Skip navigation

DSpace

機構典藏 DSpace 系統致力於保存各式數位資料(如:文字、圖片、PDF)並使其易於取用。

點此認識 DSpace
DSpace logo
English
中文
  • 瀏覽論文
    • 校院系所
    • 出版年
    • 作者
    • 標題
    • 關鍵字
    • 指導教授
  • 搜尋 TDR
  • 授權 Q&A
    • 我的頁面
    • 接受 E-mail 通知
    • 編輯個人資料
  1. NTU Theses and Dissertations Repository
  2. 理學院
  3. 應用物理研究所
請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/101698
完整後設資料紀錄
DC 欄位值語言
dc.contributor.advisor趙治宇zh_TW
dc.contributor.advisorChih-Yu Chaoen
dc.contributor.author龔毅zh_TW
dc.contributor.authorYi Kungen
dc.date.accessioned2026-02-26T16:48:30Z-
dc.date.available2026-02-27-
dc.date.copyright2026-02-26-
dc.date.issued2026-
dc.date.submitted2026-02-05-
dc.identifier.citation1. Chang JS, Chen LT, Shan YS, Chu PY, Tsai CR, Tsai HJ. The incidence and survival of pancreatic cancer by histology, including rare subtypes: a nation-wide cancer registry-based study from Taiwan. Cancer Med. 2018; 7(11):5775-5788.
2. Wang Y, Yan R, Lu J, Guo J, Teng G. Interventional management of pancreatic cancer: Current strategies and future horizons. Oncology and Translational Medicine. 2025;11:205–212.
3. Zhang X-P, Xu S, Gao Y-X, Zhao Z-M, Zhao G-D, Hu M-G, et al. Early and late recurrence patterns of pancreatic ductal adenocarcinoma after pancreaticoduodenectomy: a multicenter study. International Journal of Surgery. 2023;109(4):785–793.
4. Gupta K, Walton R, Kataria SP. Chemotherapy-Induced Nausea and Vomiting: Pathogenesis, Recommendations, and New Trends. Cancer Treatment and Research Communications. 2021;26:100278.
5. Raheja R, Reddy N, Patel T, Kilambi S, Mathew AA, Majeed A. Classification of Chemotherapy-Induced Febrile Neutropenic Episodes Into One of the Three Febrile Neutropenic Syndromes. Cureus. 2023;15(8):e42843.
6. Dardare J, Martz N, Witz A, Betz M, Michel C, Gilson P, et al. Improving Radiation Therapy in Pancreatic Cancer Through Radiosensitization Strategies. Int J Radiat Oncol Biol Phys. 2026;124(2):395–414.
7. Lendeckel U, Wolke C. Redox-Regulation in Cancer Stem Cells. Biomedicines. 2022;10(10).
8. Zhao Y, Qin C, Zhao B, Wang Y, Li Z, Li T, et al. Pancreatic cancer stemness: dynamic status in malignant progression. J Exp Clin Cancer Res. 2023;42(1):122.
9. Danieli MG, Antonelli E, Piga MA, Cozzi MF, Allegra A, Gangemi S. Oxidative stress, mitochondrial dysfunction, and respiratory chain enzyme defects in inflammatory myopathies. Autoimmun Rev. 2023;22(5):103308.
10. Yu Y, Liu S, Yang L, Song P, Liu Z, Liu X, et al. Roles of reactive oxygen species in inflammation and cancer. MedComm. 2024;5(4):e519.
11. Jomova K, Raptova R, Alomar SY, Alwasel SH, Nepovimova E, Kuca K, et al. Reactive oxygen species, toxicity, oxidative stress, and antioxidants: chronic diseases and aging. Arch Toxicol. 2023;97(10):2499–2574.
12. Murphy MP, Bayir H, Belousov V, Chang CJ, Davies KJA, Davies MJ, et al. Guidelines for measuring reactive oxygen species and oxidative damage in cells and in vivo. Nature Metabolism. 2022;4(6):651–62.
13. Houldsworth A. Role of oxidative stress in neurodegenerative disorders: a review of reactive oxygen species and prevention by antioxidants. Brain Communications. 2024;6(1).
