CVID-associated TACI mutations affect autoreactive B cell selection and activation
Neil Romberg, Nicolas Chamberlain, David Saadoun, Maurizio Gentile, Tuure Kinnunen, Yen Shing Ng, Manmeet Virdee, Laurence Menard, Tineke Cantaert, Henner Morbach, Rima Rachid, Natalia Martinez-Pomar, Nuria Matamoros, Raif Geha, Bodo Grimbacher, Andrea Cerutti, Charlotte Cunningham-Rundles, Eric Meffre
Neil Romberg, Nicolas Chamberlain, David Saadoun, Maurizio Gentile, Tuure Kinnunen, Yen Shing Ng, Manmeet Virdee, Laurence Menard, Tineke Cantaert, Henner Morbach, Rima Rachid, Natalia Martinez-Pomar, Nuria Matamoros, Raif Geha, Bodo Grimbacher, Andrea Cerutti, Charlotte Cunningham-Rundles, Eric Meffre
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Research Article

CVID-associated TACI mutations affect autoreactive B cell selection and activation

Abstract

Common variable immune deficiency (CVID) is an assorted group of primary diseases that clinically manifest with antibody deficiency, infection susceptibility, and autoimmunity. Heterozygous mutations in the gene encoding the tumor necrosis factor receptor superfamily member TACI are associated with CVID and autoimmune manifestations, whereas two mutated alleles prevent autoimmunity. To assess how the number of TACI mutations affects B cell activation and tolerance checkpoints, we analyzed healthy individuals and CVID patients carrying one or two TACI mutations. We found that TACI interacts with the cleaved, mature forms of TLR7 and TLR9 and plays an important role during B cell activation and the central removal of autoreactive B cells in healthy donors and CVID patients. However, only subjects with a single TACI mutation displayed a breached immune tolerance and secreted antinuclear antibodies (ANAs). These antibodies were associated with the presence of circulating B cell lymphoma 6–expressing T follicular helper (Tfh) cells, likely stimulating autoreactive B cells. Thus, TACI mutations may favor CVID by altering B cell activation with coincident impairment of central B cell tolerance, whereas residual B cell responsiveness in patients with one, but not two, TACI mutations enables autoimmune complications.

Authors

Neil Romberg, Nicolas Chamberlain, David Saadoun, Maurizio Gentile, Tuure Kinnunen, Yen Shing Ng, Manmeet Virdee, Laurence Menard, Tineke Cantaert, Henner Morbach, Rima Rachid, Natalia Martinez-Pomar, Nuria Matamoros, Raif Geha, Bodo Grimbacher, Andrea Cerutti, Charlotte Cunningham-Rundles, Eric Meffre

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Figure 4

A defective peripheral B cell tolerance checkpoint in CVID patients.

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A defective peripheral B cell tolerance checkpoint in CVID patients. (A)...
(A) Recombinant antibodies derived from mature naive B cells from subjects or CVID patients with or without TACI mutation(s) were tested by ELISA for anti–HEp-2 cell reactivity. Dashed lines show the ED38-positive control (21). Horizontal lines define the cutoff OD405 for positive reactivity. For each individual, the frequencies of HEp-2–reactive and non–HEp-2–reactive clones are summarized in pie charts, with the number of antibodies tested indicated in the center. (B) The frequency of HEp-2–reactive mature naive B cells was higher in all CVID patients than was observed in healthy donors with or without one TACI mutation. (C) The frequency of HEp-2–reactive clones rose between the new emigrant/transitional and mature naive B cell stages in CVID patients with a TACI mutation, whereas it decreased in healthy carriers with one TACI mutation. Statistical significance is indicated by an unpaired or paired (for C) Student’s t test.