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請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/44524
完整後設資料紀錄
DC 欄位值語言
dc.contributor.advisor邱麗珠
dc.contributor.authorHon Lie-Chenen
dc.contributor.author陳宏烈zh_TW
dc.date.accessioned2021-06-15T03:02:54Z-
dc.date.available2014-09-15
dc.date.copyright2009-09-15
dc.date.issued2009
dc.date.submitted2009-07-30
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行政院衛生署中醫藥委員會. 92 年10 月. 苦藍盤. 臺灣藥用植物資源名錄:387.
dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/44524-
dc.description.abstract本研究源自於本研究團隊的醫師成員於國立台灣大學附設醫院小兒科門診所
發現之個案研究。一位十三歲的病人患有長期抽動症狀,對於多種抗抽動藥物的
反應不佳,直到她自己喝了苦藍盤(Clerodendrum inerme)所打成的汁液,發現
其症狀有明顯地緩解,而且追蹤兩年發現,其肝、腎和血液的功能均正常。紋狀
體的多巴胺 (Striatal dopaminergic)的過度活化被認為在抽動症狀的產生扮演
重要角色,妥瑞氏症也在其中,所以本研究利用甲基安非他命來引發老鼠的過動
症狀當作模型,在開放空間測試(open field test)了一系列由苦藍盤葉萃取出
來的萃取物。結果發現苦藍盤的乙醇萃取物 (10~300 mg/kg, i.p.)可以劑量依存
性地降低甲基安非他命所造成的活動性增加,但在滾輪 (rotarod)測試和抓力測
試 (grip tests)則是沒有影響。接下來又篩了乙醇萃取物下的分層,包含水
(water)、丁醇 (butanol)、二氯甲烷 (dichloromethane)和正己烷 (n-hexane)
分層,結果發現主要的作用成分存在於二氯甲烷 (dichloromethane)和正己烷
(n-hexane)層,再以相同的模型測試,在二氯甲烷 (dichloromethane)層發現了
粗毛豚草素 (hispidulin)是主要的作用成分,並且觀察到粗毛豚草素除了會降低
甲基安非他命所引發的活動性增加之外,還會產生鎮靜的效果。粗毛豚草素已被
研究過是一種γ- 胺基丁酸A 型接受器異位性致效劑 ( GABAA receptor
allosteric agonist),但跟一般的benzodiazepine 不同的地方是他會促進含α6
次單元γ-胺基丁酸A 型接受器 (α6-subunit-containing GABAA receptors),而
這個接受器只有表現在小腦的顆粒細胞上,而且主要的作用是前突觸的抑制作用。
妥瑞氏症病人也表現出感覺運動門控(sensorimotor gating)不良。因此本
研究利用甲基安非他命來引發前脈衝抑制不良,測試粗毛豚草素 (hispidulin)能
否逆轉甲基安非他命所造成的效果。結果發現,粗毛豚草素 (hispidulin) (10~50
iv
mg/kg i.p.) 可以逆轉甲基安非他命引發之前脈衝抑制不良,但diazepam (1 ~10
mg/kg i.p.)則無法逆轉。
然後,我們在老鼠小腦雙側微量注射粗毛豚草素 (hispidulin) 10 nmole/
side 發現可以逆轉甲基安非他命引發之前脈衝抑制不良。接著,將含α6 次單元
γ-胺基丁酸A 型接受器致效劑 (α6-subunit-containing GABAA receptors) 、 含
α1 次單元γ- 胺基丁酸A 型接受器反轉致效劑 (inversed
α1-subunit-containing GABAA receptors) Ro154513 和全γ-胺基丁酸A 型接受
器致效劑 ( All GABAA receptors containg subunit agonist) (包含 α6-subunit)
的loreclezole,小腦微量注射10 nmole/side 發現皆可逆轉甲基安非他命所造成
的前脈衝抑制不良。Ro154513、loreclezole、粗毛豚草素 (hispidulin)以小腦
微量注射10 nmole/side 的效果可以被furosemide (50 nmole i.cb.)所抑制,
furosemide 為α6次單元γ-胺基丁酸A 型接受器 (α6-subunit-containing GABAA
receptors)的抑制劑,這樣的結果顯示粗毛豚草素 (hispidulin)可能是透過促進
小腦內含α6 次單元γ-胺基丁酸A 型接受器 (α6-subunit-containing GABAA
receptors)而達到促進前脈衝抑制的效果。
由於一些神經精神疾病會發生前脈衝抑制不良,包括妥瑞氏症、精神分裂症、
注意力不集中過動症、強迫症,粗毛豚草素 (hispidulin)能否改善這些疾病的前
脈衝抑制功能,還需要進一步探討。
zh_TW
dc.description.abstractThis study was inspired by a case report of one physician member of our
research group in the pediatric neurology clinic of National Taiwan
University Hospital. We found a pediatric patient with chronic motor tic
disorder refractory to multiple anti-tic therapies showed dramatic
improvement and remission after self administration of the grounded leaf
juice of Clerodendrum inerme (CI) with normal hepatic, renal and
hematological functions examined after 2 years' herb administration.
