期刊
NATURE
卷 602, 期 7897, 页码 487-+出版社
NATURE PORTFOLIO
DOI: 10.1038/s41586-021-04352-y
关键词
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资金
- National Institutes of Health [P50AI150476, U19AI135990, U19AI135972, R01AI143292, R01AI120694, P01AI063302, F32CA239333, R01GM133981]
- Excellence in Research Award (ERA) from the Laboratory for Genomics Research (LGR)
- Roddenberry Foundation
- F. Hoffmann-La Roche
- Vir Biotechnology
- Center for Research on Influenza Pathogenesis (CRIP), a NIAID [HHSN272201400008C]
- Center for Research on Influenza Pathogenesis and Transmission (CRIPT), a NIAID [75N93021C00014]
- NCI SeroNet grant [U54CA260560]
- JPB Foundation
- Open Philanthropy Project [2020-215611 (5384)]
- Defense Advanced Research Projects Agency (DARPA) [HR0011-19-2-0020]
- Wellcome Senior Fellowship by Wellcome Investigator Award [108183, 220863]
- Wellcome Investigator Award [108079, 223065, 207511]
- MRC/UKRI G2P-UK National Virology consortium [MR/W005611/1]
- UCL COVID-19 fund
- Wellcome Trust [207498, 206298]
- European Research Council (ERC-Stg) [639429]
- Rosetrees Trust [M362-F1, M553]
- CF Trust [SRC006, SRC020]
- Marie Skodowska-Curie Individual Fellowships [896014]
- National Institutes of Health Research UCL/UCLH Biomedical Research Centre
- NIHR Biomedical Research Centre at UCLH
- IDEA Bio-Medical
- DHSC COVID-19 Fighting Fund
- UCSF [133122P]
- UCB [133122P]
- GSK [133122P]
- Marie Curie Actions (MSCA) [896014] Funding Source: Marie Curie Actions (MSCA)
- European Research Council (ERC) [639429] Funding Source: European Research Council (ERC)
The Alpha variant of SARS-CoV-2 effectively suppresses innate immune responses in airway epithelial cells compared to first-wave isolates, possibly due to increased expression of specific viral antagonist proteins. This enhanced innate immune suppression may increase the likelihood of successful transmission of the Alpha variant and potentially impact in vivo replication and infection duration. Mutations outside the spike coding region, such as those observed in the N and Orf9b regulatory regions, play a crucial role in the adaptation of SARS-CoV-2 variants to humans.
The emergence of SARS-CoV-2 variants of concern suggests viral adaptation to enhance human-to-human transmission(1,2). Although much effort has focused on the characterization of changes in the spike protein in variants of concern, mutations outside of spike are likely to contribute to adaptation. Here, using unbiased abundance proteomics, phosphoproteomics, RNA sequencing and viral replication assays, we show that isolates of the Alpha (B.1.1.7) variant 3 suppress innate immune responses in airway epithelial cells more effectively than first-wave isolates. We found that the Alpha variant has markedly increased subgenomic RNA and protein levels of the nucleocapsid protein (N), Orf9b and Orf6-all known innate immune antagonists. Expression of Orf9b alone suppressed the innate immune response through interaction with TOM70, a mitochondrial protein that is required for activation of the RNA-sensing adaptor MAVS. Moreover, the activity of Orf9b and its association with TOM70 was regulated by phosphorylation. We propose that more effective innate immune suppression, through enhanced expression of specific viral antagonist proteins, increases the likelihood of successful transmission of the Alpha variant, and may increase in vivo replication and duration of infection'. The importance of mutations outside the spike coding region in the adaptation of SARS-CoV-2 to humans is underscored by the observation that similar mutations exist in the N and Orf9b regulatory regions of the Delta and Omicron variants.
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