| Literature DB >> 27447047 |
Yasuhiko Kizuka1, Sho Funayama2, Hidehiko Shogomori2, Miyako Nakano3, Kazuki Nakajima4, Ritsuko Oka1, Shinobu Kitazume1, Yoshiki Yamaguchi5, Masahiro Sano2, Hiroaki Korekane2, Tsui-Ling Hsu6, Hsiu-Yu Lee6, Chi-Huey Wong6, Naoyuki Taniguchi7.
Abstract
Fucose, a terminal sugar in glycoconjugates, critically regulates various physiological and pathological phenomena, including cancer development and inflammation. However, there are currently no probes for efficient labeling and detection of this sugar. We chemically synthesized a novel series of alkynyl-fucose analogs as probe candidates and found that 7-alkynyl-fucose gave the highest labeling efficiency and low cytotoxicity. Among the fucose analogs, 7-alkynyl-fucose was the best substrate against all five fucosyltransferases examined. We confirmed its conversion to the corresponding guanosine diphosphate derivative in cells and found that cellular glycoproteins were labeled much more efficiently with 7-alkynyl-fucose than with an existing probe. 7-Alkynyl-fucose was detected in the N-glycan core by mass spectrometry, and 7-alkynyl-fucose-modified proteins mostly disappeared in core-fucose-deficient mouse embryonic fibroblasts, suggesting that this analog mainly labeled core fucose in these cells. These results indicate that 7-alkynyl-fucose is a highly sensitive and powerful tool for basic glycobiology research and clinical application for biomarker discovery.Entities:
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Year: 2016 PMID: 27447047 DOI: 10.1016/j.chembiol.2016.06.010
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116