Striatal dopaminergic hyperactivity is believed to play an important role
in motor tic disorders, of which Tourette syndrom one of the spectrum. We,
therefore, using the mouse model of methamphetamine-induced hyperlocomotor
activity in the open-field test, examined the effects of various extraction
fractions from the CI leaves. The ethanol extract of CI (10-300 mg/kg, i.p.)
dose-dependently reduced methamphetamine-induced hyperactivity but had no
significant effect in the rotarod, except at higher doses, and grip tests
per se. We further screened the sub-fractionations of the ethanol extract,
including water, butanol, dichloromethane and n-hexane extracts, and found
the active component(s) were present in the fractions of dichloromethane
vi
and n-hexane. Through the bioassay guided isolation, we found that
hispidulin was one of the active costituents. In addition to reducing
methamphetamine-induced hyperactivity, hispidulin also had hypnotic
/sedative effect. Hispidulin has been proved to be a GABAA receptor
allosteric agonist, but unlike benzodiazepine, was effective in α6-
subunit-containing GABAA receptors. These receptors are exclusively
expressed in the cerebellar granule cells and mediate the presynaptic
inhibitory tone on these neurons.
Patients with Tourette syndrome also manifest with sensorimotor gating
deficit. We, therefore, examined if hispidulin could rescue
methamphetamine-induced impairment of prepulse inhibition (PPI) of the
startle response in mice, an animal model of sensorimotor gating.
Hispidulin (10~50 mg/kg), but not diazepam (1~10 mg/kg), when given by
intraperitoneal injection rescued methamphetamine-induced PPI impairment.
Bilateral microininjection of hispiduline, but not diazepam, at 10 nmole
/side also rescued rescued methamphetamine-induced PPI impairment.
Futhermore, microinjection of Ro154513, an agonist α6-subunit-containing
GABAA receptors and an inversed α1-subunit-containing GABAA receptors, and
vii
loreclezole, all the GABAA receptors containg subunits, including
α6-subunit, also rescued methamphetamine-induced PPI impairment.
The effects of Ro154513, Loreclezole, hispidulin administered by
intra-cerebellar injection (10 nmole/side) were reversed by intracerebellar
microinjected furosemide (50 nmole), These results demonstrate
that hispidulin is the major effective constituent in CI leave extract in
rescuing methamphetamine induced hyperlocomotion and PPI impairment. The
latter effect might be mediated by theα6-subunit-containing GABAA
receptors in the cerebellum. Several neuropsychiatric disorders, including
TS, schizophrenia, attention deficit hyerreactivity disorder and obsessive
compulsive disorder, also have impaired PPI. It remains to be further
elucidated if hispidulin might also be beneficial in improving the
sensorimotor gating problems in these diseases.
en
dc.description.provenanceMade available in DSpace on 2021-06-15T03:02:54Z (GMT). No. of bitstreams: 1
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Previous issue date: 2009
en
dc.description.tableofcontents7
目 錄
口試委員會審定書………………………………………………………i
誌謝………………………………………………………………… i i
中文摘要… … … … … … … … … … … … … … … … … … … i i i
英文摘要… … … … … … … … … … … … … … … … … … … … v
第一章 前言 …………………………………………………………1
第二章 苦藍盤萃取物對老鼠自發性探索行為的影響………………3
第一節 緒論………………………………………………………4
第二節 實驗設計與研究方法……………………………………9
第三節 實驗結果…………………………………………………11
第三章 Hispidulin 對於前脈衝抑制的影響 …………………15
第一節 緒論………………………………………………………16
第二節 實驗設計與研究方法……………………………………24
第三節 實驗結果…………………………………………………27
第四章 討論……………………………………………………………31
第五章 結論與展望……………………………………………………38
第六章 附圖………………………………………………………40
第七章 參考文獻……………………………………………… 6 1
dc.language.isozh-TW
dc.titleCI 植物萃取物抑制甲基安非他命引發老鼠的活動力增加與前脈衝抑制缺損之研究zh_TW
dc.titleThe Clerodendrum inerme extracts inhibited the
hyperlocomotor activity and impairment of prepulse
inhibition induced by methamphetamine in mice
en
dc.typeThesis
dc.date.schoolyear97-2
dc.description.degree碩士
dc.contributor.oralexamcommittee陶寶綠,何英剛,陳景宗,賴文崧
dc.subject.keyword小腦,妥瑞氏症,多巴胺,zh_TW
dc.subject.keywordcerebellum,dopamine,en
dc.relation.page71
dc.rights.note有償授權
dc.date.accepted2009-07-30
dc.contributor.author-college醫學院zh_TW
dc.contributor.author-dept藥理學研究所zh_TW
顯示於系所單位:藥理學科所

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