14. Hahm JY, Park J, Jang ES, Chi SW. 8-Oxoguanine: from oxidative damage to epigenetic and epitranscriptional modification. Exp Mol Med. 2022;54(10):1626–42.
15. Huang G, Pan ST. ROS-Mediated Therapeutic Strategy in Chemo-/Radiotherapy of Head and Neck Cancer. Oxid Med Cell Longev. 2020; 2020:5047987.
16. Jagust P, Alcalá S, Sainz Jr B, Heeschen C, Sancho P. Glutathione metabolism is essential for self-renewal and chemoresistance of pancreatic cancer stem cells. World J Stem Cells. 2020;12(11):1410–28.
17. Zhen W, Zhen H, Wang Y, Chen L, Niu X, Zhang B, et al. Mechanism of ERK/CREB pathway in pain and analgesia. Front Mol Neurosci. 2023; 16:1156674.
18. Quan Z, Yin Z, Huang Y, Huang X, Huang H, Mo Q, et al. MiR-766-3p Inhibit the Proliferation, Stemness, and Cell Cycle of Pancreatic Cancer Cells Through the MAPK/ERK Signaling Pathway. Molecular Genetics & Genomic Medicine. 2024;12(12):e70049.
19. Yang Z, Cai W, Chen Y, Guo Z, Xiao Z, Zhou T, et al. Jujuboside B Reverse CUMS-Promoted Tumor Progression via Blocking PI3K/Akt and MAPK/ERK and Dephosphorylating CREB Signaling. J Immunol Res. 2022;2022:5211368
20. Tabrizian N, Nouruzi S, Cui CJ, Kobelev M, Namekawa T, Lodhia I, et al. RETRACTED: ASCL1 is activated downstream of the ROR2/CREB signaling pathway to support lineage plasticity in prostate cancer. Cell Rep. 2023;42(8).
21. Yin Y, Chen F. Targeting human MutT homolog 1 (MTH1) for cancer eradication: current progress and perspectives. Acta Pharm Sin B. 2020 Dec;10(12):2259-2271.
22. Yildirim RM, Seli E. The role of mitochondrial dynamics in oocyte and early embryo development. Semin Cell Dev Biol. 2024;159-160:52–61.
23. Hao Q, Chen J, Lu H, Zhou X. The ARTS of p53-dependent mitochondrial apoptosis. J Mol Cell Biol. 2022;14(10).
24. Lopez A, Reyna DE, Gitego N, Kopp F, Zhou H, Miranda-Roman MA, et al. Co-targeting of BAX and BCL-XL proteins broadly overcomes resistance to apoptosis in cancer. Nature Communications. 2022;13(1):1199.
25. Manogaran P, Beeraka NM, Paulraj RS, Sathiyachandran P, Thammaiappa M. Impediment of Cancer by Dietary Plant-derived Alkaloids Through Oxidative Stress: Implications of PI3K/AKT Pathway in Apoptosis, Autophagy, and Ferroptosis. Curr Top Med Chem. 2023;23(10):860–877.
26. Üremiş N, Üremiş MM, Çiğremiş Y, Tosun E, Baysar A, Türköz Y. Cucurbitacin I exhibits anticancer efficacy through induction of apoptosis and modulation of JAK/STAT3, MAPK/ERK, and AKT/mTOR signaling pathways in HepG2 cell line. J Food Biochem. 2022;46(10):e14333.
27. Douglas H, Weinberg RA. Hallmarks of cancer: the next generation. Cell. 2011; 144(5):646-674.
28. Kari S, Subramanian K, Altomonte IA, Murugesan A, Yli-Harja O, Kandhavelu M. Programmed cell death detection methods: a systematic review and a categorical comparison. Apoptosis. 2022;27(7):482–508.
29. Mustafa M, Ahmad R, Tantry IQ, Ahmad W, Siddiqui S, Alam M, et al. Apoptosis: A Comprehensive Overview of Signaling Pathways, Morphological Changes, and Physiological Significance and Therapeutic Implications. Cells. 2024;13(22).
