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Complement C4A Regulates Autoreactive B Cells in Murine Lupus

Léa Simoni, Jessy Présumey, Cees E. van der Poel, Carlos Castrillón, Sarah E. Chang, Paul J. Utz, Michael C. Carroll

2020Cell Reports27 citationsDOIOpen Access PDF

Abstract

Systemic lupus erythematosus (SLE) is a severe autoimmune disease mediated by pathogenic autoantibodies. While complement protein C4 is associated with SLE, its isoforms (C4A and C4B) are not equal in their impact. Despite being 99% homologous, genetic studies identified C4A as more protective than C4B. By generating gene-edited mouse strains expressing either human C4A or C4B and crossing these with the 564lgi lupus strain, we show that, overall, C4A-like 564Igi mice develop less humoral autoimmunity than C4B-like 564Igi mice. This includes a decrease in the number of GCs, autoreactive B cells, autoantibodies, and memory B cells. The higher efficiency of C4A in inducing self-antigen clearance is associated with the follicular exclusion of autoreactive B cells. These results explain how the C4A isoform is protective in lupus and suggest C4A as a possible replacement therapy in lupus.

Topics & Concepts

C4ASystemic lupus erythematosusAutoantibodyImmunologyAutoimmunityBiologyComplement systemGene isoformGeneAntibodyDiseaseMedicineGeneticsPathologyComplement system in diseasesSystemic Lupus Erythematosus ResearchT-cell and B-cell Immunology