KAINIC ACID SEIZURES IN THE DEVELOPING BRAIN - STATUS EPILEPTICUS AND SPONTANEOUS RECURRENT SEIZURES

被引：244

作者：

STAFSTROM, CE

THOMPSON, JL

HOLMES, GL

机构：

[1] Department of Neurology, The Children's Hospital, Harvard Medical School, Boston

来源：

DEVELOPMENTAL BRAIN RESEARCH | 1992年 / 65卷 / 02期

关键词：

DEVELOPING BRAIN; FLUROTHYL; KAINIC ACID; SEIZURE; SPONTANEOUS RECURRENT SEIZURE; STATUS EPILEPTICUS;

D O I：

10.1016/0165-3806(92)90184-X

中图分类号：

Q [生物科学];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Acute and chronic effects of seizures induced by intraperitoneal (i.p.) injection of kainic acid (KA) were studied in developing rats (post-natal days (P) 5, 10, 20, 30, and adult 60). For 3 months following KA-induced status epilepticus, spontaneous recurrent seizure (SRS) occurrence was quantified using intermittent video monitoring. Latency to generalized seizures was then tested using flurothyl, and brains were histologically analyzed for CA3 lesions. In P5-10 rats, KA caused generalized tonic-clonic ('swimming') seizures. SRS did not develop, and there was no significant difference between control and KA-treated rats in latency to flurothyl-induced seizures. In contrast, rats P20 and older exhibited limbic automatisms followed by limbic motor seizures which secondarily generalized. Incidence and frequency of SRS increased with age. P20-30 rats with SRS had shorter latencies to flurothyl seizures than did KA-treated P20-30 rats without SRS or controls. KA-treated P60 rats (with or without SRS) had shorter latencies than controls to flurothyl seizure onset. SRS in P60 rats occurred sooner after KA than in P20-30 rats. CA3 lesions were seen in P20-60 rats with and without SRS, but not in P5-10 rats. These data suggest that there are developmental differences in both acute and chronic responses to KA, with immature animals relatively protected from the long-term deleterious effects of this convulsant.

引用

页码：227 / 236

页数：10

共 46 条

[31] PRICHARD JW, 1969, J PHARMACOL EXP THER, V166, P170
[32] MODIFICATION OF SEIZURE ACTIVITY BY ELECTRICAL STIMULATION .2. MOTOR SEIZURE
RACINE, RJ
[J]. ELECTROENCEPHALOGRAPHY AND CLINICAL NEUROPHYSIOLOGY, 1972, 32 (03): : 281 - &
[33] HIPPOCAMPAL PLASTICITY IN CHILDHOOD EPILEPSY
REPRESA, A
ROBAIN, O
TREMBLAY, E
BENARI, Y
[J]. NEUROSCIENCE LETTERS, 1989, 99 (03) : 351 - 355
[34] SHERWOOD NM, 1970, STEREOTAXIC ATLAS DE
[35] SLOVITER RS, 1990, EPILEPSIA, V31, P675
[36] RESISTANCE OF THE IMMATURE HIPPOCAMPUS TO SEIZURE-INDUCED SYNAPTIC REORGANIZATION
SPERBER, EF
HAAS, KZ
STANTON, PK
MOSHE, SL
[J]. DEVELOPMENTAL BRAIN RESEARCH, 1991, 60 (01): : 88 - 93
[37] AGE-RELATED DIFFERENCES IN SEIZURE SUSCEPTIBILITY TO FLUROTHYL
SPERBER, EF
MOSHE, SL
[J]. DEVELOPMENTAL BRAIN RESEARCH, 1988, 39 (02): : 295 - 297
[38] STAFSTROM C, 1989, Epilepsia, V30, P673
[39] EXPERIMENTAL-MODELS OF TEMPORAL-LOBE EPILEPSY - NEW INSIGHTS FROM THE STUDY OF KINDLING AND SYNAPTIC REORGANIZATION
SUTULA, TP
[J]. EPILEPSIA, 1990, 31 : S45 - S54
[40] SPONTANEOUS SECONDARILY GENERALIZED SEIZURES INDUCED BY A SINGLE MICROINJECTION OF KAINIC ACID INTO UNILATERAL AMYGDALA IN CATS
TANAKA, T
KAIJIMA, M
YONEMASU, Y
CEPEDA, C
[J]. ELECTROENCEPHALOGRAPHY AND CLINICAL NEUROPHYSIOLOGY, 1985, 61 (05): : 422 - 429

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