Literature DB >> 33777011

Granulomatous Lymphocytic Interstitial Lung Disease (GLILD) in Common Variable Immunodeficiency (CVID): A Multicenter Retrospective Study of Patients From Italian PID Referral Centers.

Francesco Cinetto1,2, Riccardo Scarpa1,2, Maria Carrabba3, Davide Firinu4, Vassilios Lougaris5,6, Helena Buso1,2, Giulia Garzi7, Sabrina Gianese1,2, Valentina Soccodato7, Alessandra Punziano8, Gianluca Lagnese8, Giulio Tessarin5,6, Giulia Costanzo4, Nicholas Landini9, Stefania Vio10, Maria Pia Bondioni11, Dario Consonni12, Carolina Marasco13, Stefano Del Giacco4, Marcello Rattazzi1,2, Angelo Vacca13, Alessandro Plebani5,6, Giovanna Fabio3, Giuseppe Spadaro8, Carlo Agostini1,2, Isabella Quinti14, Cinzia Milito14.   

Abstract

Background: Granulomatous and Lymphocytic Interstitial Lung Diseases (GLILD) is a severe non-infectious complication of Common Variable Immunodeficiency (CVID), often associated with extrapulmonary involvement. Due to a poorly understood pathogenesis, GLILD diagnosis and management criteria still lack consensus. Accordingly, it is a relevant cause of long-term loss of respiratory function and is closely associated with a markedly reduced survival. The aim of this study was to describe clinical, immunological, laboratory and functional features of GLILD, whose combination in a predictive model might allow a timely diagnosis.
Methods: In a multicenter retrospective cross-sectional study we enrolled 73 CVID patients with radiologic features of interstitial lung disease (ILD) associated to CVID (CVID-ILD) and 125 CVID patients without ILD (controls). Of the 73 CVID-ILD patients, 47 received a definite GLILD diagnosis while 26 received a clinical-radiologic diagnosis of CVID related ILD defined as uILD.
Results: In GLILD group we found a higher prevalence of splenomegaly (84.8 vs. 39.2%), autoimmune cytopenia (59.6 vs. 6.4%) and bronchiectasis (72.3 vs. 28%), and lower IgA and IgG serum levels at CVID diagnosis. GLILD patients presented lower percentage of switched-memory B cells and marginal zone B cells, and a marked increase in the percentage of circulating CD21lo B cells (14.2 vs. 2.9%). GLILD patients also showed lower total lung capacity (TLC 87.5 vs. 5.0%) and gas transfer (DLCO 61.5 vs. 5.0%) percent of predicted. By univariate logistic regression analysis, we found IgG and IgA levels at CVID diagnosis, presence of splenomegaly and autoimmune cytopenia, CD21lo B cells percentage, TLC and DCLO percent of predicted to be associated to GLILD. The joint analysis of four variables (CD21lo B cells percentage, autoimmune cytopenia, splenomegaly and DLCO percent of predicted), together in a multiple logistic regression model, yielded an area under the ROC curve (AUC) of 0.98 (95% CI: 0.95-1.0). The AUC was only slightly modified when pooling together GLILD and uILD patients (0.92, 95% CI: 0.87-0.97). Conclusions: we propose the combination of two clinical parameters (splenomegaly and autoimmune cytopenia), one lung function index (DLCO%) and one immunologic variable (CD21lo%) as a promising tool for early identification of CVID patients with interstitial lung disease, limiting the use of aggressive diagnostic procedures.
Copyright © 2021 Cinetto, Scarpa, Carrabba, Firinu, Lougaris, Buso, Garzi, Gianese, Soccodato, Punziano, Lagnese, Tessarin, Costanzo, Landini, Vio, Bondioni, Consonni, Marasco, Del Giacco, Rattazzi, Vacca, Plebani, Fabio, Spadaro, Agostini, Quinti and Milito.

Entities:  

Keywords:  CD21lo B cells; CVID-ILD; DLCO; GLILD; autoimmune cytopenia; splenomegaly

Year:  2021        PMID: 33777011      PMCID: PMC7987811          DOI: 10.3389/fimmu.2021.627423

Source DB:  PubMed          Journal:  Front Immunol        ISSN: 1664-3224            Impact factor:   7.561


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