30. Green DR. The Mitochondrial Pathway of Apoptosis: Part I: MOMP and Beyond. Cold Spring Harb Perspect Biol. 2022;14(5).
31. Morse PT, Arroum T, Wan J, Pham L, Vaishnav A, Bell J, et al. Phosphorylations and Acetylations of Cytochrome c Control Mitochondrial Respiration, Mitochondrial Membrane Potential, Energy, ROS, and Apoptosis. Cells. 2024;13(6).
32. Luo D, Tang X, Wang Y, Ying S, He Y, Lin H, et al. Selenium deficiency exacerbated Bisphenol A-induced intestinal toxicity in chickens: Apoptosis and cell cycle arrest mediated by ROS/P53. Sci Total Environ. 2024;913:169730.
33. I Vermes , C Haanen, H Steffens-Nakken, C Reutelingsperger. A novel assay for apoptosis. Flow cytometric detection of phosphatidylserine expression on early apoptotic cells using fluorescein labelled Annexin V. J. Immunol. Methods. 1995; 184(1):39-51.
34. Rajakumar T, Pugalendhi P. Allyl isothiocyanate regulates oxidative stress, inflammation, cell proliferation, cell cycle arrest, apoptosis, angiogenesis, invasion and metastasis via interaction with multiple cell signaling pathways. Histochem Cell Biol. 2024;161(3):211–21.
35. Tarar A, Peng S, Cheema S, Peng CA. Anticancer Activity, Mechanism, and Delivery of Allyl Isothiocyanate. Bioengineering (Basel). 2022;9(9).
36. Podder A, Kant R, Kumar N, Laishram N, Issrani R, Babu M. Systematic Review of the Inhibitory Effects of Naturally Occurring Isothiocyanates on Human Cytochrome P450 1A1: Implications for Dietary Chemoprevention. J Carcinog. 2025;24:213–20.
37. Sun R, Römhild S, Nakamura Y, Reichelt M, Luck K, Mai DT, et al. Multiple glutathione-S-transferases detoxify diverse glucosinolate-based defenses of Brassicales plants in a generalist lepidopteran herbivore (Spodoptera littoralis). Communications Biology. 2025;8(1):931.
38. Xiao D, Vogel V, Singh SV. Benzyl isothiocyanate-induced apoptosis in human breast cancer cells is initiated by reactive oxygen species and regulated by Bax and Bak. Mol Cancer Ther. 2006; 5(11):2931-2945.
39. Shoaib S, Tufail S, Sherwani MA, Yusuf N, Islam N. Phenethyl Isothiocyanate Induces Apoptosis Through ROS Generation and Caspase-3 Activation in Cervical Cancer Cells. Front Pharmacol. 2021; 12:673103.
40. Chiang JH, Tsai FJ, Hsu YM, Yin MC, Chiu HY, Yang JS. Sensitivity of allyl isothiocyanate to induce apoptosis via ER stress and the mitochondrial pathway upon ROS production in colorectal adenocarcinoma cells. Oncol Rep. 2020; 44(4):1415-1424.
41. Yan-feng LIU, Shao-fan YU, Jia-cheng LI, Yu-hong F, Fu-kun LI. Stability of Allyl Isothiocyanate in an Aqueous Solution. Natural Science of Hainan University. 2011;29(1):33–8.
42. Ribeiro TP, Moreira JA, Monteiro FJ, Laranjeira MS. Nanomaterials in cancer: Reviewing the combination of hyperthermia and triggered chemotherapy. Journal of Controlled Release. 2022;347:89–103.
43. Le Guevelou J, Chirila ME, Achard V, Guillemin PC, Lorton O, Uiterwijk JWE, et al. Combined hyperthermia and radiotherapy for prostate cancer: a systematic review. Int J Hyperthermia. 2022;39(1):547–56.
44. De Maio A, Alfieri G, Mattone M, Ghanouni P, Napoli A. High-Intensity Focused Ultrasound Surgery for Tumor Ablation: A Review of Current Applications. Radiol Imaging Cancer. 2024;6(1):e230074.
