选择素
化学
部分
双环分子
体内
立体化学
免疫系统
电子选择素
体外
立体选择性
细胞粘附
生物化学
粘附
细胞
免疫学
生物
有机化学
生物技术
催化作用
作者
Ryan D. Simard,Mathieu Joyal,Thomas Beaugrand,Julien Gauthier,Elodie Hardine,Axelle Desriac,Charles-Henri Buffet,Michel Prévost,Mona Nemer,Yvan Guindon
标识
DOI:10.1021/acs.joc.3c00956
摘要
E- and P-selectins are adhesion proteins implicated in immune cell recruitment at sites of infection, making them important drug targets for diseases involving excessive and uncontrolled inflammation. In this study, we developed an efficient strategy to synthesize bicyclic galactopyranosides through a key stereoselective equatorial C4-propiolate addition and TMSCN axial C-glycosidation. The nitrile group can then be converted to the carboxyl and different bioisosteres at a late stage in the synthesis, allowing for various derivatizations to potentially enhance biological activity. The sialyl LewisX glycomimetic featuring this rigidified bicyclic galactopyranoside moiety prevents neutrophil adhesion to endothelial cells in vitro by binding to both E- and P-selectins. We show here that the axial carboxyl analogue blocks immune cell recruitment in vivo, demonstrating its potential as an immunomodulator.
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