Title of article
Novel mimics of sialyl Lewis X: design, synthesis and biological activity of a series of 2- and 3-malonate substituted galactoconjugates Original Research Article
Author/Authors
Anne Marinier، نويسنده , , Alain Martel، نويسنده , , Carol Bachand، نويسنده , , Serge Plamondon، نويسنده , , Brigitte Turmel، نويسنده , , Jean-Paul Daris، نويسنده , , Jacques Banville، نويسنده , , Philippe Lapointe، نويسنده , , Carl Ouellet، نويسنده , , Pierre Dextraze، نويسنده , , Marcel Menard، نويسنده , , John J.K Wright، نويسنده , , Julie Alford، نويسنده , , Debbie Lee، نويسنده , , James Paul Stanley، نويسنده , , Xina Nair، نويسنده , , Gordon Todderud، نويسنده , , Kenneth M. Tramposch، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2001
Pages
33
From page
1395
To page
1427
Abstract
A series of potent inhibitors of P-selectin as potential anti-inflammatory agents is reported. These compounds are derivatives of galactocerebrosides bearing a malonate side chain in positions 2 and 3 of the galactose moiety. Based on the binding mode of sialyl Lewis X, the two acidic groups of the malonate are designed to form ionic interactions with two important lysines in the active site of P-selectin, Lys113 and Lys111. On the other hand, the 4- and 6-hydroxy groups on the galactose ring are arranged to chelate the calcium ion in the P-selectin active site. The synthesis and the biological activity of this series of compounds are described. Lead compounds having a greater potency than sialyl Lewis X are identified.
Journal title
Bioorganic and Medicinal Chemistry
Serial Year
2001
Journal title
Bioorganic and Medicinal Chemistry
Record number
1301558
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