DUP 996 (3,3-BIS(4-PYRINDINYLMETHYL)-1-PHENYLINDOLIN-2-ONE) ENHANCES THE STIMULUS-INDUCED RELEASE OF ACETYLCHOLINE FROM RAT-BRAIN INVITRO AND INVIVO

被引：76

作者：

NICKOLSON, VJ ^{[1
]}

TAM, SW ^{[1
]}

MYERS, MJ ^{[1
]}

COOK, L ^{[1
]}

机构：

[1] DUPONT CO,EXPTL STN,POB 80400,WILMINGTON,DE 19880

来源：

DRUG DEVELOPMENT RESEARCH | 1990年 / 19卷 / 03期

关键词：

cholinergic; cognition; dopamine; serotonin;

D O I：

10.1002/ddr.430190307

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

DuP 996, in micromolar concentrations, enhances the K+ ‐stimulated release of acetylcholine (ACh) in rat cerebral cortex, hippocampus, and caudate nucleus slices in vitro, without effect on basal release. DuP 996 has very weak affinity for rat brain muscarinic or nicotinic receptors and does not inhibit acetylcholinesterase activity of rat brain. Upon subcutaneous administration, DuP 996, in doses of 0.1 to 1 mg/kg, increase the output of ACh from the cerebral cortex of awake, freely moving rats. In the mouse, scopolamine‐induced hyperactivity is reduced by DuP 996 in doses of 0.3–0.5 mg/kg (s.c.). In addition, pancuronium HBr‐induced neuromuscular blockade is reversed by DuP 996 (ED50 = 1.7 mg/kg s.c.). The enhancement by DuP 996 of K+ ‐stimulated transmitter release is not limited to the cholinergic system but is also observed in the dopaminergic system in the rat caudate nucleus and in serotonergic systems. K+ ‐stimulated release of gamma‐aminobutyric acid and glutamic acid in rat cerebral cortex, however, is only slightly enchanced by DuP 996, whereas no effects are observed on K+ ‐stimulated release of cortical norepinephrine. DuP 996 may have therapeutic value in the treatment of diseases involving chlinergic and minoaminergic deterioration, like Alzheimer's Disease. Copyright © 1990 Wiley‐Liss, Inc.

引用

页码：285 / 300

页数：16

共 47 条

[1] BARTUS RT, 1984, AGING SERIES, V26, P191
[2] EFFICACY OF ORAL PHYSOSTIGMINE IN PRIMARY DEGENERATIVE DEMENTIA - A DOUBLE-BLIND-STUDY OF RESPONSE TO DIFFERENT DOSE LEVEL
BELLER, SA
OVERALL, JE
SWANN, AC
[J]. PSYCHOPHARMACOLOGY, 1985, 87 (02) : 147 - 151
[3] CHOLINE-ACETYLTRANSFERASE ACTIVITY AND HISTOPATHOLOGY OF FRONTAL NEOCORTEX FROM BIOPSIES OF DEMENTED PATIENTS
BOWEN, DM
BENTON, JS
SPILLANE, JA
SMITH, CCT
ALLEN, SJ
[J]. JOURNAL OF THE NEUROLOGICAL SCIENCES, 1982, 57 (2-3) : 191 - 202
[4] MEASUREMENT OF CHOLINERGIC DRUG EFFECTS ON MEMORY IN ALZHEIMERS-DISEASE
BRINKMAN, SD
GERSHON, S
[J]. NEUROBIOLOGY OF AGING, 1983, 4 (02) : 139 - 145
[5] PHYSOSTIGMINE AND ARECOLINE - EFFECTS OF INTRAVENOUS INFUSIONS IN ALZHEIMER PRESENILE-DEMENTIA
CHRISTIE, JE
SHERING, A
FERGUSON, J
GLEN, AIM
[J]. BRITISH JOURNAL OF PSYCHIATRY, 1981, 138 (JAN) : 46 - 50
[6] COGNITION ENHANCEMENT BY THE ACETYLCHOLINE RELEASER DUP 996
COOK, L
NICKOLSON, VJ
STEINFELS, GF
ROHRBACH, KW
DENOBLE, VJ
[J]. DRUG DEVELOPMENT RESEARCH, 1990, 19 (03) : 301 - 314
[7] COSTA LG, 1983, J PHARMACOL EXP THER, V226, P392
[8] DAVIS KL, 1983, PSYCHOPHARMACOL BULL, V19, P451
[9] DAVIS KL, 1982, AM J PSYCHIAT, V139, P1421
[10] FUNCTIONAL AND NEUROCHEMICAL CORTICAL CHOLINERGIC IMPAIRMENT FOLLOWING NEUROTOXIC LESIONS OF THE NUCLEUS BASALIS MAGNOCELLULARIS IN THE RAT
ELDEFRAWY, SR
COLOMA, F
JHAMANDAS, K
BOEGMAN, RJ
BENINGER, RJ
WIRSCHING, BA
[J]. NEUROBIOLOGY OF AGING, 1985, 6 (04) : 325 - 330

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