We investigated several phenotypic and functional parameters of T cell-mediated immunity in a large series of common variable immunodeficiency (CVID) patients. We demonstrated that the vast majority of CVID patients presented multiple T cell abnormalities intimately related among them, the severity of which was reflected in a parallel loss of CD4(+) naive T cells. A strong correlation between the number of CD4(+) naive T cells and clinical. features was observed, supporting the subgrouping of patients according to their number of naive CD4(+) T lymphocytes. A reduced thymic output and disrupted CD4(+) and CD8(+) TCR repertoires paralleled the contraction of CD4(+) naive T cell pools. The evaluation of activation markers and cytokine production indicated a strong T cell activation that was significantly related to the increased levels of T cell turnover and apoptosis. Finally, discrete genetic profiles could be demonstrated in groups of patients showing extremely diverse T cell subset composition and function. Naive CD4(+) T cell levels were significantly associated with the switched memory B cell-based classification, although the concordance between the respective subgroups did not exceed 58.8%. In conclusion, our data highlight the key role played by the T cell compartment in the pathogenesis of CVID, pointing to the need to consider this aspect for classification of this disease.
Unravelling the complexity of T cell abnormalities in common variable immunodeficiency / A., Giovannetti; M., Pierdominici; F., Mazzetta; M., Marziali; C., Renzi; A. M., Mileo; M., De Felice; B., Mora; A., Esposito; R., Carello; Pizzuti, Antonio; M. G., Paggi; R., Paganelli; W., Malorni; F., Aiuti. - In: JOURNAL OF IMMUNOLOGY. - ISSN 0022-1767. - 178:6(2007), pp. 3932-3943.
Unravelling the complexity of T cell abnormalities in common variable immunodeficiency
PIZZUTI, Antonio;
2007
Abstract
We investigated several phenotypic and functional parameters of T cell-mediated immunity in a large series of common variable immunodeficiency (CVID) patients. We demonstrated that the vast majority of CVID patients presented multiple T cell abnormalities intimately related among them, the severity of which was reflected in a parallel loss of CD4(+) naive T cells. A strong correlation between the number of CD4(+) naive T cells and clinical. features was observed, supporting the subgrouping of patients according to their number of naive CD4(+) T lymphocytes. A reduced thymic output and disrupted CD4(+) and CD8(+) TCR repertoires paralleled the contraction of CD4(+) naive T cell pools. The evaluation of activation markers and cytokine production indicated a strong T cell activation that was significantly related to the increased levels of T cell turnover and apoptosis. Finally, discrete genetic profiles could be demonstrated in groups of patients showing extremely diverse T cell subset composition and function. Naive CD4(+) T cell levels were significantly associated with the switched memory B cell-based classification, although the concordance between the respective subgroups did not exceed 58.8%. In conclusion, our data highlight the key role played by the T cell compartment in the pathogenesis of CVID, pointing to the need to consider this aspect for classification of this disease.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
