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研究生: 張文騰
Wen-Teng Chang
論文名稱: 台灣族群帕金森氏症Leucine-Rich Repeat Kinase 2 (LRRK2) 基因變異的分子功能研究
Molecular Characterization of LRRK2 Variations in Taiwanese Parkinson’s Disease
指導教授: 李桂楨
Lee, Guey-Jen
學位類別: 碩士
Master
系所名稱: 生命科學系
Department of Life Science
論文出版年: 2011
畢業學年度: 99
語文別: 中文
論文頁數: 60
中文關鍵詞: 帕金森氏症神經退化性疾病震顫素
英文關鍵詞: Parkinson's disease, neurodegenerative disease, dardarin
論文種類: 學術論文
相關次數: 點閱:691下載:13
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    • PARK8基因座的LRRK2 (全名leucine-rich repeat kinase 2)基因,其突變會導致體染色體顯性的帕金森氏症。LRRK2蛋白具有多個功能區域,於神經系統、大部份器官及淋巴細胞等都有表現。新穎的R767H、S885N變異及已報導過的R1441H變異,是本實驗室在臺灣帕金森氏症患者發現的突變點,R1628P和G2385R兩變異則是華人帕金森氏症的危險因子。本論文首先建構EGFP標記的野生型及R1441H、R1628P、G2385R變異的LRRK2質體(含S1647T、M2397T多型性),送到HEK-293T細胞中表現,經共軛焦顯微鏡觀察、西方轉漬分析研究,顯示上述變異對LRRK2蛋白在細胞內的位置及合成皆無受到影響。其次選殖α-synuclein cDNA,與R767H、S885N、R1441H、G2019S (白種人常見,作為對照)突變的LRRK2質體共轉染入SK-N-SH細胞,經細胞免疫螢光染色及共軛焦顯微鏡觀察,顯示野生型LRRK2廣泛分佈在細胞質並與α-synuclein有些微連繫。突變的R767H、S885N、R1441H、G2019S亦主要分佈在細胞質,R1441H和G2019S的LRRK2容易形成不含α-synuclein且鄰近細胞核的聚集。進一步的表現上述LRRK2質體於HEK-293T細胞二至六天後,螢光顯微鏡觀察及定量統計結果顯示R1441H和G2019S較野生型的LRRK2顯著地容易誘導更多的包涵體。最後,選殖V5標記的ARHGEF7 cDNA,並建構不含S1647T、M2397T多型性的Myc-His標記的LRRK2質體,共轉染入HEK-293T細胞,進行免疫共沉澱與GTP結合能力試驗的分析,結果發現S885N、R1441H、G2019S等突變影響LRRK2蛋白與ARHGEF7的交互作用。

    Mutations in PARK8 associated leucine-rich repeat kinase 2 (LRRK2) have been shown to be the leading cause of autosomal dominant Parkinson's disease (PD). The multidomain LRRK2 is expressed ubiquitously, including the central nervous system and various organs. Previously novel R767H, S885N and reported R1441H were found in Taiwanese PD patients, in addition to R1628P and G2385R risk factors in ethnic Chinese populations. In the first part of this study, EGFP-tagged wild type, R1441H, R1628P and G2385R LRRK2 constructs (with S1647T and M2397T SNPs) were prepared for transient expression in HEK-293T cells. Western blot analysis and fuorescence microscopy examination revealed that neither localization nor processing of LRRK2 was affected by R1441H, R1628P and G2385R variations. Secondly, α-synuclein cDNA was cloned and co-transfected with the EGFP-tagged wild type or mutant (R767H, S885N, R1441H, G2019S) LRRK2 constructs in SK-N-SH cells. Confocal microscopy examination revealed that wild-type LRRK2 was widespread cytoplasmic and partially in association with α-synuclein. The distribution of R767H and S885N proteins were also mainly in cytoplasm. In contrast, both R1441H and G2019S (included as an aggregation control) LRRK2 mutants formed α-synuclein-negative perinuclear aggregates in a smaller, but still appreciable, proportion of cells, in addition to cytoplasmic distribution. Fluorescent microscopy examination and quantitation of the number of cells with LRRK2-EGFP fluorescent aggregates out of the transfected HEK-293T cell population further revealed that R1441H and G2019S both induced significant more inclusions as compared to wild-type LRRK2. Finally, V5-tagged ARHGEF7 cDNA was cloned and co-expressed with the Myc-tagged wild type or mutant (R767H, S885N, R1441H, G2019S) LRRK2 constructs in HEK-293T cells. Co-immunoprecipitation assay revealed that S885N, R1441H and G2019S reduced interaction between LRRK2 and ARHGEF7.

