Effect of Leishmania infantum infection on B cell lymphopoiesis and memory in the bone marrow and spleen

Author:

Dirkx Laura1ORCID,Loyens Marlotte1ORCID,Van Acker Sara I.1ORCID,Bulté Dimitri12ORCID,Claes Mathieu1ORCID,Radwanska Magdalena34ORCID,Magez Stefan35ORCID,Caljon Guy1ORCID

Affiliation:

1. Laboratory of Microbiology, Parasitology and Hygiene (LMPH), Infla‐Med Centre of Excellence University of Antwerp Antwerp Belgium

2. San Raffaele Telethon Institute for Gene Therapy (SR‐Tiget) IRCCS San Raffaele Scientific Institute Milan Italy

3. Laboratory for Biomedical Research, Department of Environmental Technology, Food Technology and Molecular Biotechnology Ghent University Global Campus Incheon South Korea

4. Department of Biomedical Molecular Biology Ghent University Ghent Belgium

5. Brussels Center for Immunology (BCIM) Vrije Universiteit Brussel Brussels Belgium

Abstract

AbstractVisceral leishmaniasis (VL) is characterized by an uncontrolled infection of internal organs such as the spleen, liver and bone marrow (BM) and can be lethal when left untreated. No effective vaccination is currently available for humans. The importance of B cells in infection and VL protective immunity has been controversial, with both detrimental and protective effects described. VL infection was found in this study to increase not only all analyzed B cell subsets in the spleen but also the B cell progenitors in the BM. The enhanced B lymphopoiesis aligns with the clinical manifestation of polyclonal hypergammaglobulinemia and the occurrence of autoantibodies. In line with earlier reports, flow cytometric and microscopic examination identified parasite attachment to B cells of the BM and spleen without internalization, and transformation of promastigotes into amastigote morphotypes. The interaction appears independent of IgM expression and is associated with an increased detection of activated lysosomes. Furthermore, the extracellularly attached amastigotes could be efficiently transferred to infect macrophages. The observed interaction underscores the potentially crucial role of B cells during VL infection. Additionally, using immunization against a fluorescent heterologous antigen, it was shown that the infection does not impair immune memory, which is reassuring for vaccination campaigns in VL endemic areas.

Funder

Universiteit Antwerpen

Fonds Wetenschappelijk Onderzoek

Publisher

Wiley

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