SYNTHESIS OF BIOLOGICALLY-ACTIVE SIALYL-LEWIS-X MIMETICS

被引:71
|
作者
HUANG, HM [1 ]
WONG, CH [1 ]
机构
[1] Scripps Res Inst, DEPT CHEM, LA JOLLA, CA 92037 USA
来源
JOURNAL OF ORGANIC CHEMISTRY | 1995年 / 60卷 / 10期
关键词
D O I
10.1021/jo00115a027
中图分类号
O62 [有机化学];
学科分类号
070303 ; 081704 ;
摘要
The design and synthesis of two sialyl Lewis X (SLe(x)) mimetics are described. In the design of mimetic 1, an ethylene glycol linkage is used to bridge the fucose and galactose moiety, and a carboxymethyl group is placed in the 3-OH position of the galactose residue to provide the negative charge which is believed to be essential for binding to (E)-selectin. In the design of mimetic 2, a D-tartaric acid derivative is used to provide the trans-dihydroxyl groups originally from the glucosamine moiety for the linkage of the fucose and the carboxypentyl groups. At a concentration of 1.5 mM, 1 inhibits 50% of the binding of SLe(x) glycoconjugate to immobilized recombinant (E)-selectin, while 2 has an IC50 of 10 mM. Mimetic 1 is also found to be stable toward alpha-L-fucosidase. Results from the ROESY and COSY experiments indicate that compound 1 is conformationally flexible, which may explain its relatively weak activity compared to SLe(x) (IC50 = 0.8 mM).
引用
收藏
页码:3100 / 3106
页数:7
相关论文
共 50 条
  • [31] SIALYL-LEWIS-X DEMARCATES LOW-DENSITY-LIPOPROTEIN (LDL) IN INFLAMMATION
    CHAN, SE
    FASEB JOURNAL, 1995, 9 (06): : A1365 - A1365
  • [32] BINDING OF SIALYL-LEWIS-X TO E-SELECTIN AS MEASURED BY FLUORESCENCE POLARIZATION
    JACOB, GS
    KIRMAIER, C
    ABBAS, SZ
    HOWARD, SC
    STEININGER, CN
    WELPLY, JK
    SCUDDER, P
    BIOCHEMISTRY, 1995, 34 (04) : 1210 - 1217
  • [33] EXAMINATION OF THE SIALYL-LEWIS-X CALCIUM COMPLEX BY ELECTROSPRAY MASS-SPECTROMETRY
    SIUZDAK, G
    ZHENG, ZL
    RHAMPHAL, JY
    ICHIKAWA, Y
    NICOLAOU, KC
    GAETA, FCA
    CHATMAN, KS
    WONG, CH
    BIOORGANIC & MEDICINAL CHEMISTRY LETTERS, 1994, 4 (24) : 2863 - 2866
  • [34] SYNTHESIS OF BIOLOGICALLY-ACTIVE PTERIDINES
    TAYLOR, EC
    ABSTRACTS OF PAPERS OF THE AMERICAN CHEMICAL SOCIETY, 1977, 173 (MAR20): : 50 - 50
  • [35] PEPTIDE AZOLES - A NEW CLASS OF BIOLOGICALLY-ACTIVE DIPEPTIDE MIMETICS
    GORDON, T
    HANSEN, P
    MORGAN, B
    SINGH, J
    BAIZMAN, E
    WARD, S
    BIOORGANIC & MEDICINAL CHEMISTRY LETTERS, 1993, 3 (05) : 915 - 920
  • [36] APPLICATION OF GLYCALS TO THE SYNTHESIS OF OLIGOSACCHARIDES - CONVERGENT TOTAL SYNTHESES OF THE LEWIS-X TRISACCHARIDE SIALYL-LEWIS-X ANTIGENIC DETERMINANT AND HIGHER CONGENERS
    DANISHEFSKY, SJ
    GERVAY, J
    PETERSON, JM
    MCDONALD, FE
    KOSEKI, K
    GRIFFITH, DA
    ORIYAMA, T
    MARSDEN, SP
    JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1995, 117 (07) : 1940 - 1953
  • [37] SYNTHESIS OF BIOLOGICALLY-ACTIVE CYCLOPEPTIDES
    SCHMIDT, U
    CHIMIA, 1983, 37 (08) : 302 - 303
  • [38] SYNTHESIS OF BIOLOGICALLY-ACTIVE TERPENOIDS
    MORI, K
    JOURNAL OF SYNTHETIC ORGANIC CHEMISTRY JAPAN, 1974, 32 (10) : 861 - 866
  • [39] LANGERHANS CELLS EXPRESS THE E-SELECTIN LIGAND, SIALYL-LEWIS-X
    ROSS, EL
    BARKER, JNWN
    GROVES, RW
    ALLEN, MH
    CHU, AC
    MACDONALD, DM
    JOURNAL OF INVESTIGATIVE DERMATOLOGY, 1993, 100 (04) : 442 - 442
  • [40] Pitfalls in the synthesis and biological evaluation of Sialyl-Lewis(X) mimetics as potential selectin antagonists
    Kretzschmar, G
    Toepfer, A
    Hills, C
    Krause, M
    TETRAHEDRON, 1997, 53 (07) : 2485 - 2494
12345