人類肺癌抑癌基因之探討

Yi-Jiun Wu; 吳怡君

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/18464

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DC 欄位	值	語言
dc.contributor.advisor	顏伯勳
dc.contributor.author	Yi-Jiun Wu	en
dc.contributor.author	吳怡君	zh_TW
dc.date.accessioned	2021-06-08T01:06:33Z	-
dc.date.copyright	2014-10-09
dc.date.issued	2014
dc.date.submitted	2014-08-19
dc.identifier.citation	1. Collins, L. G., C. Haines, R. Perkel, and R. E. Enck. 2007. Lung cancer: diagnosis and management. Am Fam Physician 75:56-63. 2. Downward, J., P. Parker, and M. D. Waterfield. 1984. Autophosphorylation sites on the epidermal growth factor receptor. Nature 311:483-485. 3. Hirsch, F. R., M. Varella-Garcia, P. A. Bunn, Jr., M. V. Di Maria, R. Veve, R. M. Bremmes, A. E. Baron, C. Zeng, and W. A. Franklin. 2003. Epidermal growth factor receptor in non-small-cell lung carcinomas: correlation between gene copy number and protein expression and impact on prognosis. J Clin Oncol 21:3798-3807. 4. Ladanyi, M., and W. Pao. 2008. Lung adenocarcinoma: guiding EGFR-targeted therapy and beyond. Mod Pathol 21 Suppl 2:S16-22. 5. Lowenstein, E. J., R. J. Daly, A. G. Batzer, W. Li, B. Margolis, R. Lammers, A. Ullrich, E. Y. Skolnik, D. Bar-Sagi, and J. Schlessinger. 1992. The SH2 and SH3 domain-containing protein GRB2 links receptor tyrosine kinases to ras signaling. Cell 70:431-442. 6. Ma, C., S. Wei, and Y. Song. 2011. T790M and acquired resistance of EGFR TKI: a literature review of clinical reports. J Thorac Dis 3:10-18. 7. Molina, J. R., P. Yang, S. D. Cassivi, S. E. Schild, and A. A. Adjei. 2008. Non-small cell lung cancer: epidemiology, risk factors, treatment, and survivorship. Mayo Clin Proc 83:584-594. 8. Olayioye, M. A., R. M. Neve, H. A. Lane, and N. E. Hynes. 2000. The ErbB signaling network: receptor heterodimerization in development and cancer. EMBO J 19:3159-3167. 9. Schlessinger, J. 2000. Cell signaling by receptor tyrosine kinases. Cell 103:211-225. 10. Schlessinger, J. 2002. Ligand-induced, receptor-mediated dimerization and activation of EGF receptor. Cell 110:669-672. 11. Sebastian, S., J. Settleman, S. J. Reshkin, A. Azzariti, A. Bellizzi, and A. Paradiso. 2006. The complexity of targeting EGFR signalling in cancer: from expression to turnover. Biochim Biophys Acta 1766:120-139. 12. Sharma, S. V., D. W. Bell, J. Settleman, and D. A. Haber. 2007. Epidermal growth factor receptor mutations in lung cancer. Nat Rev Cancer 7:169-181. 13. Song, H., M. Hollstein, and Y. Xu. 2007. p53 gain-of-function cancer mutants induce genetic instability by inactivating ATM. Nat Cell Biol 9:573-580. 14. Stewart, B. W. W., C. P. 2014. World Cancer Report 2014. World Health Organization & International Agency for Research on Cancer. 15. Zwick, E., P. O. Hackel, N. Prenzel, and A. Ullrich. 1999. The EGF receptor as central transducer of heterologous signalling systems. Trends Pharmacol Sci 20:408-412.
dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/18464	-
dc.description.abstract	肺癌高居世界癌症相關死因的首位，每年有超過150萬人死於肺癌。罹患肺癌的病人預後情況相當不理想，五年存活率僅約15%。據研究指出在肺癌中表皮生長因子受體 (epidermal growth factor receptor；EGFR) 常受到不正常的調控，如此異常表現將導致訊息傳遞改變造成肺癌病人不良的預後。之前的研究發現一轉錄因子LCTS1 (Lung Cancer Tumor Suppressor 1) 可作為一個腫瘤抑制基因。然而，目前尚未出現此因子對於人類肺癌細胞抑癌作用的研究，因此本論文以人類肺癌細胞株為研究模式，探討此轉錄因子是否對於人類肺癌細胞株具有抑癌作用，而其抑癌作用是否透過影響EGFR訊息傳遞路徑進行調控。我們首先建立可被四環黴素 (doxycycline) 誘導表現此轉錄因子的各種肺癌細胞，探討它的表現對肺癌細胞的生長與基因表現的影響。我們發現在肺癌細胞中誘導此轉錄因子表現，會使細胞群落形成的能力顯著減弱，同時伴隨著EGFR蛋白質的明顯下降。接著，我們釐清EGFR蛋白質表現量下降的原因，發現高度表現此轉錄因子對EGFR的訊息傳遞核糖核酸 (mRNA) 表現量影響的比例不高，且由報導基因分析技術 (reporter gene analysis) 中，發現此轉錄因子並不影響EGFR的轉錄作用。接著，我們進一步證明此轉錄因子影響EGFR蛋白的穩定度，高度表現此轉錄因子後，肺癌細胞EGFR較不穩定，容易被降解。而EGFR下游訊號傳遞路徑，磷酸化Akt的表現量也明顯地減少。綜合以上結果，我們認為此轉錄因子在肺癌中能當作一種潛在性的腫瘤抑制基因，然而其詳細的功能與機制仍需日後進一步的探討。	zh_TW
