SARS-CoV-2 spike D614G variant confers enhanced replication and transmissibility

Author:

Zhou Bin,Thao Tran Thi Nhu,Hoffmann Donata,Taddeo Adriano,Ebert Nadine,Labroussaa Fabien,Pohlmann Anne,King Jacqueline,Portmann Jasmine,Halwe Nico Joel,Ulrich Lorenz,Trüeb Bettina Salome,Kelly Jenna N.,Fan Xiaoyu,Hoffmann Bernd,Steiner Silvio,Wang Li,Thomann Lisa,Lin Xudong,Stalder Hanspeter,Pozzi Berta,de Brot Simone,Jiang Nannan,Cui Dan,Hossain Jaber,Wilson Malania,Keller Matthew,Stark Thomas J.,Barnes John R.,Dijkman RonaldORCID,Jores Joerg,Benarafa Charaf,Wentworth David E.,Thiel Volker,Beer Martin

Abstract

AbstractDuring the evolution of SARS-CoV-2 in humans a D614G substitution in the spike (S) protein emerged and became the predominant circulating variant (S-614G) of the COVID-19 pandemic1. However, whether the increasing prevalence of the S-614G variant represents a fitness advantage that improves replication and/or transmission in humans or is merely due to founder effects remains elusive. Here, we generated isogenic SARS-CoV-2 variants and demonstrate that the S-614G variant has (i) enhanced binding to human ACE2, (ii) increased replication in primary human bronchial and nasal airway epithelial cultures as well as in a novel human ACE2 knock-in mouse model, and (iii) markedly increased replication and transmissibility in hamster and ferret models of SARS-CoV-2 infection. Collectively, our data show that while the S-614G substitution results in subtle increases in binding and replication in vitro, it provides a real competitive advantage in vivo, particularly during the transmission bottle neck, providing an explanation for the global predominance of S-614G variant among the SARS-CoV-2 viruses currently circulating.

Publisher

Cold Spring Harbor Laboratory

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