Statement of the WHO Working Group on COVID-19 Animal Models (WHO-COM) about the UK and South African SARS-CoV-2 new variants

– Simon Funnell, co-chair of the WHO-COM group presented a summary of the current knowledge regarding the B.1.1.7 variant in the UK including: i) Specific mutations in the spike, ORF1ab, ORF8 and N genes, ii) S gene target failure in diagnostic tests, iii) unanswered questions and iv) possible approaches. As it is being generated, information about this clade is being regularly updated at the following UK Government website location. https://www.gov.uk/government/collections/new-sars-cov-2-variant

– Public Health England and the University of KwaZulu-Natal are working as fast as possible to distribute the UK and South African variants respectively via dedicated repositories such as BEI, NIBSC, and EVA.

– Additional resources available immediately to the group are plasmids to encode the mutant spike RBD. These plasmids generated by Florian Krammer (Mount Sinai) will be distributed to group members without the need of an MTA and may help immediately to assess important questions such as possible evasion from neutralizing antibodies present in convalescent or vaccinee sera.

– The group agreed that a high priority is to test the new variant against existing COVID-19 sera. This could be done with existing non-human primate (NHP) sera or with vaccinee sera. Regarding the latter, PHE will seek collaborators to test the new variant against sera from test vaccines where permissions allow.

– With respect to the latter point, the group discussed ways to speed up sharing of sera without the need to execute new MTAs with developers. Rather than obtaining sera from clinical trials, the proposal would be to obtain and share sera from vaccinees receiving EUA vaccines. Collection of these sera by key laboratories of the WHO-COM distributed worldwide would ensure rapid testing of possible immune scape by emerging SARS-CoV-2 variants.

– With respect to pathogenicity testing, the WHO-COM agreed that, based on the fact that both variants include the N501Y mutation commonly seen in mouse-adapted SARS-CoV-2, it is likely that these viruses infect regular laboratory mice. In addition, hamster studies to compare the pathogenicity of these new variants with that of previous SARS-CoV-2 isolates was suggested.

– With respect to transmission studies, the group agreed that these experiments are important but that they may be very difficult. Transmission studies give usually yes/no results with little room for comparison. Yet, the WHO-COM has outstanding expertise in transmission studies including different models (cats, hamsters, ferrets, NHPs) as well as other experimental setups to assess airborne transmission, fomite transmission and direct contact transmission.