Polymorphisms in the sialic acid-binding immunoglobulin-like lectin-8 (Siglec-8) gene are associated with susceptibility to asthma

Gao, Pei; Shimizu, Kenichi; Grant, Audrey V.; Rafaels, Nicholas; Zhou, Lin; Hudson, Sherry A.; Konno, Satoshi; Zimmermann, Nives; Araújo, Maria Ilma; Ponte, Eduardo Vieira; Cruz, Ãlvaro A.; Nishimura, Masaharu; Su, Song Nan; Hizawa, Nobuyuki; Beaty, T.H.; Mathias, Rasika A.; Rothenberg, Marc E.; Barnes, Kathleen C.; Bochner, Bruce S.

doi:10.1038/ejhg.2009.239

Cited by 54 publications

(42 citation statements)

References 34 publications

(44 reference statements)

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“…Siglec-8 is specifically expressed on eosinophils in humans, whereas murine eosinophils and alveolar macrophages express an isofunctional paralog, Siglec-F, that shares a novel specificity for sialylated ligands as described below 54–56 . Both Siglecs have ITIMs 3 , and polymorphisms in the gene encoding Siglec-8 are correlated with increased susceptibility to asthma 57 .…”

Section: Lung Inflammatory Diseasesmentioning

confidence: 99%

“…1e). For murine eosinophils, ligation of Siglec-F with antibodies also causes apoptosis, however, the effect is modest and appears to be mediated by a different mechanism 61 , which suggests that information gleaned from disease models involving Siglec-F should be interpreted with caution before translating their relevance to Siglec-8 and human disease 56, 57 .…”

Section: Lung Inflammatory Diseasesmentioning

confidence: 99%

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Siglec-mediated regulation of immune cell function in disease

2014

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All mammalian cells display a diverse array of glycan structures that differ from those found on microbial pathogens. Siglecs are a family of sialic acid-binding immunoglobulin-like receptors that participate in the discrimination of ‘self’ and ‘non-self’ and regulate the functions of cells in the innate and adaptive immune systems through recognition of their glycan ligands. In this review, we describe the recent advances in our understanding of the roles of Siglecs in the regulation of immune cell functions in infectious diseases, inflammation, neurodegeneration, autoimmune diseases and cancer.

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Section: Lung Inflammatory Diseasesmentioning

confidence: 99%

Section: Lung Inflammatory Diseasesmentioning

confidence: 99%

Siglec-mediated regulation of immune cell function in disease

2014

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“…If regulation by inhibitory CD33rSiglecs is perturbed, pathologies may ensue including eosinophilic airway inflammation in mSiglec-F knockout mice [14], elevated pro-inflammatory cytokines in mice lacking mSiglec-G [8], asthma associated with hSiglec-8 polymorphisms [15], or exaggerated T-cell responses linked to an hSiglec-9 gene polymorphism [16]. Mouse microglial cells lacking mSiglec-E showed increased inflammatory responses and neurotoxicity in neuronal co-culture experiments [17], and hSiglec-10 is a selective modulator of the immune response to the DAMP HMGB1 released by necrotic cells [8].…”

Section: Introductionmentioning

confidence: 99%

Host and pathogen hyaluronan signal through human siglec-9 to suppress neutrophil activation

et al. 2015

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Inhibitory CD33-related Siglec receptors regulate immune cell activation upon engaging ubiquitous sialic acids (Sias) on host cell surface glycans. Through molecular mimicry, Sia-expressing pathogen group B Streptococcus binds inhibitory human Siglec-9 (hSiglec-9) to blunt neutrophil activation and promote bacterial survival. We unexpectedly discovered that hSiglec-9 also specifically binds high molecular weight hyaluronan (HMW-HA), another ubiquitous host glycan, through a region of its terminal Ig-like V-set domain distinct from the Sia-binding site. HMW-HA recognition by hSiglec-9 limited neutrophil extracellular trap (NET) formation, oxidative burst, and apoptosis, defining HMW-HA as a regulator of neutrophil activation. However, the pathogen group A Streptococcus (GAS) expresses a HMW-HA capsule that engages hSiglec-9, blocking NET formation and oxidative burst, thereby promoting bacterial survival. Thus, a single inhibitory lectin receptor detects two distinct glycan “self-associated molecular patterns” to maintain neutrophil homeostasis, and two leading human bacterial pathogens have independently evolved molecular mimicry to exploit this immunoregulatory mechanism.

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“…There is increasing awareness that dysregulated Siglec-8 function might be critically involved in the pathobiology of allergic and chronic inflammatory disorders, including asthma, where accumulation and delayed apoptosis of activated eosinophils and mast cells in the airways are among the leading causes of persistent inflammation and tissue damage (19,20). Indeed, Siglec-8 gene polymorphisms were identified to correlate with increased asthma risk (21), albeit the detailed molecular pathways linking Siglec-8 to disease have yet to be clarified. On account of its potent eosinophil proapoptotic and mast cell-inhibitory activities, combined with its selective expression on these key inflammatory effector cells, Siglec-8 is considered a promising target for novel antiinflammatory, proresolving treatment strategies for asthma and other disease conditions in which inappropriate and/or prolonged inflammatory responses of these cell types contributes to pathology (20,(22)(23)(24)(25).…”

Section: Significancementioning

confidence: 99%

Structural basis for sulfation-dependent self-glycan recognition by the human immune-inhibitory receptor Siglec-8

Pröpster

Yang

Rabbani

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

121

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Siglec-8 is a human immune-inhibitory receptor that, when engaged by specific self-glycans, triggers eosinophil apoptosis and inhibits mast cell degranulation, providing an endogenous mechanism to down-regulate immune responses of these central inflammatory effector cells. Here we used solution NMR spectroscopy to dissect the fine specificity of Siglec-8 toward different sialylated and sulfated carbohydrate ligands and determined the structure of the Siglec-8 lectin domain in complex with its prime glycan target 6′-sulfo sialyl Lewis x . A canonical motif for sialic acid recognition, extended by a secondary motif formed by unique loop regions, recognizing 6-O-sulfated galactose dictates tight specificity distinct from other Siglec family members and any other endogenous glycan recognition receptors. Structure-guided mutagenesis revealed key contacts of both interfaces to be equally essential for binding. Our work provides critical structural and mechanistic insights into how Siglec-8 selectively recognizes its glycan target, rationalizes the functional impact of site-specific glycan sulfation in modulating this lectin-glycan interaction, and will enable the rational design of Siglec-8-targeted agonists to treat eosinophil-and mast cell-related allergic and inflammatory diseases, such as asthma.NMR spectroscopy | protein-carbohydrate recognition | glycan sulfation | immune regulation | glycoimmunology

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Polymorphisms in the sialic acid-binding immunoglobulin-like lectin-8 (Siglec-8) gene are associated with susceptibility to asthma

Cited by 54 publications

References 34 publications

Siglec-mediated regulation of immune cell function in disease

Siglec-mediated regulation of immune cell function in disease

Host and pathogen hyaluronan signal through human siglec-9 to suppress neutrophil activation

Structural basis for sulfation-dependent self-glycan recognition by the human immune-inhibitory receptor Siglec-8

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