45. Ohara G, Okabe K, Toyama N, Ohta Y, Xinman S, Ichimura N, et al. Hyperthermia maintains death receptor expression and promotes TRAIL-induced apoptosis. J Oral Pathol Med. 2023;52(8):718–26.
46. Gorbaslieva I, Quisenaerts T, Bogers J, Peeters M, Saldien V, Ysebaert D. Temperature-Dependent Effects of Induced Hyperthermia, Including Whole-Body Hyperthermia, on the Hallmarks of Cancer: A Systematic Review. Cancers (Basel). 2025;17(23).
47. Richter K, Haslbeck M, Buchner J. The heat shock response: life on the verge of death. Mol Cell. 2010; 40(2):253-266.
48. Helmueller S, Song X, Kim D-H, Lee YJ. The efficacy of hyperthermia-based multimodal therapy is dependent on gatekeeper protein, BID. Int J Hyperthermia. 2025;42(1):2544017.
49. Fajardo LF. Pathological effects of hyperthermia in normal tissues. Cancer Res. 1984; 44(10 Suppl):4826s-4835s.
50. Liu KC, Chen TM. Comparative study of heat transfer and thermal damage assessment models for hyperthermia treatment. J Therm Biol. 2021; 98:102907.
51. Alimoradi H, Matikonda SS, Gamble AB, Giles GI, Greish K. Hypoxia Responsive Drug Delivery Systems in Tumor Therapy. Curr Pharm Des. 2016;22(19):2808–2820.
52. Lu CH, Chen WT, Hsieh CH, Kuo YY, Chao CY. Thermal cycling-hyperthermia in combination with polyphenols, epigallocatechin gallate and chlorogenic acid, exerts synergistic anticancer effect against human pancreatic cancer PANC-1 cells. PLoS One. 2019; 14(5):e0217676.
53. van der Zee J. Heating the patient: a promising approach? Ann Oncol. 2002; 13(8):1173-1184.
54. Ba MC, Long H, Wang S, Wu YB, Zhang BH, Yan ZF, et al. Hyperthermia enhances radiosensitivity of colorectal cancer cells through ROS inducing autophagic cell death. J Cell Biochem. 2018; 119(4):3763-3774.
55. Ba MC, Long H, Cui SZ, Gong YF, Yan ZF, Wang S, et al. Mild hyperthermia enhances sensitivity of gastric cancer cells to chemotherapy through reactive oxygen species-induced autophagic death. Tumour Biol. 2017; 39(6):1010428317711952.
56. Jin HB, Lu L, Xie L, Yang JF, Zhang XF, Ma SL. Concentration changes in gemcitabine and its metabolites after hyperthermia in pancreatic cancer cells assessed using RP-HPLC. Cell Mol Biol Lett. 2019; 24:30.
57. Piao JL, Jin YJ, Li ML, Zakki S, Sun L, Feng Q, et al. Excessive Oxidative Stress in the Synergistic Effects of Shikonin on the Hyperthermia-Induced Apoptosis. Curr Mol Med. 2018;18.
58. Chen WT, Sun YK, Lu CH, Chao CY. Thermal cycling as a novel thermal therapy to synergistically enhance the anticancer effect of propolis on PANC‑1 cells. Int J Oncol. 2019; 55(3):617-628.
59. Zhao B, Qin C, Li Z, Wang Y, Li T, Cao H, et al. Multidrug resistance genes screening of pancreatic ductal adenocarcinoma based on sensitivity profile to chemotherapeutic drugs. Cancer Cell Int. 2022;22(1):374.
60. Tuli HS, Kaur J, Vashishth K, Sak K, Sharma U, Choudhary R, et al. Molecular mechanisms behind ROS regulation in cancer: A balancing act between augmented tumorigenesis and cell apoptosis. Arch Toxicol. 2023;97(1):103–20.
61. Liu Y, Chakravarty S, Dey M. Phenethylisothiocyanate Alters Site- and Promoter-Specific Histone Tail Modifications in Cancer Cells. PLoS One. 2013;8(5):e64535.
