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Literature DB >> 19089612

The N-glycolyl form of mouse sialyl Lewis X is recognized by selectins but not by HECA-452 and FH6 antibodies that were raised against human cells.

Junya Mitoma¹, Tatsuo Miyazaki, Mark Sutton-Smith, Misa Suzuki, Hideo Saito, Jiunn-Chern Yeh, Takehiro Kawano, Ole Hindsgaul, Peter H Seeberger, Maria Panico, Stuart M Haslam, Howard R Morris, Richard D Cummings, Anne Dell, Minoru Fukuda.

Abstract

E-, P- and L-selectins critically function in lymphocyte recirculation and recruiting leukocytes to inflammatory sites. MECA-79 antibody inhibits L-selectin-mediated lymphocyte adhesion in several species and does not require sialic acid in its epitope. Many other antibodies, however, recognize human selectin ligands expressing N-acetylneuraminic acid but not mouse selectin ligands expressing N-glycolylneuraminic acid, suggesting that difference in sialic acid in sialyl Lewis X leads to differential reactivity. We found that HECA-452 and FH6 monoclonal antibodies bind Chinese hamster ovary (CHO) cells expressing N-acetylneuraminyl Lewis X oligosaccharide but not its N-glycolyl form. Moreover, synthetic N-acetylneuraminyl Lewis X oligosaccharide but not its N-glycolyl oligosaccharide inhibited HECA-452 and FH6 binding. By contrast, E-, P- and L-selectin bound to CHO cells regardless of whether they express N-acetyl or N-glycolyl form of sialyl Lewis X, showing that selectins have a broader recognition capacity than HECA-452 and FH-6 anti-sialyl Lewis x antibodies.

Entities: CellLine Chemical Disease Gene Species

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Year: 2008 PMID： 19089612 PMCID： PMC2743473 DOI： 10.1007/s10719-008-9207-8

Source DB: PubMed Journal: Glycoconj J ISSN： 0282-0080 Impact factor: 2.916

56 in total

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