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Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools

INTRODUCTION: Common Variable Immunodeficiency (CVID) is characterized by defective antibody production and hypogammaglobulinemia. Flow cytometry immunophenotyping of blood lymphocytes has become of great relevance for the diagnosis and classification of CVID, due to an impaired differentiation of m...

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Autores principales: del Pino-Molina, Lucía, López-Granados, Eduardo, Lecrevisse, Quentin, Torres Canizales, Juan, Pérez-Andrés, Martín, Blanco, Elena, Wentink, Marjolein, Bonroy, Carolien, Nechvatalova, Jana, Milota, Tomas, Kienzler, Anne-Kathrin, Philippé, Jan, Sousa, Ana E., van der Burg, Mirjam, Kalina, Tomas, van Dongen, Jacques J.M., Orfao, Alberto
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7925888/
https://www.ncbi.nlm.nih.gov/pubmed/33679693
http://dx.doi.org/10.3389/fimmu.2020.603972
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author del Pino-Molina, Lucía
López-Granados, Eduardo
Lecrevisse, Quentin
Torres Canizales, Juan
Pérez-Andrés, Martín
Blanco, Elena
Wentink, Marjolein
Bonroy, Carolien
Nechvatalova, Jana
Milota, Tomas
Kienzler, Anne-Kathrin
Philippé, Jan
Sousa, Ana E.
van der Burg, Mirjam
Kalina, Tomas
van Dongen, Jacques J.M.
Orfao, Alberto
author_facet del Pino-Molina, Lucía
López-Granados, Eduardo
Lecrevisse, Quentin
Torres Canizales, Juan
Pérez-Andrés, Martín
Blanco, Elena
Wentink, Marjolein
Bonroy, Carolien
Nechvatalova, Jana
Milota, Tomas
Kienzler, Anne-Kathrin
Philippé, Jan
Sousa, Ana E.
van der Burg, Mirjam
Kalina, Tomas
van Dongen, Jacques J.M.
Orfao, Alberto
author_sort del Pino-Molina, Lucía
collection PubMed
description INTRODUCTION: Common Variable Immunodeficiency (CVID) is characterized by defective antibody production and hypogammaglobulinemia. Flow cytometry immunophenotyping of blood lymphocytes has become of great relevance for the diagnosis and classification of CVID, due to an impaired differentiation of mature post-germinal-center (GC) class-switched memory B-cells (MBC) and severely decreased plasmablast/plasma cell (Pb) counts. Here, we investigated in detail the pre-GC B-cell maturation compartment in blood of CVID patients. METHODS: In this collaborative multicentric study the EuroFlow PID 8-color Pre-GC B-cell tube, standardized sample preparation procedures (SOPs) and innovative data analysis tools, were used to characterize the maturation profile of pre-GC B-cells in 100 CVID patients, vs 62 age-matched healthy donors (HD). RESULTS: The Pre-GC B-cell tube allowed identification within pre-GC B-cells of three subsets of maturation associated immature B-cells and three subpopulations of mature naïve B-lymphocytes. CVID patients showed overall reduced median absolute counts (vs HD) of the two more advanced stages of maturation of both CD5(+) CD38(+/++) CD21(het) CD24(++) (2.7 vs 5.6 cells/µl, p=0.0004) and CD5(+) CD38(het) CD21(+) CD24(+) (6.5 vs 17 cells/µl, p<0.0001) immature B cells (below normal HD levels in 22% and 37% of CVID patients). This was associated with an expansion of CD21(-)CD24(-) (6.1 vs 0.74 cells/µl, p<0.0001) and CD21(-)CD24(++) (1.8 vs 0.4 cells/µl, p<0.0001) naïve B-cell counts above normal values in 73% and 94% cases, respectively. Additionally, reduced IgMD(+) (21 vs 32 cells/µl, p=0.03) and IgMD(-) (4 vs 35 cells/µl, p<0.0001) MBC counts were found to be below normal values in 25% and 77% of CVID patients, respectively, always together with severely reduced/undetectable circulating blood pb. Comparison of the maturation pathway profile of pre-GC B cells in blood of CVID patients vs HD using EuroFlow software tools showed systematically altered patterns in CVID. These consisted of: i) a normally-appearing maturation pathway with altered levels of expression of >1 (CD38, CD5, CD19, CD21, CD24, and/or smIgM) phenotypic marker (57/88 patients; 65%) for a total of 3 distinct CVID patient profiles (group 1: 42/88 patients, 48%; group 2: 8/88, 9%; and group 3: 7/88, 8%) and ii) CVID patients with a clearly altered pre-GC B cell maturation pathway in blood (group 4: 31/88 cases, 35%). CONCLUSION: Our results show that maturation of pre-GC B-cells in blood of CVID is systematically altered with up to four distinctly altered maturation profiles. Further studies, are necessary to better understand the impact of such alterations on the post-GC defects and the clinical heterogeneity of CVID.
