Atlantic Salmon Carries a Range of Novel O-Glycan Structures Differentially Localized on Skin and Intestinal Mucins

被引:56
作者
Jin, Chunsheng [1 ]
Padra, Janos Tamas [1 ]
Sundell, Kristina [2 ]
Sundh, Henrik [2 ]
Karlsson, Niclas G. [1 ]
Linden, Sara K. [1 ]
机构
[1] Univ Gothenburg, Dept Med Chem & Cell Biol, SE-40530 Gothenburg, Sweden
[2] Univ Gothenburg, Dept Biol & Environm Sci, SE-40530 Gothenburg, Sweden
基金
瑞典研究理事会;
关键词
Atlantic salmon; fish; O-glycan; mucins; skin; gastrointestinal tract; mucus; glycosylation; RAINBOW-TROUT; OLIGOSACCHARIDE-ALDITOLS; JELLY COATS; MUC2; MUCIN; GLYCOPROTEIN; ZEBRAFISH; EGGS; HISTOCHEMISTRY; GLYCOSYLATION; PURIFICATION;
D O I
10.1021/acs.jproteome.5b00232
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Aquaculture is a growing industry, increasing the need for understanding host-pathogen interactions in fish. The skin and mucosal surfaces, covered by a mucus layer composed of mucins, is the first point of contact between fish and pathogens. Highly O-glycosylated mucins have been shown to be an important part of the defense against pathogens, and pathogens bind to host surfaces using lectin-like adhesins. However, knowledge of piscine O-glycosylation is very limited. We characterized mucin O-glycosylation of five freshwater acclimated Atlantic salmon, using mass spectrometry. Of the 109 O-glycans found, most were sialylated and differed in distribution among skin, pyloric ceca, and proximal and distal intestine. Skin O-glycans were shorter (2-6 residues) and less diverse (33 structures) than intestinal O-glycans (2-13 residues, 93 structures). Skin mucins carried O-glycan cores 1, 2, 3, and 5 and three types of sialic acids (Neu5Ac, Neu5Gc, and Kdn) and had sialyl-Tn as the predominant structure. Intestinal mucins carried only cores 1, 2, and 5, Neu5Ac was the only sialic acid present, and sialylated core S was the most dominant structure. This structural characterization can be used for identifying structures of putative importance in host-pathogen interactions for further testing in biological assays and disease intervention therapies.
引用
收藏
页码:3239 / 3251
页数:13
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