A safe, effective and adaptable live-attenuated SARS-CoV-2 vaccine to reduce disease and transmission using one-to-stop genome modifications

一种安全、有效且适应性强的减毒活SARS-CoV-2疫苗,利用一站式基因组改造技术降低疾病发生率和传播率。

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作者:Jacob Schön # ,G Tuba Barut # ,Bettina Salome Trüeb # ,Nico Joel Halwe ,Inês Berenguer Veiga ,Annika Kratzel ,Lorenz Ulrich ,Jenna N Kelly ,Melanie Brügger ,Claudia Wylezich ,Adriano Taddeo ,Etori Aguiar Moreira ,Demeter Túrós ,Llorenç Grau-Roma ,Ann Kathrin Ahrens ,Kore Schlottau ,Tobias Britzke ,Angele Breithaupt ,Björn Corleis ,Jana Kochmann ,Blandina I Oliveira Esteves ,Lea Almeida ,Lisa Thomann ,Christelle Devisme ,Hanspeter Stalder ,Silvio Steiner ,Sarah Ochsenbein ,Kimberly Schmied ,Fabien Labroussaa ,Jörg Jores ,Philip V'kovski ,Vladimir Cmiljanovic ,Marco P Alves ,Charaf Benarafa ,Nadine Ebert ,Donata Hoffmann ,Martin Beer ,Volker Thiel

Abstract

Approved vaccines are effective against severe COVID-19, but broader immunity is needed against new variants and transmission. Therefore, we developed genome-modified live-attenuated vaccines (LAV) by recoding the SARS-CoV-2 genome, including 'one-to-stop' (OTS) codons, disabling Nsp1 translational repression and removing ORF6, 7ab and 8 to boost host immune responses, as well as the spike polybasic cleavage site to optimize the safety profile. The resulting OTS-modified SARS-CoV-2 LAVs, designated as OTS-206 and OTS-228, are genetically stable and can be intranasally administered, while being adjustable and sustainable regarding the level of attenuation. OTS-228 exhibits an optimal safety profile in preclinical animal models, with no side effects or detectable transmission. A single-dose vaccination induces a sterilizing immunity in vivo against homologous WT SARS-CoV-2 challenge infection and a broad protection against Omicron BA.2, BA.5 and XBB.1.5, with reduced transmission. Finally, this promising LAV approach could be applicable to other emerging viruses.

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