclonal antibodies that target the N-terminal domain (9 out of 10) and the receptor-binding motif (5 out of 31), but not for monoclonal antibodies that recognize the receptor-binding domain that bind outside the receptor-binding motif. Introduction of the mutation that encodes the E484K substitution in the B.1.1.7 background to reflect a newly emerged variant of concern (VOC 202102/02) led to a more-substantial loss of neutralizing activity by vaccine-elicited antibodies and monoclonal antibodies (19 out of 31) compared with the loss of neutralizing activity conferred by the mutations in B.1.1.7 alone. The emergence of the E484K substitution in a B.1.1.7 background represents a threat to the efficacy of the BNT162b2 vaccine.
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页码:136 / 141
页数:5
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