ANTICONVULSANT ACTIVITY OF THE NMDA ANTAGONISTS, D(-)4-(3-PHOSPHONOPROPYL)PIPERAZINE-2-CARBOXYLIC ACID (D-CPP) AND D(-)(E)-4-(3-PHOSPHONOPROP-2-ENYL) PIPERAZINE-2-CARBOXYLIC ACID (D-CPPENE) IN A RODENT AND A PRIMATE MODEL OF REFLEX EPILEPSY

被引：77

作者：

PATEL, S

CHAPMAN, AG

GRAHAM, JL

MELDRUM, BS

FREY, P

机构：

[1] INST PSYCHIAT,DEPT NEUROL,DECRESPIGNY PK,LONDON SE5 8AF,ENGLAND

[2] SANDOZ RES INST BERNE LTD,CH-3007 BERN,SWITZERLAND

来源：

EPILEPSY RESEARCH | 1990年 / 7卷 / 01期

基金：

英国惠康基金;

关键词：

Anticonvulsants; CPP; CPP-ene; DBA/2; mice; Epilepsy; Excitatory amino acid antagonists; Papio papio;

D O I：

10.1016/0920-1211(90)90049-2

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

d-(-)4-(3-phosphonopropyl)piperazine-2-carboxylic acid (D-CPP) and its unsaturated analogue (d(-)(E)-4-(3-phosphonoprop-2-enyl) piperazine-2-carboxylic acid (D-CPPene) have been administered to DBA/2 mice (intracerebroventricularly, i.c.v., intraperitoneally, i.p., and orally, p.o.) and to photosensitive baboons, Papio papio (intravenously, i.v., and orally), and their effects on reflexly induced epileptic responses assessed. In DBA/2 mice the clonic phase of the seizure response to sound is suppressed by D-CPP with an ED50 of 5.5 μg/mouse, i.c.v.; 0.69 mg (2.75 μmol)/kg i.p. and 16.6 mg (65.8 μmol)/kg p.o. compared with, for D-CPPene, 2.2 μg/mouse i.c.v., 0.41 mg (1.54 μmol)/kg i.p. and 10.8 mg (40.2 μmol)/kg, p.o. In Papio papio myoclonic responses to strobostopic stimulation are suppressed 24 and 48 h after D-CPP 32 mg (127 μmol)/kg p.o. Administration of D-CPPene 8-16 mg (30-60 μmol)/kg i.v. produces protection against myoclonic responses after 1-2 h, lasting for 48 h. Oral administration of D-CPPene 32-64 mg (119-239 μmol)/kg produces protection beginning after 4 h and sustained for 48 h. Measurements of plasma D-CPPene concentration show clearance after i.v. injection and a low plasma concentration 1.5-5 h after oral administration. The prolonged anticonvulsant action of D-CPP and D-CPPene following oral administration suggests that these compounds merit evaluation as antiepileptic therapy in man. © 1990.

引用

页码：3 / 10

页数：8

共 18 条

[1] AEBISCHER B, 1989, HELV CHIM ACTA, V72, P1
[2] POTENT ORAL ANTICONVULSANT ACTION OF CPP AND CPPENE IN DBA/2 MICE
CHAPMAN, AG
GRAHAM, J
MELDRUM, BS
[J]. EUROPEAN JOURNAL OF PHARMACOLOGY, 1990, 178 (01) : 97 - 99
[3] ANTICONVULSANT ACTION AND BIOCHEMICAL EFFECTS IN DBA 2 MICE OF CPP (3-((+/-)-2-CARBOXYPIPERAZIN-4-YL)-PROPYL-1-PHOSPHONATE), A NOVEL N-METHYL-D-ASPARTATE ANTAGONIST
CHAPMAN, AG
MELDRUM, BS
NANJI, N
WATKINS, JC
[J]. EUROPEAN JOURNAL OF PHARMACOLOGY, 1987, 139 (01) : 91 - 96
[4] CHAPMAN AG, 1989, J CEREB BLOOD FLOW M, V9, P5309
[5] ANTICONVULSANT ACTION OF EXCITATORY AMINO-ACID ANTAGONISTS
CROUCHER, MJ
COLLINS, JF
MELDRUM, BS
[J]. SCIENCE, 1982, 216 (4548) : 899 - 901
[6] CPP, A NEW POTENT AND SELECTIVE NMDA ANTAGONIST - DEPRESSION OF CENTRAL NEURON RESPONSES, AFFINITY FOR [H-3] D-AP5 BINDING-SITES ON BRAIN MEMBRANES AND ANTICONVULSANT ACTIVITY
DAVIES, J
EVANS, RH
HERRLING, PL
JONES, AW
OLVERMAN, HJ
POOK, P
WATKINS, JC
[J]. BRAIN RESEARCH, 1986, 382 (01) : 169 - 173
[7] FAGG G E, 1989, British Journal of Pharmacology, V97, p582P
[8] FAGG GE, 1989, CURRENT FUTURE TREND
[9] HERRLING P L, 1989, Society for Neuroscience Abstracts, V15, P327
[10] LEHMANN J, 1987, J PHARMACOL EXP THER, V240, P737

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