IS THERE A COMMON, HIGH-AFFINITY OPIOID BINDING-SITE IN RAT-BRAIN

被引：23

作者：

BLURTON, PA ^{[1
]}

BROADHURST, AM ^{[1
]}

WOOD, MD ^{[1
]}

WYLLIE, MG ^{[1
]}

机构：

[1] WYETH LABS, BIOCHEM PHARMACOL, MAIDENHEAD SL6 0PH, BERKS, ENGLAND

来源：

JOURNAL OF RECEPTOR RESEARCH | 1986年 / 6卷 / 01期

关键词：

D O I：

10.3109/10799898609073926

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

At low concentrations, 3H-naloxone apparently bound to two sites, of high (KD 0.50 nM) and low (KD 2.0nM) affinity. Binding to the high affinity site was preferentially blocked by naloxonazine. This is consistent with the high and low affinity sites representing the .mu.1 and .mu.2 sites respectively. Binding of 3H-naloxnone to the .mu.1 and .mu.2 sites was differentially inhibited by opioids. Compared to .mu.2 binding, DADLE and DAGO preferentially inhibited .mu.1 binding. DADLE inhibited the binding of 3H-DAGO potently and in a competitive manner. DAGO inhibited the binding of 3H-DADLE from two sites for which DAGO had high and low affinities. Scatchard analysis indicated that both 3H-DAGO and 3H-DADLE bound to one class of sites, with 3H-DADLE having a 2-3 fold greater Bmax. It is concluded that 3H-opioids bind to at least three sites -.mu.1, .mu.2 and .delta.. The .mu.1 site represents a high affinity binding site for both opioid peptides and opioid alkaloids. DAGO is a selective ligand for the .mu.1 site, whilst DADLE interacts with .mu.1 and .delta. sites with similar affinities.

引用

页码：85 / 93

页数：9

共 50 条

[21] A NOVEL SPECIFIC BINDING-SITE FOR HOMOPHTHALAZINES IN THE RAT-BRAIN
HORVATH, EJ
HUDAK, J
PALKOVITS, M
LENKEI, Z
FEKETE, MIK
ARANYI, P
EUROPEAN JOURNAL OF PHARMACOLOGY, 1993, 236 (01) : 151 - 153
[22] HIGH-AFFINITY (H-3)-DEXOXADROL BINDING TO RAT-BRAIN MEMBRANES
SETHY, VH
MCCALL, JM
DRUG DEVELOPMENT RESEARCH, 1984, 4 (06) : 635 - 645
[23] CHARACTERIZATION OF HIGH-AFFINITY [H-3] TRIAZOLAM BINDING IN RAT-BRAIN
EARLE, M
CONCAS, A
YAMAMURA, HI
FEDERATION PROCEEDINGS, 1986, 45 (03) : 663 - 663
[24] HIGH-AFFINITY BINDING OF [H-3]ETHYLKETOCYCLAZOCINE TO RAT-BRAIN HOMOGENATE
HARRIS, DW
SETHY, VH
EUROPEAN JOURNAL OF PHARMACOLOGY, 1980, 66 (01) : 121 - 123
[25] [H-3] OUABAIN BINDING TO OX BRAIN MEMBRANES - CHARACTERIZATION OF A HIGH-AFFINITY BINDING-SITE
MAZZONI, MR
MARTINI, C
LUCACCHINI, A
NEUROCHEMISTRY INTERNATIONAL, 1990, 16 (02) : 193 - 197
[26] OPIOID-INHIBITED ADENYLYL CYCLASE IN RAT-BRAIN MEMBRANES - LACK OF CORRELATION WITH HIGH-AFFINITY OPIOID RECEPTOR-BINDING SITES
NIJSSEN, PCG
SEXTON, T
CHILDERS, SR
JOURNAL OF NEUROCHEMISTRY, 1992, 59 (06) : 2251 - 2262
[27] MYELIN BASIC-PROTEIN IS AN ENDOGENOUS INHIBITOR OF THE HIGH-AFFINITY CANNABINOID BINDING-SITE IN BRAIN
NYE, JS
VOGLMAIER, S
MARTENSON, RE
SNYDER, SH
JOURNAL OF NEUROCHEMISTRY, 1988, 50 (04) : 1170 - 1178
[28] HIGH-AFFINITY PROLINE UPTAKE IN RAT-BRAIN SYNAPTOSOMES
HAUPTMANN, M
WILSON, DF
ERECINSKA, M
FEBS LETTERS, 1983, 161 (02) : 301 - 305
[29] HIGH-AFFINITY KAINATE AND DOMOATE RECEPTORS IN RAT-BRAIN
LOMELI, H
WISDEN, W
KOHLER, M
KEINANEN, K
SOMMER, B
SEEBURG, PH
FEBS LETTERS, 1992, 307 (02) : 139 - 143
[30] INDUCIBLE HIGH-AFFINITY BINDING-SITE FOR BENZO(A)PYRENE IN CYTOSOL FROM RAT-LIVER
MURESAN, Z
STOICA, A
STAFIDOV, N
VOICULETZ, N
NEOPLASMA, 1987, 34 (05) : 523 - 535

← 1 2 3 4 5 →