Serum Free Light Chains in Common Variable Immunodeficiency Disorders: Role in Differential Diagnosis and Association With Clinical Phenotype.

Cinzia Milito,Antonio Pecoraro,Federica Pulvirenti,Sara Altinier,Andrea Matucci,Isabella Quinti,Giuseppe Spadaro,Fabrizio Vianello,Alessandra Vultaggio,Angelo Vacca,Davide Firinu,Carolina Marasco,Francesco Cinetto,Marco De Carli,Roberto Ria,Carlo Agostini,Riccardo Scarpa,Mario Plebani,Nicolò Compagno

doi:10.3389/fimmu.2020.00319

Abstract

We report on an observational, multicenter study of 345 adult CVID patients, designed to assess the diagnostic value and the clinical association of serum free light chain (sFLC) pattern in Common Variable Immunodeficiency disorders (CVID). Sixty CVID patients were tested twice in order to assess intraindividual variability of sFLC. As control groups we included 138 patients affected by undefined primary antibody defects (UAD), lymphoproliferative diseases (LPDs), and secondary antibody deficiencies not related to hematological malignancies (SID). CVID patients presented lower κ and λ chain concentration compared to controls, showing low intraindividual sFLC variability. On the basis of the sFLC pattern, patients were classified into four groups: κ−λ+, κ+λ−, κ−λ−, κ+λ+. The most common pattern in CVID patients was κ−λ− (51%), followed by κ−λ+, (25%), κ+λ+ (22%), and κ+λ− (3%). In UAD, LPD, and SID groups κ+λ+ was the most common pattern observed. By analyzing the possible association between sFLC patterns and disease-related complications of CVID, we observed that patients belonging to the κ−λ− group presented more commonly unexplained enteropathy compared to the κ+λ+ group and showed higher frequency of bronchiectasis and splenomegaly compared to both the κ−λ+ and κ+λ+ patients. When compared to the other groups, κ−λ− had also lower serum IgG, IgA, and IgM concentrations at diagnosis, lower frequency of CD27+IgD–IgM– switched memory B cells, and higher frequency of CD21low B cells, receiving earlier CVID diagnosis. Thus, lower levels of sFLC might be an epiphenomenon of impairment in B cell differentiation, possibly leading κ−λ− patients to a higher risk for bacterial infections and chronic lung damage. Based on these results, we suggest adding sFLC assay to the diagnostic work-up of hypogammaglobulinemia and during follow-up. The assay may be useful to differentiate CVID from other causes of hypogammaglobulinemia and to early detect monoclonal lymphoproliferation occurring over years. Moreover, since the sFLC pattern seems to be related to disease phenotypes and clinical manifestations of CVID and after confirmation by further studies, sFLC assay might be considered a promising prognostic tool for identifying patients at higher risk of developing enteropathy and chronic lung damage or splenomegaly. This will allow designing a tailored follow-up for CVID patients.

Highlights

Common variable immunodeficiency disorder (CVID) is the most common symptomatic primary antibody deficiency (PAD) diagnosed in adulthood, affecting 1:25,000–1:50,000 patients in western countries [1, 2]
Baseline Characteristics serum FLC (sFLC) concentrations were measured in 345 CVID patients and in 138 controls (59 unclassified antibody deficiency (UAD), 41 lymphoproliferative diseases sFLC in CVID Patients (LPDs), and 38 secondary to protein loss or medications (SID) subjects)
This latter group was further divided, on the basis of the final diagnosis, into a lymphoproliferative disease group (LPD), including MM, B-CLL, Non-Hodgkin Lymphomas and MGUS, and a secondary immunodeficiency group (SID) whose hypogammaglobulinemia was not related to LPDs

Summary

BACKGROUND

Common variable immunodeficiency disorder (CVID) is the most common symptomatic primary antibody deficiency (PAD) diagnosed in adulthood, affecting 1:25,000–1:50,000 patients in western countries [1, 2]. Monoclonal increase of κ or λ chain serum levels, leading to an abnormal serum FLC ratio (FLCr), may reveal the presence of a non-secretory myeloma in case a paraprotein is absent, reducing diagnostic delay [7]. In the case of immunoglobulin light chain (AL) amyloid deposition, sFLC assay has been shown to be more sensitive for diagnostic purposes than conventional serum electrophoresis or immunofixation [5]. A significant imbalance in sFLC secretion has been suggested as a sensitive indicator of B-cell clonality and as a prognostic marker in chronic lymphocytic leukemia (B-CLL), monoclonal B-cell lymphocytosis (MBL), and some B-cell non-Hodgkin lymphomas (NHL) [8,9,10]. Simple, and reproducible indicator of B-cell biologic activity, the potentiality of sFLC assay has been more recently explored in the context of primary B-cell impairments/deficiency, including PAD and CVID. Our findings suggest a diagnostic and potential prognostic role of sFLC assay that might be taken into account when designing personalized follow-up strategies and support its inclusion in the diagnostic work-up of CVID and other forms of hypogammaglobulinemia

METHODS

Study Design

RESULTS

DISCUSSION

ETHICS STATEMENT