Comparison of 10 emerging SARS-CoV-2 Variants: infectivity, animal tropism, and antibody neutralization (preprint)

Ten emerging SARS-CoV-2 variants—B.1.1.298, B.1.1.7, B.1.351, P.1, P.2, B.1.429, B.1.525, B.1.526-1, B.1.526-2, B.1.1.318—and seven corresponding single amino acid mutations in the receptor-binding domain were examined using SARS-CoV-2 pseudovirus. The results indicate that the current SARS-CoV-2 variants do not increase infectivity among humans. The K417N/T, N501Y, or E484K-carrying variants exhibited increased abilities to infect to mouse ACE2-overexpressing cells. The activities of Furin, TMPRSS2, and cathepsin L were increased against most of the variants. RBD amino acid mutations comprising K417T/N, L452R, Y453F, S477N, E484K, and N501Y caused significant immune escape from 11 of 13 monoclonal antibodies. However, the resistance to neutralization by convalescent serum or vaccines was mainly caused by the E484K mutation, while the neutralization of E484K-carrying variants was decreased by 1.1–6.2-fold. The convalescent serum from B.1.1.7- and B.1.351-infected patients neutralized the variants themselves better than other SARS-CoV-2 variants.

BU-Trace: A Permissionless Mobile System for Privacy-Preserving Intelligent Contact Tracing (preprint)

The coronavirus disease 2019 (COVID-19) pandemic has caused an unprecedented health crisis for the global. Digital contact tracing, as a transmission intervention measure, has shown its effectiveness on pandemic control. Despite intensive research on digital contact tracing, existing solutions can hardly meet users' requirements on privacy and convenience. In this paper, we propose BU-Trace, a novel permissionless mobile system for privacy-preserving intelligent contact tracing based on QR code and NFC technologies. First, a user study is conducted to investigate and quantify the user acceptance of a mobile contact tracing system. Second, a decentralized system is proposed to enable contact tracing while protecting user privacy. Third, an intelligent behavior detection algorithm is designed to ease the use of our system. We implement BU-Trace and conduct extensive experiments in several real-world scenarios. The experimental results show that BU-Trace achieves a privacy-preserving and intelligent mobile system for contact tracing without requesting location or other privacy-related permissions.

The Infectivity and Antigenicity of Epidemic SARS-CoV-2 Variants in the United Kingdom (preprint)

The SARS-CoV-2 variant VUI/202012/01 has been reported to spread unexpectedly fast in the United Kingdom. It is estimated that its transmissibility may increase by 70%. In this study, the top five variants circulating in the UK including D614G+L18F+A222V, D614G+A222V, D614G+S477N, VUI/202012/01 and D614G+69-70del+439K were analyzed for their infective and neutralizing characteristics. The pseudotyped viruses were constructed for the five variants and 12 single mutants composed those variants. We found that the VUI/202012/01 variant does enhance its infectivity due to the cumulative effect of multiple mutations including 69-70del and 144/145del mutations in NTD, A570D in RBD, and S982A in S2. Meanwhile, mutations N501Y, N439K and S477N in RBD can cause a significant decrease in the neutralization activity for some mAbs. Although VUI/202012/01 did not affect the neutralization effect of convalescent sera, it affected the neutralization activity of animal immunized sera by RBD protein or recombinant spike DNA to some extent.