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Identification of a human splenic marginal zone B cell precursor with NOTCH2-dependent differentiation properties.
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Integrating autoimmune risk loci with gene-expression data identifies specific pathogenic immune cell subsets.
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BAFF and selection of autoreactive B cells.
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Human memory B cells originate from three distinct germinal center-dependent and -independent maturation pathways.
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Anergic responses characterize a large fraction of human autoreactive naive B cells expressing low levels of surface IgM.
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