STRUCTURE-ACTIVITY-RELATIONSHIPS OF 8-STYRYLXANTHINES AS A(2)-SELECTIVE ADENOSINE ANTAGONISTS

被引：140

作者：

JACOBSON, KA ^{[1
]}

GALLORODRIGUEZ, C ^{[1
]}

MELMAN, N ^{[1
]}

FISCHER, B ^{[1
]}

MAILLARD, M ^{[1
]}

VANBERGEN, A ^{[1
]}

VANGALEN, PJM ^{[1
]}

KARTON, Y ^{[1
]}

机构：

[1] ISRAEL INST BIOL RES,DEPT ORGAN CHEM,IL-70450 NESS ZIONA,ISRAEL

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1993年 / 36卷 / 10期

关键词：

D O I：

10.1021/jm00062a005

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

A series of substituted 8-styryl derivatives of 1,3,7-alkylxanthines was synthesized as potential A2-selective adenosine receptor antagonists, and the potency at rat brain A1- and A2-receptors was studied in radioligand binding experiments. At the xanthine 7-position, only small hydrophobic substituents were tolerated in receptor binding. 7-Methyl analogues were roughly 1 order of magnitude more selective for A2 versus A1 receptors than the corresponding 7-H analogues. 1,3-Dimethylxanthine derivatives tended to be more selective for A2-receptors than the corresponding 1,3-diallyl, diethyl, or dipropyl derivatives. Substitutions of the phenyl ring at the 3-(monosubstituted) and 3,5-(disubstituted) positions were favored. 1,3,7-Trimethyl-8-(3-chlorostyryl)xanthine was a moderately potent (K(i) vs [H-3]CGS 21680 was 54 nM) and highly A2-selective (520-fold) adenosine antagonist. 1,3,7-Trimethyl-8-[3-[(3-carboxy-1-oxopropyl)amino]styryl]xanthine was highly A2-selective (250-fold) and of enhanced water solubility (max 19 mM). 1,3-Dipropyl-7-methyl-8-(3,5-dimethoxystyryl)xanthine was a potent (K(i) = 24 nM) and very A2-selective (110-fold) adenosine antagonist.

引用

页码：1333 / 1342

页数：10

共 25 条

[1] NUCLEOSIDES AND NUCLEOTIDES .107. 2-(CYCLOALKYLALKYNYL)ADENOSINES - ADENOSINE A2-RECEPTOR AGONISTS WITH POTENT ANTIHYPERTENSIVE EFFECTS
ABIRU, T
MIYASHITA, T
WATANABE, Y
YAMAGUCHI, T
MACHIDA, H
MATSUDA, A
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1992, 35 (12) : 2253 - 2260
[2] IDENTIFICATION OF THE A2 ADENOSINE RECEPTOR-BINDING SUBUNIT BY PHOTOAFFINITY CROSSLINKING
BARRINGTON, WW
JACOBSON, KA
HUTCHISON, AJ
WILLIAMS, M
STILES, GL
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (17) : 6572 - 6576
[3] BECKER ED, 1980, HIGH RESOLUTION NMR
[4] CHENG Y, 1973, BIOCHEM PHARMACOL, V22, P3099
[5] CAFFEINE AND THEOPHYLLINE ANALOGS - CORRELATION OF BEHAVIORAL-EFFECTS WITH ACTIVITY AS ADENOSINE RECEPTOR ANTAGONISTS AND AS PHOSPHODIESTERASE INHIBITORS
CHOI, OH
SHAMIM, MT
PADGETT, WL
DALY, JW
[J]. LIFE SCIENCES, 1988, 43 (05) : 387 - 398
[6] 1,3,8-TRISUBSTITUTED XANTHINES - EFFECTS OF SUBSTITUTION PATTERN UPON ADENOSINE RECEPTOR-A1/A2 AFFINITY
ERICKSON, RH
HINER, RN
FEENEY, SW
BLAKE, PR
RZESZOTARSKI, WJ
HICKS, RP
COSTELLO, DG
ABREU, ME
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1991, 34 (04) : 1431 - 1435
[7] ADENOSINE DOPAMINE INTERACTIONS IN THE BRAIN
FERRE, S
FUXE, K
VONEULER, G
JOHANSSON, B
FREDHOLM, BB
[J]. NEUROSCIENCE, 1992, 51 (03) : 501 - 512
[8] STRUCTURE ACTIVITY PROFILE OF A SERIES OF NOVEL TRIAZOLOQUINAZOLINE ADENOSINE ANTAGONISTS
FRANCIS, JE
CASH, WD
PSYCHOYOS, S
GHAI, G
WENK, P
FRIEDMANN, RC
ATKINS, C
WARREN, V
FURNESS, P
HYUN, JL
STONE, GA
DESAI, M
WILLIAMS, M
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1988, 31 (05) : 1014 - 1020
[9] ELECTROPHILIC DERIVATIVES OF PURINES AS IRREVERSIBLE INHIBITORS OF A1-ADENOSINE RECEPTORS
JACOBSON, KA
BARONE, S
KAMMULA, U
STILES, GL
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1989, 32 (05) : 1043 - 1051
[10] ADENOSINE RECEPTORS - PHARMACOLOGY, STRUCTURE-ACTIVITY-RELATIONSHIPS, AND THERAPEUTIC POTENTIAL
JACOBSON, KA
VANGALEN, PJM
WILLIAMS, M
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1992, 35 (03) : 407 - 422

← 1 2 3 →