顫抖症藥物療效差異的小腦機制：以神經活動的時空同步性做探討

陳亮穎; Liang-Ying Chen

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/102180

完整後設資料紀錄

DC 欄位	值	語言
dc.contributor.advisor	潘明楷	zh_TW
dc.contributor.advisor	Ming-Kai Pan	en
dc.contributor.author	陳亮穎	zh_TW
dc.contributor.author	Liang-Ying Chen	en
dc.date.accessioned	2026-03-18T16:11:09Z	-
dc.date.available	2026-03-19	-
dc.date.copyright	2026-03-18	-
dc.date.issued	2025	-
dc.date.submitted	2025-06-24	-
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dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/102180	-
dc.description.abstract	原發性顫抖（Essential Tremor, ET）是最常見的運動障礙疾病，其主要特徵為動作性顫抖。儘管盛行率高，目前藥物療效普遍有限，且不同顫抖亞型對藥物反應差異顯著，反映其病理機轉可能並不相同。本研究結合體內電生理記錄與雙光子鈣影像技術，探討兩種顫抖小鼠模型中的神經機制，分別為對藥物反應有效的 harmaline 誘導模型與對藥物具抗性的 Grid2dupE3 模型。在時間編碼層面，兩種模型在產生顫抖頻率的群體編碼機制上高度相似：無論單一神經元的放電頻率為何，多個神經元的平均放電頻率會趨近於各自模型的顫抖頻率。然而，在空間同步性分析中，我們觀察到小腦蒲肯野細胞（Purkinje cell, PC）在兩模型中的活動模式存在顯著差異：harmaline 小鼠呈現區域性同步，而 Grid2dupE3小鼠則表現出全域性同步。我們將進一步透過計算模型與藥物測試，驗證此同步性差異是否為造成兩者藥物反應差異的關鍵因素。本研究結果顯示，兩種顫抖模型在小腦神經迴路動態上存在差異，這些差異可能與其對藥物反應的不同有所關聯。我們期許後續的計算模型研究能進一步釐清這類關聯，協助預測治療反應，並為原發性顫抖更有效治療策略的開發提供參考依據。	zh_TW
dc.description.abstract	Essential tremor (ET), the most prevalent movement disorder, is primarily characterized by action tremor. Despite its high prevalence, fewer than 50% of patients respond effectively to current medications, and the development of new treatments has largely stagnated in recent years. Importantly, patients with different tremor subtypes often exhibit variable responses to the same pharmacological therapies. In this study, we employed in vivo electrophysiology and two-photon calcium imaging to investigate the underlying neuronal mechanisms in two mouse models of tremor: the drug-responsive harmaline-induced tremor model and the drug-refractory Grid2dupE3 model. At the level of temporal coding, we found that the population-level mechanism responsible for generating tremor frequency was similar in both models: the activity frequencies of multiple neurons converged toward the tremor frequency, regardless of its precise value. However, spatiotemporal neural dynamics revealed a striking difference in cerebellar Purkinje cell (PC) synchrony. In harmaline mice, PC activity exhibited regional synchrony, whereas in Grid2dupE3 mice, PC activity exhibited widespread global synchrony. To determine whether this difference in spatial synchrony contributes to the models’ differential drug responses, we plan to perform computational modeling and drug testing. We speculate that the divergent drug responses in the two tremor models may be linked to differences in cerebellar network activity. We anticipate that our forthcoming modeling efforts will aid in predicting treatment outcomes and inform the development of more effective therapies for ET.	en
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dc.description.tableofcontents	Table of contents 致謝 I 摘要 III Abstract IV Table of contents VI List of figures VIII Chapter 1 - Introduction 1 1.1 Epidemiology and treatment limitations of essential tremor 1 1.2 Pathophysiological heterogeneity of essential tremor 1 1.3 Neural circuitry of the cerebellum 2 1.4 Mouse-based research and analysis 3 1.5 Aim of the study 4 Chapter 2 - Methods 4 2.1 Animals 4 2.2 Force-plate-based tremor measurement in freely moving mice 5 2.3 Optetrode implantation and neural recording 6 2.4 Spike sorting for single units 7 2.5 Burst detection of single unit activities 8 2.6 Vector strength analysis 8 2.7 Correlation spectrum analysis 9 2.8 Tissue clearing and histological validation 9 2.9 Two-photon calcium imaging 10 2.10 2D and 3Danalysis 12 2.11 Statistical analysis 15 Chapter 3 - Results 16 3.1 Harmaline and Grid2dupE3 mice have differential drug responses: 16 3.2 Population coding mechanisms for tremor frequencies are similar in the two mouse models 17 3.3 Regional and global PC spatial synchrony in harmaline and Grid2dupE3 mice, respectively 18 Chapter 4 - Discussion 21 4.1 Two complementary mouse models mimic clinically distinct ET subtypes 21 4.2 Spatial synchrony patterns reflect distinct mechanisms of tremor generation 21 4.3 Divergent mechanisms may underlie the limitations of neuromodulator therapies 22 4.4 Future directions using computational modeling 23 4.5 Limitations 24 Reference 26 Figures 30	-
dc.language.iso	en	-
dc.subject	原發性顫抖症	-
dc.subject	小腦	-
dc.subject	駱駝蓬鹼	-
dc.subject	蒲肯野細胞	-
dc.subject	攀爬纖維	-
dc.subject	藥物反應	-
dc.subject	神經動態學	-
dc.subject	頻率	-
dc.subject	電生理	-
dc.subject	空間同步性	-
dc.subject	活體鈣離子影像	-
dc.subject	雙光子顯微鏡	-
dc.subject	Essential Tremor	-
dc.subject	Cerebellum	-
dc.subject	Harmaline	-
dc.subject	Purkinje cell	-
dc.subject	Climbing fiber	-
dc.subject	Drug response	-
dc.subject	Neural dynamics	-
dc.subject	Frequency	-
dc.subject	Electrophysiology	-
dc.subject	Spatial synchrony	-
dc.subject	in vivo calcium imaging	-
dc.subject	Two-photon microscopy	-
dc.title	顫抖症藥物療效差異的小腦機制：以神經活動的時空同步性做探討	zh_TW
dc.title	The spatiotemporal neurodynamics of tremors and their contributions to the differential therapeutic effects in tremor mouse models.	en
dc.type	Thesis	-
dc.date.schoolyear	113-2	-
dc.description.degree	碩士	-
dc.contributor.oralexamcommittee	羅中泉;朱士維;吳順吉	zh_TW
dc.contributor.oralexamcommittee	Chung-Chuan Lo;Shi-Wei Chu;Shun-Chi Wu	en
dc.subject.keyword	原發性顫抖症,小腦駱駝蓬鹼蒲肯野細胞攀爬纖維藥物反應神經動態學頻率電生理空間同步性活體鈣離子影像雙光子顯微鏡	zh_TW
dc.subject.keyword	Essential Tremor,CerebellumHarmalinePurkinje cellClimbing fiberDrug responseNeural dynamicsFrequencyElectrophysiologySpatial synchronyin vivo calcium imagingTwo-photon microscopy	en
dc.relation.page	60	-
dc.identifier.doi	10.6342/NTU202501258	-
dc.rights.note	同意授權(限校園內公開)	-
dc.date.accepted	2025-06-25	-
dc.contributor.author-college	醫學院	-
dc.contributor.author-dept	藥理學研究所	-
dc.date.embargo-lift	2030-06-22	-
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