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spelling pubmed-79258882021-03-04 Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools del Pino-Molina, Lucía López-Granados, Eduardo Lecrevisse, Quentin Torres Canizales, Juan Pérez-Andrés, Martín Blanco, Elena Wentink, Marjolein Bonroy, Carolien Nechvatalova, Jana Milota, Tomas Kienzler, Anne-Kathrin Philippé, Jan Sousa, Ana E. van der Burg, Mirjam Kalina, Tomas van Dongen, Jacques J.M. Orfao, Alberto Front Immunol Immunology INTRODUCTION: Common Variable Immunodeficiency (CVID) is characterized by defective antibody production and hypogammaglobulinemia. Flow cytometry immunophenotyping of blood lymphocytes has become of great relevance for the diagnosis and classification of CVID, due to an impaired differentiation of mature post-germinal-center (GC) class-switched memory B-cells (MBC) and severely decreased plasmablast/plasma cell (Pb) counts. Here, we investigated in detail the pre-GC B-cell maturation compartment in blood of CVID patients. METHODS: In this collaborative multicentric study the EuroFlow PID 8-color Pre-GC B-cell tube, standardized sample preparation procedures (SOPs) and innovative data analysis tools, were used to characterize the maturation profile of pre-GC B-cells in 100 CVID patients, vs 62 age-matched healthy donors (HD). RESULTS: The Pre-GC B-cell tube allowed identification within pre-GC B-cells of three subsets of maturation associated immature B-cells and three subpopulations of mature naïve B-lymphocytes. CVID patients showed overall reduced median absolute counts (vs HD) of the two more advanced stages of maturation of both CD5(+) CD38(+/++) CD21(het) CD24(++) (2.7 vs 5.6 cells/µl, p=0.0004) and CD5(+) CD38(het) CD21(+) CD24(+) (6.5 vs 17 cells/µl, p<0.0001) immature B cells (below normal HD levels in 22% and 37% of CVID patients). This was associated with an expansion of CD21(-)CD24(-) (6.1 vs 0.74 cells/µl, p<0.0001) and CD21(-)CD24(++) (1.8 vs 0.4 cells/µl, p<0.0001) naïve B-cell counts above normal values in 73% and 94% cases, respectively. Additionally, reduced IgMD(+) (21 vs 32 cells/µl, p=0.03) and IgMD(-) (4 vs 35 cells/µl, p<0.0001) MBC counts were found to be below normal values in 25% and 77% of CVID patients, respectively, always together with severely reduced/undetectable circulating blood pb. Comparison of the maturation pathway profile of pre-GC B cells in blood of CVID patients vs HD using EuroFlow software tools showed systematically altered patterns in CVID. These consisted of: i) a normally-appearing maturation pathway with altered levels of expression of >1 (CD38, CD5, CD19, CD21, CD24, and/or smIgM) phenotypic marker (57/88 patients; 65%) for a total of 3 distinct CVID patient profiles (group 1: 42/88 patients, 48%; group 2: 8/88, 9%; and group 3: 7/88, 8%) and ii) CVID patients with a clearly altered pre-GC B cell maturation pathway in blood (group 4: 31/88 cases, 35%). CONCLUSION: Our results show that maturation of pre-GC B-cells in blood of CVID is systematically altered with up to four distinctly altered maturation profiles. Further studies, are necessary to better understand the impact of such alterations on the post-GC defects and the clinical heterogeneity of CVID. Frontiers Media S.A. 2021-02-17 /pmc/articles/PMC7925888/ /pubmed/33679693 http://dx.doi.org/10.3389/fimmu.2020.603972 Text en Copyright © 2021 del Pino-Molina, López-Granados, Lecrevisse, Torres Canizales, Pérez-Andrés, Blanco, Wentink, Bonroy, Nechvatalova, Milota, Kienzler, Philippé, Sousa, van der Burg, Kalina, van Dongen and Orfao http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
del Pino-Molina, Lucía
López-Granados, Eduardo
Lecrevisse, Quentin
Torres Canizales, Juan
Pérez-Andrés, Martín
Blanco, Elena
Wentink, Marjolein
Bonroy, Carolien
Nechvatalova, Jana
Milota, Tomas
Kienzler, Anne-Kathrin
Philippé, Jan
Sousa, Ana E.
van der Burg, Mirjam
Kalina, Tomas
van Dongen, Jacques J.M.
Orfao, Alberto
Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title_full Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title_fullStr Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title_full_unstemmed Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title_short Dissection of the Pre-Germinal Center B-Cell Maturation Pathway in Common Variable Immunodeficiency Based on Standardized Flow Cytometric EuroFlow Tools
title_sort dissection of the pre-germinal center b-cell maturation pathway in common variable immunodeficiency based on standardized flow cytometric euroflow tools
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7925888/
https://www.ncbi.nlm.nih.gov/pubmed/33679693
http://dx.doi.org/10.3389/fimmu.2020.603972
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