    目錄 I 中文摘要 VI Abstract VII 圖表目錄 VIII 壹、緒論 1 一、帕金森氏症 1 (一)臨床病徵 1 (二)神經病理學 2 (三)病因學 2 二、帕金森氏症的遺傳分析 4 三、LRRK2基因 5 (一) LRRK2的構造、表現與功能 6 (二) LRRK2基因變異與帕金森氏症 6 貳、研究目的 8 參、研究材料與方法 9 一、R1441H、R1628P、G2385R對LRRK2蛋白在細胞內的位置及合成的影響 9 (一) EGFP標記的LRRK2 cDNA質體建構 9 (二)細胞培養 10 (三)基因轉染(Transfection) 10 (四)西方轉漬法(Western blot) 11 (五)共軛焦顯微鏡觀察 12 (1)觀察LRRK2- EGFP融合蛋白於細胞中的表現…..…..….12 (2)觀察LRRK2- EGFP與粒腺體重疊情形 13 (3)觀察LRRK2- EGFP與溶小體重疊情形 13 (4)觀察LRRK2- EGFP與內質網重疊情形 13 二、R767H、S885N、R1441H、G2019S突變的LRRK2形成聚集的情形 14 (一) α-synuclein cDNA選殖 14 (二) EGFP標計的LRRK2 cDNA質體建構 14 (三)細胞培養 15 (四)基因共轉染(co-transfection) 15 (五)細胞免疫螢光染色及螢光顯微鏡觀察 16 (六)活細胞影像儀觀察 17 三、R767H、S885N、R1441H、G2019S突變的LRRK2形成二元體的情形 17 (一) Myc-His標記的LRRK2質體建構 17 (二) 基因轉染及西方轉漬分析 18 (三) LRRK2-Myc-His與LRRK2-EGFP形成二元體的分析 18 四、R767H、S885N、R1441H、G2019S等突變的LRRK2蛋白與ARHGEF7蛋白結合測試 19 (一) ARHGEF7 cDNA選殖 19 (二) LRRK2與ARHGEF7蛋白的免疫共沉澱分析 20 肆、結果 22 一、R1441H、R1628P、G2385R對LRRK2蛋白在細胞內的位置及合成的影響 22 (一) EGFP標記的LRRK2 cDNA選殖 22 (二) 西方轉漬法分析R1441H、R1628P、G2385R對LRRK2合成的影響 22 (三) LRRK2-EGFP的共軛焦螢光顯微鏡觀察 23 二、R767H、S885N、R1441H、G2019S突變的LRRK2形成聚集的情形 23 (一) α-synuclein cDNA選殖 23 (二) EGFP標記的LRRK2/G2019S cDNA質體 23 (三) α-synuclein免疫螢光染色及共軛焦螢光顯微鏡觀察 24 (四)活細胞影像儀觀察突變的LRRK2形成聚集的情形 24 三、R767H、S885N、R1441H、G2019S突變的LRRK2形成二元體的情形 24 (一) Myc-His標記的LRRK2 cDNA 25 (二) Myc-His標記的LRRK2 cDNA表現 25 (三) LRRK2-Myc-His、LRRK2-EGFP蛋白的二元化情形 26 四、R767H、S885N、R1441H、G2019S等突變的LRRK2蛋白的與ARHGEF7蛋白的結合情形 26 (一) ARHGEF7 cDNA選殖 26 (二) LRRK2與ARHGEF7蛋白間交互的作用 27 伍、討論 28 一、R1441H、R1628P、G2385R對LRRK2蛋白在細胞內的位置及合成的影響 28 二、R767H、S885N、R1441H、G2019S突變的LRRK2形成聚集的情形 29 三、R767H、S885N、R1441H、G2019S突變的LRRK2形成二元體的情形 30 四、R767H、S885N、R1441H、G2019S等突變的LRRK2蛋白與ARHGEF7蛋白的交互作用 31 陸、參考文獻 33 柒、附錄圖表 42

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