Publication | Open Access
Identification of a human splenic marginal zone B cell precursor with NOTCH2-dependent differentiation properties
126
Citations
42
References
2014
Year
Op9 CellsImmunogeneticsCell LineageDevelopmental BiologyNotch2-dependent Differentiation PropertiesLymphocyte DevelopmentImmune Cell DevelopmentMedicineImmunologyAutoimmunityYoung ChildrenImmunopathologyMarginal Zone BCell BiologyCell SignalingCell DevelopmentMyelopoiesisCell Specialization
Mouse splenic marginal zone precursors (MZPs) differentiate into marginal zone B (MZB) cells under a signaling pathway involving Notch2 and its ligand, delta-like 1 ligand (Dll1). We report the identification of an MZP subset in the spleen of young children. These MZPs differentiate into MZ-like B cells in vitro in the presence of OP9 cells expressing human DLL1, as demonstrated by the up-regulation of classical MZB cell markers. A set of diagnostic genes discriminating IgM+IgD+CD27+ blood and splenic MZB cells from switched B cells was identified (up-regulation of SOX7, down-regulation of TOX, COCH, and HOPX), and their expression during the induction assay mirrored the one of MZB cells. Moreover, Alagille patients with a NOTCH2 haploinsufficiency display a marked reduction of IgM+IgD+CD27+ B cells in blood, whereas their switched memory B cells are not affected. Altogether, these results argue in favor of the existence of a rodent-like MZB cell lineage in humans.
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