Lack of galectin-3 up-regulates IgA expression by peritoneal B1 lymphocytes during B cell differentiation

Oliveira, Felipe Leite de; Bernardes, Emerson Soares; Brand, Camila; Santos, Sofia Nascimento dos; Cabanel, Mariana; Arcanjo, Katia; Brito, José M.; Borojević, Radovan; Chammas, Roger; El-Cheikh, Márcia Cury

doi:10.1007/s00441-015-2203-y

Cited by 14 publications

(12 citation statements)

References 47 publications

(53 reference statements)

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“…Gal-3 has been described as significant regulator of B cell differentiation 3 , 4 , 7 , 8 . However, the molecular and cellular mechanisms involved are poorly understood.…”

Section: Discussionmentioning

confidence: 99%

“…In non-conventional peritoneal B1 lymphocytes biology, gal-3 also plays regulatory roles in the differentiation of both B1a and B1b cells into plasma cells by IL-5 and Blimp-1 signaling-dependent manner 5 . Clearly, gal-3 interferes with B cell compartments in distinct lymphoid organs 4 – 8 . However, the mechanisms that correlate gal-3 with molecular pathways during bone marrow B lymphopoiesis, peripheral mobilization and settlement mainly in the spleen, are poorly understood.…”

Section: Introductionmentioning

confidence: 99%

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Lack of galectin-3 modifies differentially Notch ligands in bone marrow and spleen stromal cells interfering with B cell differentiation

Oliveira

Santos

Ricon

et al. 2018

Sci Rep

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Galectin-3 (Gal-3) is a β-galactoside binding protein that controls cell-cell and cell-extracellular matrix interactions. In lymphoid organs, gal-3 inhibits B cell differentiation by mechanisms poorly understood. The B cell development is dependent on tissue organization and stromal cell signaling, including IL-7 and Notch pathways. Here, we investigate possible mechanisms that gal-3 interferes during B lymphocyte differentiation in the bone marrow (BM) and spleen. The BM of gal-3-deficient mice (Lgals3−/− mice) was evidenced by elevated numbers of B220+CD19+c-Kit+IL-7R+ progenitor B cells. In parallel, CD45− bone marrow stromal cells expressed high levels of mRNA IL-7, Notch ligands (Jagged-1 and Delta-like 4), and transcription factors (Hes-1, Hey-1, Hey-2 and Hey-L). The spleen of Lgals3−/− mice was hallmarked by marginal zone disorganization, high number of IgM+IgD+ B cells and CD138+ plasma cells, overexpression of Notch ligands (Jagged-1, Delta-like 1 and Delta-like 4) by stromal cells and Hey-1. Morever, IgM+IgD+ B cells and B220+CD138+ CXCR4+ plasmablasts were significantly increased in the BM and blood of Lgals3−/− mice. For the first time, we demonstrated that gal-3 inhibits Notch signaling activation in lymphoid organs regulating earlier and terminal events of B cell differentiation.

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“…Gal-3 has been described as significant regulator of B cell differentiation 3 , 4 , 7 , 8 . However, the molecular and cellular mechanisms involved are poorly understood.…”

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Lack of galectin-3 modifies differentially Notch ligands in bone marrow and spleen stromal cells interfering with B cell differentiation

Oliveira

Santos

Ricon

et al. 2018

Sci Rep

Self Cite

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“…An inhibitory role of galectin-3 was demonstrated in a model of galectin-3 knockout mouse, where B lymphocytes of the peritoneal cavity favored differentiating into plasma cells [ 153 ]. More specifically, a significant increase of IgA-producing cells in the peritoneal cavity was observed in comparison to galectin-3-expressing mice during chronic schistosomiasis as well as in response to interleukin-5 and transforming growth factor-β [ 154 ]. Although the mechanisms of galectin-3-dependent inhibition of B cell differentiation are obscure, a recent study revealed that Notch signaling pathways might play an important regulatory role [ 155 ].…”

Section: Galectin-3mentioning

confidence: 99%

The Emerging Role of Galectins and O-GlcNAc Homeostasis in Processes of Cellular Differentiation

