政大機構典藏-National Chengchi University Institutional Repository(NCCUR):Item 140.119/55324
English  |  正體中文  |  简体中文  |  Post-Print筆數 : 27 |  全文笔数/总笔数 : 113311/144292 (79%)
造访人次 : 50891650      在线人数 : 616
RC Version 6.0 © Powered By DSPACE, MIT. Enhanced by NTU Library IR team.
搜寻范围 查询小技巧:
  • 您可在西文检索词汇前后加上"双引号",以获取较精准的检索结果
  • 若欲以作者姓名搜寻,建议至进阶搜寻限定作者字段,可获得较完整数据
  • 进阶搜寻


    请使用永久网址来引用或连结此文件: https://nccur.lib.nccu.edu.tw/handle/140.119/55324


    题名: 大腦多巴胺的認知功能:以動物的風險選擇行為模式 (I)
    其它题名: Cognitive Function of Brain Dopamine--- Animal Behavior Model of Risky Choice
    作者: 廖瑞銘;楊立行
    贡献者: 國立政治大學心理學系
    行政院國家科學委員會
    关键词: 風險選擇;大腦多巴胺系統;酬賞動機;神經毒素破壞;藥理檢測;數學公設模擬
    risky choice;brain dopamine systems;reward motivation;neurotoxin lesion;pharmacological evaluation;axiomatic modeling
    日期: 2010
    上传时间: 2012-11-08 14:05:49 (UTC+8)
    摘要: 探討決策認知行為的神經基礎,是最近神經科學研究的重點之一。決策選擇背後的動機因素,是多種認知行為內含的核心歷程。神經科學研究大腦內多巴胺主導行為發展與建構初等級之酬賞動機議題的工作雖然都是持續的在推展,但是對於與酬賞相關的較高等認知學習功能的議題研究則仍有許多不明之處,例如:以成本利益為分析導向的決策。雖然與這個例子有關的延宕酬賞減扣的研究已於近期開始受到注意,但對於另一類由不等機率況下獲得酬賞影響的減扣效果所致之行為反應(又稱風險選擇),則尚有更多待釐清其行為神經機制之處。已有漸增的文獻指出大腦多巴胺有參與注意力歷程,或以成本利益分析行為增強的歷程,或甚至預測失誤之心智監控反應。本研究循此進一步假設大腦多巴胺的行為功能與風險選擇是有關的,然而這項假設尚未建立嚴謹實驗控制的資料,特別是針對鼠類動物實驗探討風險選擇行為的神經機制。據此,本研究計劃將以三年的時間設定六項實驗以檢視大腦多巴胺是如何參與支配風險選擇行為。實驗一及實驗二分別操弄獲較高酬賞的風險機率、不等的期望值、及不同動機狀態,有系統的測試以建立鼠類動物在T 型迷津上的風險選擇行為。實驗三操弄神經毒素破壞八個大腦多巴胺有關的腦區部位,以測試其對風險選擇行為表現的影響效果。實驗四就其中有明顯破壞影響效果的腦區,針對在該區的多巴胺D1 及D2 亞型受器,以周邊及中樞的神經藥理的方式檢視多巴胺致效劑及拮抗劑對風險選擇行為的影響。實驗六將以上述實驗所收集的行為數據建立數學函數,模擬風險選擇行為及其內涵大腦在解剖部位及受器層面的機制。本計畫將以嚴謹的動物實驗操弄大腦多巴胺系統與風險選擇行為所得之動物實驗資料,來剖析大腦多巴胺的認知功能。
    To study the neural mechanisms for cognitive behavior such as decision making is now a major mission in contemporary neuroscience. The motivation involved in decision making or choice is the core of many kinds of cognitive behavior, which could serve as the basis of economical activity in humans and/or other animal species. The progress of investigating the neural mechanisms of brain dopamine (DA) underlying the primary reward motivation to drive the organization and development of behavior has been continuing in neuroscience. However, it remains uncertain about how brain DA systems mediate the higher order cognitive function such as decision making or choice behavior. Despite the issue of delay reward discounting is getting focused in recent years, a similar but in different domain of reward discounting so-called probabilistic reward discounting remains obscure for its underlying neurobehavioral mechanisms. In real life, for all kinds of animals including human, there is no perfect certainty that will (not) lead to a certain end. This type of behavioral phenomena has been studied as the risky choice in the decision science, but not in neuroscience until recently. A growing body of evidence shows that brain DA systems are involved in attention processing, the cost/benefit analysis of behavioral reinforcement, or prediction error. Thus, it is posited that behavioral function of mesocorticolimbic DA systems could be sub-serving for risky choice. However, there is still short of well-controlled empirical data collected from the rodent animal to deal with the neural mechanisms of risky choice. Accordingly, this 3-year project proposes, with six experiments designed, to study how the brain DA systems are involved in risky choice behavior in the rat. First two experiments intend to establish an animal model of risky choice behavior in a T-maze by systemically manipulating the probabilities with different expected values and further tested in different motivational states. Following this animal model set up, Experiment 3 applying neurotoxin lesion techniques will examine whether the performance of risky choice would be affected after the damage of certain brain DA area(s). The eight brain sites to be detected are all related to the terminal areas of the mesocorticolimbic DA systems including the medial prefrontal cortex, orbital frontal cortex, anterior cingulated cortex, nucleus accumbens, dorsolateral striatum, amygdale, dorsal hippocampus and ventral hippocampus. Experiment 4 and Experiment 5 will run neuropharmacological challenges from systemic injection to local infusion of DA agonists and antagonists to verify the role of DA in modulating the performance of risky choice. Experiment 6 will take behavioral data of risky choice into axiomatic modeling, which will be further tested for the fitness or deviation by emerging with other related data of pharmacological tests. This proposed project manipulates dopamine and risky choice behavior, which data collected from these stringent animal experiments are expected to further elaborate the cognitive function of brain dopamine.
    關聯: 基礎研究
    學術補助
    研究期間:9908~ 10007
    研究經費:1286仟元
    数据类型: report
    显示于类别:[心理學系] 國科會研究計畫

    文件中的档案:

    档案 描述 大小格式浏览次数
    99-2410-H004-090-MY2.pdf1935KbAdobe PDF2477检视/开启


    在政大典藏中所有的数据项都受到原著作权保护.


    社群 sharing

    著作權政策宣告 Copyright Announcement
    1.本網站之數位內容為國立政治大學所收錄之機構典藏,無償提供學術研究與公眾教育等公益性使用,惟仍請適度,合理使用本網站之內容,以尊重著作權人之權益。商業上之利用,則請先取得著作權人之授權。
    The digital content of this website is part of National Chengchi University Institutional Repository. It provides free access to academic research and public education for non-commercial use. Please utilize it in a proper and reasonable manner and respect the rights of copyright owners. For commercial use, please obtain authorization from the copyright owner in advance.

    2.本網站之製作,已盡力防止侵害著作權人之權益,如仍發現本網站之數位內容有侵害著作權人權益情事者,請權利人通知本網站維護人員(nccur@nccu.edu.tw),維護人員將立即採取移除該數位著作等補救措施。
    NCCU Institutional Repository is made to protect the interests of copyright owners. If you believe that any material on the website infringes copyright, please contact our staff(nccur@nccu.edu.tw). We will remove the work from the repository and investigate your claim.
    DSpace Software Copyright © 2002-2004  MIT &  Hewlett-Packard  /   Enhanced by   NTU Library IR team Copyright ©   - 回馈