Pre-B cell receptor binding to galectin-1 modifies galectin-1/carbohydrate affinity to modulate specific galectin-1/glycan lattice interactions

Bonzi, Jeremy; Bornet, Olivier; Betzi, S.; Kasper, Brian; Mahal, Lara K.; Mancini, Stéphane; Schiff, Claudine; Sebban‐Kreuzer, Corinne; Guerlesquin, Françoise; Elantak, Latifa

doi:10.1038/ncomms7194

Cited by 49 publications

(44 citation statements)

References 53 publications

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“…2D and movie S3), which is best explained by the formation of complex aggregates containing pre-BCR, galectin-1, and other cell surface glycoproteins. To provide evidence that the marked slowdown of the pre-BCR bound to galectin-1 could be attributed in part to carbohydrate-mediated lattices with other glycoproteins (37), we also performed experiments in the presence of excess lactose (10 mM) to block the lectin-binding site of galectin-1 (fig. S6B).…”

Section: Resultsmentioning

confidence: 99%

Dynamic pre-BCR homodimers fine-tune autonomous survival signals in B cell precursor acute lymphoblastic leukemia

et al. 2016

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The pre-B cell receptor (pre-BCR) is an immature form of the BCR critical for early B lymphocyte development. It is composed of the membrane-bound immunoglobulin (Ig) heavy chain, surrogate light chain components, and the signaling subunits Igα and Igβ. We developed monovalent Quantum Dot (QD)-labeled probes specific for Igβ to study the behavior of pre-BCRs engaged in autonomous, ligand-independent signaling in live B cells. Single-particle tracking revealed that QD-labeled pre-BCRs engaged in transient, but frequent, homotypic interactions. Receptor motion was correlated at short separation distances, consistent with the formation of dimers and higher-order oligomers. Repeated encounters between diffusing pre-BCRs appeared to reflect transient co-confinement in plasma membrane domains. In human B cell precursor acute lymphoblastic leukemia (BCP-ALL) cells, we showed that frequent, short-lived, homotypic pre-BCR interactions stimulated survival signals, including expression of BCL6, which encodes a transcriptional repressor. These survival signals were blocked by inhibitory monovalent antigen-binding antibody fragments (Fabs) specific for the surrogate light chain components of the pre-BCR or by inhibitors of the tyrosine kinases Lyn and Syk. For comparison, we evaluated pre-BCR aggregation mediated by dimeric galectin-1, which has binding sites for carbohydrate and for the λ5 component of the surrogate light chain. Galectin-1 binding resulted in the formation of large, highly immobile pre-BCR aggregates, which was partially relieved by the addition of lactose to prevent the crosslinking of galectin-BCR complexes to other glycosylated membrane components. Analysis of the pre-BCR and its signaling partners suggested that they could be potential targets for combination therapy in BCP-ALL.

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Section: Resultsmentioning

confidence: 99%

Dynamic pre-BCR homodimers fine-tune autonomous survival signals in B cell precursor acute lymphoblastic leukemia

et al. 2016

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“…Gal-1 recognizes multiple galactose-b1-4-N-acetyl-glucosamine (N-acetyl-lactosamine [LacNAc]) units present on the branches of N-or O-linked glycans on diverse cell surface receptors, including CD45, CD43, CD69, pre-BCR, and vascular endothelial growth factor R2 (11,(19)(20)(21). Different glycosyltransferases act in concert to create Gal-1-specific ligands, including N-acetylglucosaminyltransferase 5 (MGAT5), an enzyme that generates b1,6-N-acetylglucosamine-branched complex N-glycans and the core-2 b1-6-N-acetylglucosaminyltransferase 1 (C2GNT1), an enzyme that catalyzes branching of core-2 O-glycans.…”

Section: Gal-1: a Sweet Checkpoint In The Resolution Of Inflammatorymentioning

confidence: 99%

Galectin-1: A Jack-of-All-Trades in the Resolution of Acute and Chronic Inflammation

