Functions of galectins as ‘self/non-self’-recognition and effector factors

Vasta, Gerardo R.; Feng, Chiguang; González-Montalbán, Núria; Mancini, Justin; Yang, Lishi; Abernathy, Kelsey; Frost, Frederick G.; Palm, Cheyenne

doi:10.1093/femspd/ftx046

Cited by 57 publications

(39 citation statements)

References 89 publications

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“…However, as mentioned above, administration of Gal-1 ameliorated corneal immunopathology induced by Pseudomonas aeruginosa by suppressing Th17 responses (36). Finally, Gal-1, as well as other galectins, have been proposed to serve as pathogen-recognition receptors that could positively or negatively regulate inflammatory responses by sensing glycans on the surface of pathogenic microbes (141). Thus, Gal-1 may play multifaceted roles during infection by subverting antimicrobial responses, orchestrating host immunity, or curbing pathogen-driven immunopathology.…”

Section: Subverting Antimicrobial Responses By Co-opting the Gal-1 Pamentioning

confidence: 97%

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

159

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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Section: Subverting Antimicrobial Responses By Co-opting the Gal-1 Pamentioning

confidence: 97%

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

159

136

View full text Add to dashboard Cite

show abstract

“…Glycosylation of stromal mouse counter-receptors is important for pre-B cells signaling and proliferation [35] and retention in bone marrow for B cells [36]. Maturation and activation of human B and T cells in mouse primary (bone marrow and thymus) and secondary lymphoid organs (spleen, lymph nodes) will likely affect B and T cell receptors repertoire and development [37]. Using the same donor of HSPC, we compared the B and T cell receptors repertoires in the new and existing NSG strain at 8 months of age.…”

Section: Resultsmentioning

confidence: 99%

Human-like NSG mouse glycoproteins sialylation pattern changes the phenotype of human lymphocytes and sensitivity to HIV-1 infection

Dagur

Woods

Mathews

et al. 2018

Preprint

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“…Recent insights have led to the suggestion that galectins originally functioned as recognition and effector factors in innate immunity, through binding to surface glycans of pathogenic microbes, while parasites attempted subvert the recognition roles of host galectins (57). It will be interesting to investigate whether proteins with a galectin scaffold consisting of β-sandwich/jerry roll structures really have greater binding potential for β-galactosides than others.…”

Section: G Conclusionmentioning

confidence: 99%

Carbohydrate Recognition Mechanism of the Mushroom Galectin ACG

Hirabayashi

Tateno

et al. 2018

TIGG

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The fruiting body of the edible mushroom Agrocybe cylindracea contains a proto-type galectin named ACG, which shows affinity to a wide range of β-galactosides. Unlike other galectins, it also binds to disaccharides (GalNAcα1-3Gal/GalNAc) found in blood group A and Forssman epitopes. Structurally, ACG lacks an evolutionarily conserved Asn located on the S4 strand (Ala64) but is compensated for by Asn46, which is located on the extended loop region unique to this galectin. A recent site-directed mutagenesis study revealed that the N46A mutant had selective affinity to oligosaccharides containing GalNAcα1-3Gal/GalNAc epitopes (Hu et al., (2013) Biochem. J., 453, 261-270). Taking into consideration the previous observation that Pro45 takes the cis conformation, Hu et al. assumed that ACG has evolved to attain two conformations at the imide group of Pro45: a cis conformation, where it can recognize β-galactosides, and a Pro45-tras conformation while it binds to the unique GalNAcα1-3Gal/GalNAc. The proposed dual recognition mechanism was proved through further site-directed mutagenesis and X-ray crystallography analysis. Notably, N46A recognizes even non-reducing terminal disaccharides, GalNAcα1-3Gal/GalNAc. Thus, the one face of this "Janus-type" lectin fulfills the conventional definition of galectins, whereas the other face does not. A possible scenario of galectin deviation is discussed.

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Functions of galectins as ‘self/non-self’-recognition and effector factors

Cited by 57 publications

References 89 publications

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

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

Human-like NSG mouse glycoproteins sialylation pattern changes the phenotype of human lymphocytes and sensitivity to HIV-1 infection

Carbohydrate Recognition Mechanism of the Mushroom Galectin ACG

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