Molecular and cytogenetic characterization of expanded B-cell clones from multiclonal versus monoclonal B-cell chronic lymphoproliferative disorders
Ana Henriques,
Arancha Rodríguez-Caballero,
Ignacio Criado,
Anton W. Langerak,
Wendy G. Nieto,
Quentin Lécrevisse,
Marcos González,
Emília Cortesão,
Artur Paiva,
Julia Almeida,
Alberto Orfao
Affiliations
Ana Henriques
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain;Blood and Transplantation Center of Coimbra/Portuguese Institute of Blood and Transplantation, Portugal
Arancha Rodríguez-Caballero
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Ignacio Criado
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Anton W. Langerak
Department of Immunology, Erasmus MC, University Medical Center Rotterdam, the Netherlands
Wendy G. Nieto
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Quentin Lécrevisse
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Marcos González
Service of Hematology, University Hospital of Salamanca, IBMCC, IBSAL and Department of Medicine, University of Salamanca, Spain
Emília Cortesão
Service of Hematology, University Hospital Center of Coimbra, Portugal
Artur Paiva
Blood and Transplantation Center of Coimbra/Portuguese Institute of Blood and Transplantation, Portugal
Julia Almeida
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Alberto Orfao
Cancer Research Center (IBMCC, USAL-CSIC), Department of Medicine and Cytometry Service (NUCLEUS), University of Salamanca and Institute for Biomedical Research of Salamanca, Salamanca, Spain
Chronic antigen-stimulation has been recurrently involved in the earlier stages of monoclonal B-cell lymphocytosis, chronic lymphocytic leukemia and other B-cell chronic lymphoproliferative disorders. The expansion of two or more B-cell clones has frequently been reported in individuals with these conditions; potentially, such coexisting clones have a greater probability of interaction with common immunological determinants. Here, we analyzed the B-cell receptor repertoire and molecular profile, as well as the phenotypic, cytogenetic and hematologic features, of 228 chronic lymphocytic leukemia-like and non-chronic lymphocytic leukemia-like clones comparing multiclonal (n=85 clones from 41 cases) versus monoclonal (n=143 clones) monoclonal B-cell lymphocytosis, chronic lymphocytic leukemia and other B-cell chronic lymphoproliferative disorders. The B-cell receptor of B-cell clones from multiclonal cases showed a slightly higher degree of HCDR3 homology than B-cell clones from mono clonal cases, in association with unique hematologic (e.g. lower B-lymphocyte counts) and cytogenetic (e.g. lower frequency of cytogenetically altered clones) features usually related to earlier stages of the disease. Moreover, a subgroup of coexisting B-cell clones from individual multiclonal cases which were found to be phylogenetically related showed unique molecular and cytogenetic features: they more frequently shared IGHV3 gene usage, shorter HCDR3 sequences with a greater proportion of IGHV mutations and del(13q14.3), than other unrelated B-cell clones. These results would support the antigen-driven nature of such multiclonal B-cell expansions, with potential involvement of multiple antigens/epitopes.
