The Leukocyte Activation Receptor CD69 Controls T Cell Differentiation through Its Interaction with Galectin-1

Fuente, Hortensia de la; Cruz-Adalia, Aránzazu; Martín, Pilar; Cibrián-Vera, Danay; Bonay, Pedro; Pérez-Hernández, Daniel; Vázquez, Jesús; Navarro, Pilar; Gutiérrez-Gallego, Ricardo; Ramírez-Huesca, Marta; Martı́n, Pilar; Sánchez-Madrid, Francisco

doi:10.1128/mcb.00348-14

Cited by 77 publications

(70 citation statements)

References 41 publications

(51 reference statements)

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“…More recently, the DC‐derived galectin‐1 ligand was shown to negatively regulate T helper (T h )17 effector cell differentiation via CD69 (24), whereas the positive expression of CD69 in Foxp3 + T reg cells was shown to maintain immune tolerance (8). However, the role of CD69 in the switch of CD4 + naive T cells into CD25 + Foxp3 + T reg cells has yet to be elucidated.…”

mentioning

confidence: 99%

Glycosylation‐dependent interaction between CD69 and S100A8/S100A9 complex is required for regulatory T‐cell differentiation

Lin

Wei

Tsai³

et al. 2015

FASEB j.

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Cluster of differentiation (CD)69 is a leukocyte activation receptor involved in the maintenance of immune homeostasis and is positively selected in activated regulatory T (Treg) cells, implicating its role during Treg-cell differentiation. By RNA interference, we show that CD69 is not sufficient to support the conversion of CD4(+) naive T cells into Treg cells, whereas it does that of human peripheral blood mononuclear cells (hPBMCs) (P < 0.01), suggesting that a ligand-receptor interaction is required for CD69 function. Using immunoprecipitation and mass spectrometry, we identified the S100A8/S100A9 complex as the natural ligand of CD69 in hPBMCs. CD69 specifically associates with S100A8/S100A9 complex as confirmed by in vitro binding and competition assay, and the treatment of CD69 with peptide-N-glycosidase significantly abolishes such association. In agreement, the glycomics analysis determines the glycosylation site and the N-glycan composition of CD69, and terminal removal of sialic acid from that N-linked glycans reverses the generation of forkhead box P3-positive Treg cells (23.21%; P < 0.05). More specifically, we showed that CD69-S100A8/S100A9 association is required for the up-regulation of suppressor of cytokine signaling 3 resulting in inhibited signaling of signal transducer and activator of transcription 3 (36.54% increase upon CD69 silencing; P < 0.01). This might in turn support the secretion of key regulator TGF-β (∼ 3.28-fold decrease upon CD69 silencing; P < 0.05), leading to reduced production of IL-4 in hPBMCs. Our results demonstrate the functional and mechanistic interplays between CD69 and S100A8/S100A9 in supporting Treg-cell differentiation.

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mentioning

confidence: 99%

Glycosylation‐dependent interaction between CD69 and S100A8/S100A9 complex is required for regulatory T‐cell differentiation

Lin

Wei

Tsai³

et al. 2015

FASEB j.

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“…6D). Given the fact that galectin‐1, a β‐galactoside‐binding immune‐suppressive protein, has recently been discovered as a ligand for CD69 on DCs [34], the presence of Gal‐1 on MultiStem was also studied. Fluorescence microscopy revealed Gal‐1 expression (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Based on the MultiStem‐mediated elevated levels of CD69 in T cells and the presence of its ligand Gal‐1 [34] in MultiStem, Gal‐1/CD69 binding could be an important mechanism of immune modulation by adult stem cells, independent of cytotoxicity suppression. de la Fuente et al already proved inhibition of T h 17 differentiation and function in mice and humans upon CD69 recruitment [34]. In our study, we demonstrated that Gal‐1 signaling did not mediate the inhibitory effect of MultiStem on T‐cell cytotoxicity.…”

Section: Discussionmentioning

confidence: 99%

Clinical-Grade Human Multipotent Adult Progenitor Cells Block CD8+ Cytotoxic T Lymphocytes

Plessers

Dekimpe

Woensel

et al. 2016

Stem Cells Translational Medicine

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Because multipotent adult progenitor cells (MAPCs) are among the noteworthy adult mesenchymal stem cell populations for immune therapy and have the advantage over mesenchymal stem cells (MSCs) of large-scale manufacturing and banking potential and thus prompt availability, it is important to understand how MAPCs interact with immune cells to validate their widespread therapeutic applicability. Cytotoxic immune effector cells play a crucial role in immune homeostasis and in the pathogenesis of some autoimmune diseases. This study assessed for the first time the in vitro influence of a clinical-grade human MAPC product (MultiStem) on the cytotoxic function of CD8 T cells (CTLs) by evaluating the immunogenicity of MAPCs and the susceptibility of MAPCs toward CTL-mediated lysis and by analyzing the mechanism of MAPC-mediated modulation of CTL functionality. These results may represent a highly relevant contribution to the current knowledge and, in combination with the results of future phase II/III trials using MultiStem, could lead to an intriguing continuation of stem cell-based research for immunotherapy.

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“…In fact, Gal-1-expressing DCs greatly contributed to the resolution of antigen-specific and autoimmune diseases [93]. Although the precise molecular mechanisms involved in this effect still remain to be explored, recent studies identified CD69 as a counter-receptor for DC-derived Gal-1 on T cells, suggesting that a Gal-1-CD69 axis may contribute to DC-mediated suppression of pro-inflammatory T cell responses [98]. Moreover, DC expression of Gal-1 mediates, at least in part, the tolerogenic effects triggered by IL-10 and apoptotic cells [99,100].…”

Section: Tolerogenic Dendritic 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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The Leukocyte Activation Receptor CD69 Controls T Cell Differentiation through Its Interaction with Galectin-1

Cited by 77 publications

References 41 publications

Glycosylation‐dependent interaction between CD69 and S100A8/S100A9 complex is required for regulatory T‐cell differentiation

Glycosylation‐dependent interaction between CD69 and S100A8/S100A9 complex is required for regulatory T‐cell differentiation

Clinical-Grade Human Multipotent Adult Progenitor Cells Block CD8+ Cytotoxic T Lymphocytes

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

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