dc.description.abstract	Lung cancer, the leading cause of cancer-related deaths worldwide, is responsible for more than 1.5 million deaths annually. The overall 5-year survival rate for patients with lung cancer is less than 15%. It has been reported that epidermal growth factor receptor (EGFR) is usually abnormal in lung cancer and its expression is correlated with poor prognosis. Previously, we identified LCTS1 (Lung Cancer Tumor Suppressor 1) as a candidate gene associated with disease progress of lung cancer. However, the precise role and molecular mechanisms of the factor in lung cancer remain unclear. Therefore, the objective of this study is to identify the functional role and potential contribution of the LCTS1 in lung cancer. We overexpressed the LCTS1 in several lung cancer cell lines under the control of doxycycline and found that overexpression of the protein in lung cancer cell lines dramatically decreased the ability of colony formation as well as the EGFR protein level. In addition, we showed that down-regulation of EGFR protein level was not due to the change of EGFR transcriptional ability but resulted from the instability of EGFR protein. Our results suggested that the LCTS1 may function as a tumor suppressor in lung cancer. However, the detailed mechanisms and functions of the LCTS1 need to be further elucidated in the future.	en
dc.description.provenance	Made available in DSpace on 2021-06-08T01:06:33Z (GMT). No. of bitstreams: 1 ntu-103-R01442010-1.pdf: 2223883 bytes, checksum: b3a2349d7cd6c0d9561a345c61e84253 (MD5) Previous issue date: 2014	en
dc.description.tableofcontents	誌謝 i 摘要 ii Abstract iii 目錄 iv 圖目錄 vii 表目錄 viii 第一章緒論 1 1.1 肺癌 1 1.1.1 流行病學 1 1.1.2 組織學分類與治療 1 1.2 表皮生長因子受體 (Epidermal growth factor receptor；EGFR) 2 1.2.1 EGFR的簡介 2 1.2.2 EGFR的去活化 3 1.2.3 EGFR與肺癌的關係 3 1.3 LCTS1 (Lung Cancer Tumor Suppressor 1) 4 1.3.1 LCTS1腫瘤抑制基因 4 1.4 研究目的 4 第二章材料與方法 6 2.1 質體及其建構 (Plasmids and construction) 6 2.1.1 pHAGE-TRE-LCTS1 full length-UBC-rtTA-IRES-PuroR 6 2.1.2 pHAGE-TRE-eGFP-UBC-rtTA-IRES-PuroR 6 2.1.3 pHAGE-TRE-LCTS1 short form (Δ3)-UBC- rtTA-IRES-PuroR 6 2.2 細胞株培養 (Cell culture) 7 2.3 藥物處理 (Drug treatment) 7 2.3.1 四環黴素 (Doxycycline；DOX) 7 2.3.2 環己醯亞胺 (Cycloheximide；CHX) 7 2.3.3 表皮生長因子 (Epidermal growth factor；EGF) 8 2.3.4 MG132 8 2.4 DNA轉染 (Transfection) 8 2.5 慢病毒顆粒製備與感染 (Lentivirus particle production and infection) 8 2.6 細胞蛋白質之收取 9 2.7 蛋白質定量 9 2.8 正十二烷硫酸鈉-聚丙烯醯胺膠體電泳(SDS-polyacrylamide gel electrophoresis；SDS-PAGE) 9 2.9 西方墨點法 (Western blot analysis) 10 2.10 細胞群落形成分析 (Colony formation assay) 11 2.11 核糖核酸萃取 (RNA extraction) 11 2.12 反轉錄反應 (Reverse transcription) 11 2.13 即時定量聚合酶連鎖反應 (Quantitative real-time polymerase chain reaction ) 12 2.14 報導基因分析 (Reporter gene analysis) 12 2.15 免疫沉澱 (Immunoprecipitation) 13 2.16 統計分析 (Statistical analysis) 13 第三章實驗結果 14 3.1 建立可藉由誘導表現LCTS1的細胞株 14 3.2 LCTS1對於肺癌細胞增殖作用的影響 14 3.3 LCTS1對於EGFR訊息傳遞的影響 15 3.4 LCTS1對於EGFR轉錄作用的影響 15 3.5 LCTS1對於EGFR蛋白穩定的影響 16 3.6 LCTS1對於p21、PUMA mRNA表現量的影響 16 第四章討論 18 參考文獻 20 附錄 22
dc.language.iso	zh-TW
dc.title	人類肺癌抑癌基因之探討	zh_TW
dc.title	Investigation of a Potent Tumor Suppressor in Human Lung Cancer	en
dc.type	Thesis
dc.date.schoolyear	102-2
dc.description.degree	碩士
dc.contributor.oralexamcommittee	陳美齡,林敬哲
dc.subject.keyword	肺癌,抑癌基因,表皮生長因子受體,蛋白穩定度,	zh_TW
dc.subject.keyword	lung cancer,tumor suppressor gene (TSG),epidermal growth factor receptor (EGFR),protein stability,	en
dc.relation.page	43
dc.rights.note	未授權
dc.date.accepted	2014-08-19
dc.contributor.author-college	醫學院	zh_TW
dc.contributor.author-dept	生物化學暨分子生物學研究所	zh_TW
顯示於系所單位：	生物化學暨分子生物學科研究所

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