覚醒剤精神病モデルラットにおけるgamma-aminobutyric acid(GABA) : benzodiazepine神経伝達系の役割について

伊藤, 耕一


Hokkaido University \| Library \| HUSCAP	Advanced Search		言語

	Home
	About HUSCAP
	Open Access Policy

	Browse by Author

Browse
	Communities & Collections

	Scholarly Journals
	Theses
	Doctoral Dissertations Listed by Graduate Schools
	Conference Procs.
	Events

	HUSCAP Senior (in Japanese)

	Societies

	Downloads (country)

For university staff
	How to post your papers to HUSCAP
	Publication of theses
	Helpline about theses publication

Open Archives Compliant

You can search our collection also at:
	Google
	Google Scholar
	CiNii
	IRDB
	OAIster
	NDLTD

Hokkaido University Collection of Scholarly and Academic Papers >
Theses >
博士　（医学） >

覚醒剤精神病モデルラットにおけるgamma-aminobutyric acid(GABA) : benzodiazepine神経伝達系の役割について

Files in This Item:

000000336533.pdf

25.61 MB

PDF

View/Open

Please use this identifier to cite or link to this item:https://doi.org/10.11501/3151343

Title:	覚醒剤精神病モデルラットにおけるgamma-aminobutyric acid(GABA) : benzodiazepine神経伝達系の役割について
Other Titles:	The Role of Gamma-aminobutyric Acid (GABA) : Benzodiazepine Neurotransmission in the Animal Modei of Methamphetamine-induced Psychosis
Authors:	伊藤, 耕一¹ Browse this author
Authors(alt):	Ito, Kouich¹
Keywords:	Methamphetamine
	Sensitization
	Clonazepam
	Flumazenil
	Benzodiazepine
	GABA
Issue Date:	25-Mar-1999
Publisher:	Hokkaido University
Abstract:	Repeated administration of amphetamine or methamphetamine (MA) results in an augmentation of its locomotor activating effects, a phenomenon known as behavioral sensitization. In humans, the chronic use of the drug elicits a progressive augmentation in paranoid symptoms that closely resemble schizophrenia. Behavioral sensitization has some common properties with other forms of neural plasticity such as kindling, learning and long-term potentiation (LTP). The present study examined whether behavioral sensitization would be blocked by GABA-benzodiazepine agonists, known to inhibit kindling, learning as well as LTP. Rats (Male Wistar-King rats) treated with MA (1mg/kg, s.c.) for 1O days displayed significantly enhanced motor activity when tested with MA (1mg/kg) after a 7-8 day withdrawal, indicating the acquisition of behavioral sensitization. Pretreatment with clonazepam (CZP) (0.5 and 2.0mg/kg), a GABA-benzodiazepine agonists, prior to MA administration prevented the acquisition of the phenomenon. In contrast, pretreatment with flumazenil (Flu) (1Omg/kg), a GABA-benzodiazepine antagonist, prior to MA administration has no influence on the acquisition of sensitization. However, pretreatment with Flu prior to CZP administration reversed the inhibitory effect of CZP. CZP showed no effect on the expression of sensitization in the sensitized rats when given prior to the MA readminisiration. These results suggest that stimulation of GABA-benzodiazepine receptors plays a role in the acquisition but not in the expression of behavioral sensitization.
Conffering University:	北海道大学
Degree Report Number:	甲第4661号
Degree Level:	博士
Degree Discipline:	医学
Type:	theses (doctoral)
URI:	http://hdl.handle.net/2115/51584
Appears in Collections:	学位論文 (Theses) > 博士　（医学）

Submitter: 伊藤耕一

OAI-PMH ( junii2 , jpcoar_1.0 )

- Hokkaido University