Extrafollicular B cell responses correlate with neutralizing antibodies and morbidity in COVID-19

滤泡外B细胞反应与中和抗体和COVID-19发病率相关

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作者:Matthew C Woodruff # ,Richard P Ramonell # ,Doan C Nguyen ,Kevin S Cashman ,Ankur Singh Saini ,Natalie S Haddad ,Ariel M Ley ,Shuya Kyu ,J Christina Howell ,Tugba Ozturk ,Saeyun Lee ,Naveenchandra Suryadevara ,James Brett Case ,Regina Bugrovsky ,Weirong Chen ,Jacob Estrada ,Andrea Morrison-Porter ,Andrew Derrico ,Fabliha A Anam ,Monika Sharma ,Henry M Wu ,Sang N Le ,Scott A Jenks ,Christopher M Tipton ,Bashar Staitieh ,John L Daiss ,Eliver Ghosn ,Michael S Diamond ,Robert H Carnahan ,James E Crowe Jr ,William T Hu ,F Eun-Hyung Lee ,Ignacio Sanz

Abstract

A wide spectrum of clinical manifestations has become a hallmark of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) COVID-19 pandemic, although the immunological underpinnings of diverse disease outcomes remain to be defined. We performed detailed characterization of B cell responses through high-dimensional flow cytometry to reveal substantial heterogeneity in both effector and immature populations. More notably, critically ill patients displayed hallmarks of extrafollicular B cell activation and shared B cell repertoire features previously described in autoimmune settings. Extrafollicular activation correlated strongly with large antibody-secreting cell expansion and early production of high concentrations of SARS-CoV-2-specific neutralizing antibodies. Yet, these patients had severe disease with elevated inflammatory biomarkers, multiorgan failure and death. Overall, these findings strongly suggest a pathogenic role for immune activation in subsets of patients with COVID-19. Our study provides further evidence that targeted immunomodulatory therapy may be beneficial in specific patient subpopulations and can be informed by careful immune profiling.

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