Tracing CLL-biased Stereotyped Immunoglobulin Gene Rearrangements in Normal B Cell Subsets Using a High-throughput Immunogenetic Approach

Overview

Journal Mol Med

Publisher Biomed Central

Specialties General Medicine
Molecular Biology

Date 2020 Mar 12

PMID 32156260

Citations 13

Authors

Monica Colombo

Davide Bagnara

Daniele Reverberi

Serena Matis

Martina Cardillo

Rosanna Massara

Luca Mastracci

Jean Louis Ravetti

Luca Agnelli

Antonino Neri

Michela Mazzocco

Margherita Squillario

Andrea Nicola Mazzarello

Giovanna Cutrona

Andreas Agathangelidis

Kostas Stamatopoulos

Manlio Ferrarini

Franco Fais

Affiliations

Soon will be listed here.

Abstract

Background: B cell receptor Immunoglobulin (BcR IG) repertoire of Chronic Lymphocytic Leukemia (CLL) is characterized by the expression of quasi-identical BcR IG. These are observed in approximately 30% of patients, defined as stereotyped receptors and subdivided into subsets based on specific VH CDR3 aa motifs and phylogenetically related IGHV genes. Although relevant to CLL ontogeny, the distribution of CLL-biased stereotyped immunoglobulin rearrangements (CBS-IG) in normal B cells has not been so far specifically addressed using modern sequencing technologies. Here, we have investigated the presence of CBS-IG in splenic B cell subpopulations (s-BCS) and in CD5 and CD5 B cells from the spleen and peripheral blood (PB).

Methods: Fractionation of splenic B cells into 9 different B cell subsets and that of spleen and PB into CD5 and CD5 cells were carried out by FACS sorting. cDNA sequences of BcR IG gene rearrangements were obtained by NGS. Identification of amino acidic motifs typical of CLL stereotyped subsets was carried out on IGHV1-carrying gene sequences and statistical evaluation has been subsequently performed to assess stereotypes distribution.

Results: CBS-IG represented the 0.26% average of IGHV1 genes expressing sequences, were detected in all of the BCS investigated. CBS-IG were more abundant in splenic and circulating CD5 B (0.57%) cells compared to CD5 B cells (0.17%). In all instances, most CBS IG did not exhibit somatic hypermutation similar to CLL stereotyped receptors. However, compared to CLL, they exhibited a different CLL subset distribution and a broader utilization of the genes of the IGHV1 family.

Conclusions: CBS-IG receptors appear to represent a part of the "public" BcR repertoire in normal B cells. This repertoire is observed in all BCS excluding the hypothesis that CLL stereotyped BcR accumulate in a specific B cell subset, potentially capable of originating a leukemic clone. The different relative representation of CBS-IG in normal B cell subgroups suggests the requirement for additional selective processes before a full transformation into CLL is achieved.

Citing Articles

Stereotyped B-Cell Receptor Immunoglobulins in B-Cell Lymphomas.

Agathangelidis A, Roussos A, Kardamiliotis K, Psomopoulos F, Stamatopoulos K Methods Mol Biol. 2024; 2865:125-143.

PMID: 39424723 DOI: 10.1007/978-1-0716-4188-0_6.

CLL stereotyped B-cell receptor immunoglobulin sequences are recurrent in the B-cell repertoire of healthy individuals: Apparent lack of central and early peripheral tolerance censoring.

Vergani S, Bagnara D, Agathangelidis A, Ng A, Ferrer G, Mazzarello A Front Oncol. 2023; 13:1112879.

PMID: 37007084 PMC: 10063922. DOI: 10.3389/fonc.2023.1112879.

Characterization of clonal immunoglobulin heavy V-D-J gene rearrangements in Chinese patients with chronic lymphocytic leukemia: Clinical features and molecular profiles.

Deng X, Zhang M, Wang J, Zhou X, Xiao M Front Oncol. 2023; 13:1120867.

PMID: 36874132 PMC: 9978106. DOI: 10.3389/fonc.2023.1120867.

Old and New Facts and Speculations on the Role of the B Cell Receptor in the Origin of Chronic Lymphocytic Leukemia.

Bagnara D, Mazzarello A, Ghiotto F, Colombo M, Cutrona G, Fais F Int J Mol Sci. 2022; 23(22).

PMID: 36430731 PMC: 9693457. DOI: 10.3390/ijms232214249.

Characterizing Features of Human Circulating B Cells Carrying CLL-Like Stereotyped Immunoglobulin Rearrangements.

Bagnara D, Colombo M, Reverberi D, Matis S, Massara R, Cardente N Front Oncol. 2022; 12:894419.

PMID: 35837088 PMC: 9275393. DOI: 10.3389/fonc.2022.894419.

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