Author: de Camposâ€Mata, Leire; Tejedor Vaquero, Sonia; Tachóâ€Piñot, Roser; Piñero, Janet; Grasset, Emilie K; Arrieta Aldea, Itziar; Rodrigo Melero, Natalia; Carolis, Carlo; Horcajada, Juan P; Cerutti, Andrea; Villarâ€GarcÃa, Judit; Magri, Giuliana
Title: SARSâ€CoVâ€2 sculpts the immune system to induce sustained virusâ€specific naïveâ€like and memory Bâ€cell responses Cord-id: drfempan Document date: 2021_9_5
ID: drfempan
Snippet: OBJECTIVES: SARSâ€CoVâ€2 infection induces virusâ€reactive memory B cells expressing unmutated antibodies, which hints at their emergence from naïve B cells. Yet, the dynamics of virusâ€specific naïve B cells and their impact on immunity and immunopathology remain unclear. METHODS: We longitudinally profiled SARSâ€CoVâ€2â€specific Bâ€cell responses in 25 moderateâ€toâ€severe COVIDâ€19 patients by highâ€dimensional flow cytometry and isotyping and subtyping ELISA. We also explored t
Document: OBJECTIVES: SARSâ€CoVâ€2 infection induces virusâ€reactive memory B cells expressing unmutated antibodies, which hints at their emergence from naïve B cells. Yet, the dynamics of virusâ€specific naïve B cells and their impact on immunity and immunopathology remain unclear. METHODS: We longitudinally profiled SARSâ€CoVâ€2â€specific Bâ€cell responses in 25 moderateâ€toâ€severe COVIDâ€19 patients by highâ€dimensional flow cytometry and isotyping and subtyping ELISA. We also explored the relationship of Bâ€cell responses to SARSâ€CoVâ€2 with the activation of effector and regulatory cells from the innate or adaptive immune system. RESULTS: We found a virusâ€specific antibody response with a broad spectrum of classes and subclasses during acute infection, which evolved into an IgG1â€dominated response during convalescence. Acute infection was associated with increased mature Bâ€cell progenitors in the circulation and the unexpected expansion of virusâ€targeting naïveâ€like B cells. The latter further augmented during convalescence together with virusâ€specific memory B cells. In addition to a transitory increase in tissueâ€homing CXCR3(+) plasmablasts and extrafollicular memory B cells, most COVIDâ€19 patients showed persistent activation of CD4(+) and CD8(+) T cells along with transient or longâ€lasting changes of key innate immune cells. Remarkably, virusâ€specific antibodies and the frequency of naïve B cells were among the major variables defining distinct immune signatures associated with disease severity and inflammation. CONCLUSION: Aside from providing new insights into the complexity of the immune response to SARSâ€CoVâ€2, our findings indicate that the de novo recruitment of mature Bâ€cell precursors into the periphery may be central to the induction of antiviral immunity.
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