Tazhitdinova

Timoshenko

2020

Cells

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Galectins are a family of soluble β-galactoside-binding proteins with diverse glycan-dependent and glycan-independent functions outside and inside the cell. Human cells express twelve out of sixteen recognized mammalian galectin genes and their expression profiles are very different between cell types and tissues. In this review, we summarize the current knowledge on the changes in the expression of individual galectins at mRNA and protein levels in different types of differentiating cells and the effects of recombinant galectins on cellular differentiation. A new model of galectin regulation is proposed considering the change in O-GlcNAc homeostasis between progenitor/stem cells and mature differentiated cells. The recognition of galectins as regulatory factors controlling cell differentiation and self-renewal is essential for developmental and cancer biology to develop innovative strategies for prevention and targeted treatment of proliferative diseases, tissue regeneration, and stem-cell therapy.

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“…In accordance, B1 cells may modulate their adhesion molecules and differentiate into plasma cells still in the peritoneal cavity. On the other hand, these cells can adhere to mesenteric membranes or omentum, as described in the literature, if previously activated by the absence of galectin-3 [26].…”

Section: B1 Cellmentioning

confidence: 91%

“…In addition to the constitutive expression of STAT3 by B1 cells, and in contrast to B2 cells, these cells also express the interleukin-5 receptor alpha (IL-R5α) chain, which renders to this subset the ability to specifically respond to interleukin 5 (IL-5), GM-CSF, and IL-3 [29]. In this way, B1 lymphocytes can be maintained in vitro if properly stimulated by IL-5 allowing the analysis of their behavior such as the proliferation rate, survival, and/or differentiation into Ig-producing cells and IgA switch under experimental conditions [26,30,31].…”

Section: B1 Cellmentioning

confidence: 99%

Epigenetic Therapy as a Putative Molecular Target to Modulate B Cell Biology and Behavior in the Context of Immunological Disorders

Costa

El-Cheikh

Carneiro

2020

Journal of Immunology Research

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Histone Deacetylase- (HDAC-) dependent epigenetic mechanisms have been widely explored in the last decade in different types of malignancies in preclinical studies. This effort led to the discovery and development of a range of new HDAC inhibitors (iHDAC) with different chemical properties and selective abilities. In fact, hematological malignancies were the first ones to have new iHDACs approved for clinical use, such as Vorinostat and Romidepsin for cutaneous T cell lymphoma and panobinostat for multiple myeloma. Besides these promising already approved iHDACs, we highlight a range of studies focusing on the HDAC-dependent epigenetic control of B cell development, behavior, and/or function. Here, we highlight 21 iHDACs which have been studied in the literature in the context of B cell development and/or dysfunction mostly focused on B cell lymphomagenesis. Regardless, we have identified 55 clinical trials using 6 out of 21 iHDACs to approach their putative roles on B cell malignancies; none of them focuses on peritoneal B cell populations. Since cells belonging to this peculiar body compartment, named B1 cells, may contribute to the development of autoimmune pathologies, such as lupus, a better understanding of the HDAC-dependent epigenetic mechanisms that control its biology and behavior might shed light on iHDAC use to manage these immunological dysfunctions. In this sense, iHDACs might emerge as a promising new approach for translational studies in this field. In this review, we discuss a putative role of iHDACs in the modulation of peritoneal B cell subpopulation’s balance as well as their role as therapeutic agents in the context of chronic diseases mediated by peritoneal B cells.

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Lack of galectin-3 up-regulates IgA expression by peritoneal B1 lymphocytes during B cell differentiation

Cited by 14 publications

References 47 publications

Lack of galectin-3 modifies differentially Notch ligands in bone marrow and spleen stromal cells interfering with B cell differentiation

Lack of galectin-3 modifies differentially Notch ligands in bone marrow and spleen stromal cells interfering with B cell differentiation

The Emerging Role of Galectins and O-GlcNAc Homeostasis in Processes of Cellular Differentiation

Epigenetic Therapy as a Putative Molecular Target to Modulate B Cell Biology and Behavior in the Context of Immunological Disorders

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