Computationally designed Spike antigens induce neutralising responses against the breadth of SARS-COV-2 variants

Author:

Vishwanath SnehaORCID,Carnell George WilliamORCID,Billmeier Martina,Ohlendorf Luis,Neckermann Patrick,Asbach Benedikt,George CharlotteORCID,Sans Maria Suau,Chan Andrew,Olivier Joey,Nadesalingam Angalee,Einhauser Sebastian,Temperton NigelORCID,Cantoni Diego,Grove Joe,Jordan IngoORCID,Sandig Volker,Tonks Paul,Geiger Johannes,Dohmen Christian,Mummert Verena,Samuel Anne Rosalind,Plank Christian,Kinsley Rebecca,Wagner Ralf,Heeney Jonathan LukeORCID

Abstract

AbstractUpdates of SARS-CoV-2 vaccines are required to generate immunity in the population against constantly evolving SARS-CoV-2 variants of concerns (VOCs). Here we describe three novel in-silico designed spike-based antigens capable of inducing neutralising antibodies across a spectrum of SARS-CoV-2 VOCs. Three sets of antigens utilising pre-Delta (T2_32), and post-Gamma sequence data (T2_35 and T2_36) were designed. T2_32 elicited superior neutralising responses against VOCs compared to the Wuhan-1 spike antigen in DNA prime-boost immunisation regime in guinea pigs. Heterologous boosting with the attenuated poxvirus - Modified vaccinia Ankara expressing T2_32 induced broader neutralising immune responses in all primed animals. T2_32, T2_35 and T2_36 elicited broader neutralising capacity compared to the Omicron BA.1 spike antigen administered by mRNA immunisation in mice. These findings demonstrate the utility of structure-informed computationally derived modifications of spike-based antigens for inducing broad immune responses covering more than 2 years of evolved SARS-CoV-2 variants.

Publisher

Springer Science and Business Media LLC

Reference52 articles.

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