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Immunology

B-cell maturation defects in common variable immunodeficiency and association with clinical features

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Pages 288-294 | Received 19 Feb 2007, Accepted 27 May 2007, Published online: 06 Jul 2009
 

Summary

Aims: Patients with common variable immunodeficiency (CVID) often have defects in post-antigenic B-cell differentiation with fewer memory B cells and impaired isotype switching. We aimed to classify CVID patients according to these defects and determine whether this predicted clinical manifestations.

Methods: We analysed the memory marker CD27, maturation marker CD21, and IgD on peripheral blood B cells from 31 CVID patients and 23 controls using a whole-blood lysis technique, allocated patients according to two classifications (‘Freiburg’ and ‘Paris’) and correlated results with clinical manifestations.

Results: CVID patients had fewer memory (CD27+) B cells and isotype-switched (IgD) memory B cells in absolute number and proportion. Many CVID patients had increased immature (CD21) B cells. Lymphoproliferation and autoimmune cytopenias were found almost exclusively in these patients, including Freiburg group Ia (decreased switched memory and increased immature B cells), but also those with normal switched memory and increased immature B cells. The Paris classification was less useful in predicting clinical manifestations.

Conclusions: CVID is associated with defects in memory B-cell differentiation. Subclassification helps identify patients with clinical manifestations, particularly lymphoproliferation and autoimmune cytopenias in those with impaired B-cell maturation and isotype switching. Routine B-cell phenotyping may assist clinicians in predicting these clinical features.

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