| Literature DB >> 35819358 |
Alessandro Camponeschi1, Kathrin Kläsener2,3, Timothy Sundell1, Christina Lundqvist1, Paul T Manna4, Negar Ayoubzadeh1, Martina Sundqvist1, Katrin Thorarinsdottir1, Mariele Gatto1,5, Marcella Visentini6, Karin Önnheim1, Alaitz Aranburu1, Huamei Forsman1, Olov Ekwall1,7, Linda Fogelstrand8,9, Inger Gjertsson1, Michael Reth2,3, Inga-Lill Mårtensson1.
Abstract
CD38 is a multifunctional protein expressed on the surface of B cells in healthy individuals but also in B cell malignancies. Previous studies have suggested a connection between CD38 and components of the IgM class B cell antigen receptor (IgM-BCR) and its coreceptor complex. Here, we provide evidence that CD38 is closely associated with CD19 in resting B cells and with the IgM-BCR upon engagement. We show that targeting CD38 with an antibody, or removing this molecule with CRISPR/Cas9, inhibits the association of CD19 with the IgM-BCR, impairing BCR signaling in normal and malignant B cells. Together, our data suggest that CD38 is a new member of the BCR coreceptor complex, where it exerts a modulatory effect on B cell activation upon antigen recognition by regulating CD19. Our study also reveals a new mechanism where α-CD38 antibodies could be a valuable option in therapeutic approaches to B cell malignancies driven by aberrant BCR signaling.Entities:
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Year: 2022 PMID: 35819358 PMCID: PMC9280193 DOI: 10.1084/jem.20220201
Source DB: PubMed Journal: J Exp Med ISSN: 0022-1007 Impact factor: 17.579