Background: Chronic granulomatous disease (CGD) is a primary immune deficiency characterized by a defect in reactive oxygen species production. Although the effect of CGD mainly reflects on the phagocytic compartment, B-cell responses are also impaired in patients with CGD. Objective: We sought to investigate how defective gp91phox expression in patients with CGD and CGD carriers might affect the B-cell compartment and maintenance of long-term memory. Methods: We studied the B-cell compartment of patients with CGD in terms of phenotype and ability to produce reactive oxygen species and proliferate on stimuli differently directed to the B-cell receptor and Toll-like receptor 9. We further studied their capacity to maintain long-term memory by measuring cellular and serologic responses to measles. Results: We show that the memory B-cell compartment is impaired among patients with CGD, as indicated by reduced total (CD191CD271) and resting (CD191CD271CD211) memory B cells in parallel to increased naive (CD191CD272IgD1) B-cell frequencies. Data on CGD carriers reveal that such alterations are related to gp91phox expression. Moreover, proliferative capabilities of B cells on selective in vitro stimulation of B-cell receptor or Toll-like receptor 9 pathways were reduced in patients with CGD compared with those seen in age-matched healthy control subjects. Significantly lower measles-specific antibody levels and antibody-secreting cell numbers were also observed, indicating a poor ability to maintain long-term memory in these patients. Conclusion: Altogether, our data suggest that patients with CGD present a defective B-cell compartment in terms of frequencies of memory B cells, response to in vitro stimulation, and maintenance of long-term antigen-specific memory.

Cotugno, N., Finocchi, A., Cagigi, A., DI MATTEO, G., Chiriaco, M., DI CESARE, S., et al. (2014). Defective B-cell proliferation and maintenance of long-term memory in patients with chronic granulomatous disease. JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY [10.1016/j.jaci.2014.07.012].

Defective B-cell proliferation and maintenance of long-term memory in patients with chronic granulomatous disease

Cotugno, N;FINOCCHI, ANDREA;DI MATTEO, GIGLIOLA;DI CESARE, SILVIA;ROSSI, PAOLO;AIUTI, ALESSANDRO;Palma, P;
2014-08-29

Abstract

Background: Chronic granulomatous disease (CGD) is a primary immune deficiency characterized by a defect in reactive oxygen species production. Although the effect of CGD mainly reflects on the phagocytic compartment, B-cell responses are also impaired in patients with CGD. Objective: We sought to investigate how defective gp91phox expression in patients with CGD and CGD carriers might affect the B-cell compartment and maintenance of long-term memory. Methods: We studied the B-cell compartment of patients with CGD in terms of phenotype and ability to produce reactive oxygen species and proliferate on stimuli differently directed to the B-cell receptor and Toll-like receptor 9. We further studied their capacity to maintain long-term memory by measuring cellular and serologic responses to measles. Results: We show that the memory B-cell compartment is impaired among patients with CGD, as indicated by reduced total (CD191CD271) and resting (CD191CD271CD211) memory B cells in parallel to increased naive (CD191CD272IgD1) B-cell frequencies. Data on CGD carriers reveal that such alterations are related to gp91phox expression. Moreover, proliferative capabilities of B cells on selective in vitro stimulation of B-cell receptor or Toll-like receptor 9 pathways were reduced in patients with CGD compared with those seen in age-matched healthy control subjects. Significantly lower measles-specific antibody levels and antibody-secreting cell numbers were also observed, indicating a poor ability to maintain long-term memory in these patients. Conclusion: Altogether, our data suggest that patients with CGD present a defective B-cell compartment in terms of frequencies of memory B cells, response to in vitro stimulation, and maintenance of long-term antigen-specific memory.
29-ago-2014
In corso di stampa
Rilevanza internazionale
Articolo
Comitato scientifico
Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA
English
Con Impact Factor ISI
measles; proliferation; long-term memory; reactive oxygen species deficiency; memory B-cell compartment; Chronic granulomatous disease; B cell
European research projects on rare diseases, Italian Ministry of Health (
Cotugno, N., Finocchi, A., Cagigi, A., DI MATTEO, G., Chiriaco, M., DI CESARE, S., et al. (2014). Defective B-cell proliferation and maintenance of long-term memory in patients with chronic granulomatous disease. JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY [10.1016/j.jaci.2014.07.012].
Cotugno, N; Finocchi, A; Cagigi, A; DI MATTEO, G; Chiriaco, M; DI CESARE, S; Rossi, P; Aiuti, A; Palma, P; Douagi, I
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/100772
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