[PDF][PDF] Core 2 oligosaccharide biosynthesis distinguishes between selectin ligands essential for leukocyte homing and inflammation

LG Ellies, S Tsuboi, B Petryniak, JB Lowe, M Fukuda… - Immunity, 1998 - cell.com
LG Ellies, S Tsuboi, B Petryniak, JB Lowe, M Fukuda, JD Marth
Immunity, 1998cell.com
Mammalian serine/threonine-linked oligosaccharides (O-glycans) are commonly
synthesized with the Golgi enzyme core 2 β-1, 6-N-acetylglucosaminyltransferase (C2
GlcNAcT). Core 2 O-glycans have been hypothesized to be essential for mucin production
and selectin ligand biosynthesis. We report that mice lacking C2 GlcNAcT exhibit a restricted
phenotype with neutrophilia and a partial deficiency of selectin ligands. Loss of core 2
oligosaccharides reduces neutrophil rolling on substrata bearing E-, L-, and P-selectins and …
Abstract
Mammalian serine/threonine-linked oligosaccharides (O-glycans) are commonly synthesized with the Golgi enzyme core 2 β-1,6-N-acetylglucosaminyltransferase (C2 GlcNAcT). Core 2 O-glycans have been hypothesized to be essential for mucin production and selectin ligand biosynthesis. We report that mice lacking C2 GlcNAcT exhibit a restricted phenotype with neutrophilia and a partial deficiency of selectin ligands. Loss of core 2 oligosaccharides reduces neutrophil rolling on substrata bearing E-, L-, and P-selectins and neutrophil recruitment to sites of inflammation. However, the diminished presence of L-selectin ligands on lymph node high endothelial venules does not affect lymphocyte homing. These studies indicate that core 2 oligosaccharide biosynthesis segregates the physiologic roles of selectins and reveal a function for the C2 GlcNAcT in myeloid homeostasis and inflammation.
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