Dominant extrafollicular B cell responses in severe COVID-19 disease correlate with robust viral-specific antibody production but poor clinical outcomes

Author:

Woodruff Matthew C.,Ramonell Richard P.,Cashman Kevin S.,Nguyen Doan C.,Saini Ankur Singh,Haddad Natalie,Ley Ariel M.,Kyu Shuya,Howell J. Christina,Ozturk Tugba,Lee Saeyun,Chen Weirong,Estrada Jacob,Morrison-Porter Andrea,Derrico Andrew,Anam Fabliha A.,Sharma Monika,Wu Henry,Le Sang N.,Jenks Scott A.,Tipton Christopher M.,Daiss John L.,Hu William T.,Lee F. Eun-Hyung,Sanz Ignacio

Abstract

Abstract/IntroductionA wide clinical spectrum has become a hallmark of the SARS-CoV-2 (COVID-19) pandemic, although its immunologic underpinnings remain to be defined. We have performed deep 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 as previously described in autoimmune settings. Extrafollicular activation correlated strongly with large antibody secreting cell expansion and early production of high levels of SARS-CoV-2-specific antibodies. Yet, these patients fared poorly with elevated inflammatory biomarkers, multi-organ failure, and death. Combined, the findings strongly indicate a major pathogenic role for immune activation in subsets of COVID-19 patients. Our study suggests that, as in autoimmunity, targeted immunomodulatory therapy may be beneficial in specific patient subpopulations that can be identified by careful immune profiling.

Publisher

Cold Spring Harbor Laboratory

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