Early computational detection of potential high-risk SARS-CoV-2 variants

被引:17
作者
Beguir, Karim [1 ]
Skwark, Marcin J. [1 ]
Fu, Yunguan [1 ]
Pierrot, Thomas [1 ]
Carranza, Nicolas Lopez [1 ]
Laterre, Alexandre [1 ]
Kadri, Ibtissem [1 ]
Korched, Abir [1 ]
Lowegard, Anna U. [1 ]
Lui, Bonny Gaby [2 ]
Saenger, Bianca [2 ]
Liu, Yunpeng [3 ]
Poran, Asaf [3 ]
Muik, Alexander [2 ]
Sahin, Ugur [2 ]
机构
[1] InstaDeep Ltd, 5 Merchant Sq, London W2 1AY, England
[2] BioNTech SE, Goldgrube 12, D-55131 Mainz, Germany
[3] BioNTech US, 40 Erie St, Cambridge, MA 02139 USA
关键词
Supported by BioNTech and InstaDeep. We thank the BioNTech German clinical trial (NCT04380701; EudraCT:; 2020-001038-36); participants; from whom the post-immunisation human sera for the cross-neutralisation analysis were obtained.Supported by BioNTech and InstaDeep . We thank the BioNTech German clinical trial (NCT04380701; from whom the post-immunisation human sera for the cross-neutralisation analysis were obtained;
D O I
10.1016/j.compbiomed.2023.106618
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
The ongoing COVID-19 pandemic is leading to the discovery of hundreds of novel SARS-CoV-2 variants daily. While most variants do not impact the course of the pandemic, some variants pose an increased risk when the acquired mutations allow better evasion of antibody neutralisation or increased transmissibility. Early detection of such high-risk variants (HRVs) is paramount for the proper management of the pandemic. However, experimental assays to determine immune evasion and transmissibility characteristics of new variants are resource-intensive and time-consuming, potentially leading to delays in appropriate responses by decision makers. Presented herein is a novel in silico approach combining spike (S) protein structure modelling and large protein transformer language models on S protein sequences to accurately rank SARS-CoV-2 variants for immune escape and fitness potential. Both metrics were experimentally validated using in vitro pseudovirus-based neutralisation test and binding assays and were subsequently combined to explore the changing landscape of the pandemic and to create an automated Early Warning System (EWS) capable of evaluating new variants in minutes and risk-monitoring variant lineages in near real-time. The system accurately pinpoints the putatively dangerous variants by selecting on average less than 0.3% of the novel variants each week. The EWS flagged all 16 variants designated by the World Health Organization (WHO) as variants of interest (VOIs) if applicable or variants of concern (VOCs) otherwise with an average lead time of more than one and a half months ahead of their designation as such.
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