Author:
Marcotte Harold,Cao Yunlong,Zuo Fanglei,Simonelli Luca,Sammartino Josè Camilla,Pedotti Mattia,Sun Rui,Cassaniti Irene,Hagbom Marie,Piralla Antonio,Yang Jinxuan,Du Likun,Percivalle Elena,Bertoglio Federico,Schubert Maren,Abolhassani Hassan,Sherina Natalia,Guerra Concetta,Borte Stephan,Razaei Nima,Kumagai-Braesch Makiko,Xue Yintong,Grönwall Caroline,Klareskog Lars,Calzolai Luigi,Cavalli Andrea,Wang Qiao,Robbiani Davide F.,Hust Michael,Shi Zhengli,Feng Liqiang,Svensson Lennart,Chen Ling,Bao Linlin,Baldanti Fausto,Qin Chuan,Xiao Junyu,Hammarström Lennart,Yang Xing Lou,Varani Luca,Xie Xiaoliang Sunney,Pan-Hammarström Qiang
Abstract
AbstractThe emergence of Omicron lineages and descendent subvariants continues to present a severe threat to the effectiveness of vaccines and therapeutic antibodies. We have previously suggested that an insufficient mucosal IgA response induced by the mRNA vaccines is associated with a surge in breakthrough infections. Here, we further show that the intramuscular mRNA and/or inactivated vaccines cannot sufficiently boost the mucosal sIgA response in uninfected individuals, particularly against the Omicron variant. We thus engineered and characterized recombinant monomeric, dimeric and secretory IgA1 antibodies derived from four neutralizing IgG monoclonal antibodies targeting the receptor-binding domain of the spike protein (01A05, rmAb23, DXP-604 and XG014). Compared to their parental IgG antibodies, dimeric and secretory IgA1 antibodies showed a higher neutralizing activity against different variants of concern (VOCs), in part due to an increased avidity. Importantly, the dimeric or secretory IgA1 form of the DXP-604 antibody significantly outperformed its parental IgG antibody, and neutralized the Omicron lineages BA.1, BA.2 and BA.4/5 with a 50-150-fold increase in potency, reaching the level of the most potent monoclonal antibodies described till date. In hACE2 transgenic mice, a single intranasal dose of the dimeric IgA DXP-604 conferred prophylactic and therapeutic protection against Omicron BA.5. Conversion of IgA and dimerization further enhanced or restored the neutralizing ability against the emerging Omicron sub-variants (DXP-604 for BQ.1, BQ.1.1 and BA2.75; 01A05 for BA2.75, BA.2.75.2 and XBB.1). Thus, dimeric or secretory IgA delivered by nasal administration may potentially be exploited for the treatment and prevention of Omicron infection, thereby providing an alternative tool for combating immune evasion by subvariants and, potentially, future VOCs.One Sentence SummaryEngineered dimeric and secretory IgA1 neutralized Omicron variant with higher potency than parental IgG.
Publisher
Cold Spring Harbor Laboratory