Sundblad

Morosi

Geffner

et al. 2017

The Journal of Immunology

152

136

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Regulatory signals provide negative input to immunological networks promoting resolution of acute and chronic inflammation. Galectin-1 (Gal-1), a member of a family of evolutionarily conserved glycan-binding proteins, displays broad anti-inflammatory and proresolving activities by targeting multiple immune cell types. Within the innate immune compartment, Gal-1 acts as a resolution-associated molecular pattern by counteracting the synthesis of proinflammatory cytokines, inhibiting neutrophil trafficking, targeting eosinophil migration and survival, and suppressing mast cell degranulation. Likewise, this lectin controls T cell and B cell compartments by modulating receptor clustering and signaling, thus serving as a negative-regulatory checkpoint that reprograms cellular activation, differentiation, and survival. In this review, we discuss the central role of Gal-1 in regulatory programs operating during acute inflammation, autoimmune diseases, allergic inflammation, pregnancy, cancer, and infection. Therapeutic strategies aimed at targeting Gal-1-glycan interactions will contribute to overcome cancer immunosuppression and reinforce antimicrobial immunity, whereas stimulation of Gal-1-driven immunoregulatory circuits will help to mitigate exuberant inflammation.

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“…Following antigen challenge, Gal-3 deficiency led to enhanced plasma cell differentiation and unleashed immunoglobulin production, both in B1 and B2 cells [87,88]. Finally, elegant studies reported that, during B-cell development, Gal-1 secreted by bone marrow stromal cells acts as a pre-B cell receptor ligand to modulate B cell maturation through mechanisms involving displacement of Gal-1/glycan lattices and shift toward a glycosylation-independent Gal-1-mediated protein-protein interaction [89]. Thus, although not investigated in such detail as the T cell compartment, these studies suggest that galectins may play different regulatory roles during the lifespan of B cells, targeting their maturation, differentiation, signaling, tolerance and survival.…”

Section: Regulatory B Cellsmentioning

confidence: 99%

Re‐wiring regulatory cell networks in immunity by galectin–glycan interactions

et al. 2015

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Edited by Wilhelm JustKeywords: Galectin Regulatory T cell Tolerogenic dendritic cell M2-type macrophage Myeloid-derived suppressor cell Immunosuppression a b s t r a c tPrograms that control immune cell homeostasis are orchestrated through the coordinated action of a number of regulatory cell populations, including regulatory T cells, regulatory B cells, myeloidderived suppressor cells, alternatively-activated macrophages and tolerogenic dendritic cells. These regulatory cell populations can prevent harmful inflammation following completion of protective responses and thwart the development of autoimmune pathology. However, they also have a detrimental role in cancer by favoring escape from immune surveillance. One of the hallmarks of regulatory cells is their remarkable plasticity as they can be positively or negatively modulated by a plethora of cytokines, growth factors and co-stimulatory signals that tailor their differentiation, stability and survival. Here we focus on the emerging roles of galectins, a family of highly conserved glycan-binding proteins in regulating the fate and function of regulatory immune cell populations, both of lymphoid and myeloid origins. Given the broad distribution of circulating and tissue-specific galectins, understanding the relevance of lectin-glycan interactions in shaping regulatory cell compartments will contribute to the design of novel therapeutic strategies aimed at modulating their function in a broad range of immunological disorders.

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Pre-B cell receptor binding to galectin-1 modifies galectin-1/carbohydrate affinity to modulate specific galectin-1/glycan lattice interactions

Cited by 49 publications

References 53 publications

Dynamic pre-BCR homodimers fine-tune autonomous survival signals in B cell precursor acute lymphoblastic leukemia

Dynamic pre-BCR homodimers fine-tune autonomous survival signals in B cell precursor acute lymphoblastic leukemia

Galectin-1: A Jack-of-All-Trades in the Resolution of Acute and Chronic Inflammation

Re‐wiring regulatory cell networks in immunity by galectin–glycan interactions

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