Literature DB >> 27920204

Studies on the Detection, Expression, Glycosylation, Dimerization, and Ligand Binding Properties of Mouse Siglec-E.

Shoib Siddiqui1, Flavio Schwarz1, Stevan Springer1, Zahra Khedri1, Hai Yu2, Lingquan Deng1, Andrea Verhagen1, Yuko Naito-Matsui1, Weiping Jiang3, Daniel Kim3, Jie Zhou3, Beibei Ding3, Xi Chen2, Nissi Varki1, Ajit Varki4.   

Abstract

CD33-related Siglecs are a family of proteins widely expressed on innate immune cells. Binding of sialylated glycans or other ligands triggers signals that inhibit or activate inflammation. Immunomodulation by Siglecs has been extensively studied, but relationships between structure and functions are poorly explored. Here we present new data relating to the structure and function of Siglec-E, the major CD33-related Siglec expressed on mouse neutrophils, monocytes, macrophages, and dendritic cells. We generated nine new rat monoclonal antibodies specific to mouse Siglec-E, with no cross-reactivity to Siglec-F. Although all antibodies detected Siglec-E on transfected human HEK-293T cells, only two reacted with mouse bone marrow neutrophils by flow cytometry and on spleen sections by immunohistochemistry. Moreover, whereas all antibodies recognized Siglec-E-Fc on immunoblots, binding was dependent on intact disulfide bonds and N-glycans, and only two antibodies recognized native Siglec-E within spleen lysates. Thus, we further investigated the impact of Siglec-E homodimerization. Homology-based structural modeling predicted a cysteine residue (Cys-298) in position to form a disulfide bridge between two Siglec-E polypeptides. Mutagenesis of Cys-298 confirmed its role in dimerization. In keeping with the high level of 9-O-acetylation found in mice, sialoglycan array studies indicate that this modification has complex effects on recognition by Siglec-E, in relationship to the underlying structures. However, we found no differences in phosphorylation or SHP-1 recruitment between dimeric and monomeric Siglec-E expressed on HEK293A cells. Phylogenomic analyses predicted that only some human and mouse Siglecs form disulfide-linked dimers. Notably, Siglec-9, the functionally equivalent human paralog of Siglec-E, occurs as a monomer.
© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  Siglec-9; Siglec-E; cell signaling; dimerization; flow cytometry; monoclonal antibody; sialic acid

Mesh:

Substances:

Year:  2016        PMID: 27920204      PMCID: PMC5247637          DOI: 10.1074/jbc.M116.738351

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  34 in total

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Journal:  Biochem J       Date:  2001-02-01       Impact factor: 3.857

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6.  Microglial CD33-related Siglec-E inhibits neurotoxicity by preventing the phagocytosis-associated oxidative burst.

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8.  Broad and direct interaction between TLR and Siglec families of pattern recognition receptors and its regulation by Neu1.

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10.  Targeting Siglecs with a sialic acid-decorated nanoparticle abrogates inflammation.

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Journal:  Sci Transl Med       Date:  2015-09-02       Impact factor: 17.956

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3.  The Alzheimer's disease-protective CD33 splice variant mediates adaptive loss of function via diversion to an intracellular pool.

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Review 6.  Sialic Acids in the Immune Response during Sepsis.

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  8 in total

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