62. Zhu X, Zhang Y, Wang Y, Zhang H, Wang X, Tang H, et al. Agrimoniin sensitizes pancreatic cancer to apoptosis through ROS-mediated energy metabolism dysfunction. Phytomedicine. 2022;96:153807.
63. Hu Y, Li R, Jin J, Wang Y, Ma R. Quercetin improves pancreatic cancer chemo-sensitivity by regulating oxidative-inflammatory networks. J Food Biochem. 2022;46(12):e14453.
64. Lu Y, Liu B, Liu Y, Yu X, Cheng G. Dual effects of active ERK in cancer: A potential target for enhancing radiosensitivity. Oncol Lett. 2020; 20(2):993-1000.
65. Acosta-Casique A, Montes-Alvarado JB, Barragán M, Larrauri-Rodríguez KA, Perez-Gonzalez A, Delgado-Magallón A, et al. ERK activation modulates invasiveness and Reactive Oxygen Species (ROS) production in triple negative breast cancer cell lines. Cell Signal. 2023;101:110487.
66. Yan Z, Ohuchida K, Fei S, Zheng B, Guan W, Feng H, et al. Inhibition of ERK1/2 in cancer-associated pancreatic stellate cells suppresses cancer-stromal interaction and metastasis. J Exp Clin Cancer Res. 2019;38(1):221.
67. Hayes TK, Neel NF, Hu C, Gautam P, Chenard M, Long B, et al. Long-Term ERK Inhibition in KRAS-Mutant Pancreatic Cancer Is Associated with MYC Degradation and Senescence-like Growth Suppression. Cancer Cell. 2016;29(1):75–89
68. Lai KC, Lu CC, Tang YJ, Chiang JH, Kuo DH, Chen FA, et al. Allyl isothiocyanate inhibits cell metastasis through suppression of the MAPK pathways in epidermal growth factor‑stimulated HT29 human colorectal adenocarcinoma cells. Oncol Rep. 2014 Jan;31(1):189-196.
69. Ding Y, Liu Q. Targeting the nucleic acid oxidative damage repair enzyme MTH1: a promising therapeutic option. Front Cell Dev Biol. 2024;12:1334417
70. Helleday T. Mitotic MTH1 Inhibitors in Treatment of Cancer. Cancer Treat Res. 2023;186:223–37.
71. Lin GB, Chen WT, Kuo YY, Liu HH, Chen YM, Leu SJ, et al. Thermal cycling‑hyperthermia sensitizes non‑small cell lung cancer A549 cells to EGFR tyrosine kinase inhibitor erlotinib. Oncol Rep. 2025;53(5).		-
dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/101698-
dc.description.abstract胰臟癌為目前臨床上預後最差之惡性腫瘤之一,其高度侵襲性與對傳統化學治療及放射治療之低反應性,使整體存活率長期維持在較低水準。因此,發展具有效性且副作用較低之輔助治療策略,仍為胰臟癌研究的重要課題。異硫氰酸烯丙酯 (allyl isothiocyanate, AITC) 為十字花科植物中常見之具有生物活性之天然化合物,過去研究顯示其具有抑制癌細胞增殖、誘發細胞凋亡及氧化壓力之潛力。然而,AITC於實際應用上仍受限於溶解度不佳、穩定性不足等問題,限制其進一步發展為抗癌治療的手段。
近年來,熱療被視為一種有潛力的癌症輔助治療方式,其中本實驗室提出的循環加熱 (thermal cycling-hyperthermia, TC-HT) 相較於傳統持續高溫熱療,具有對正常細胞傷害較低等優點,並被認為可能透過調控細胞內壓力反應而增強藥物治療效果。然而,TC-HT是否能與AITC產生協同作用,以及其可能涉及之分子機制,仍有待進一步探討。因此,本研究旨在評估TC-HT與AITC聯合處理對胰臟癌細胞之抗癌效果,並分析其對細胞活性、氧化壓力、細胞凋亡及相關蛋白表現之影響。
本研究以人類胰臟癌細胞株PANC-1作為體外細胞模型,分別施予AITC、TC-HT以及兩者聯合處理,以比較不同處理條件下對癌細胞之影響。細胞存活率透過MTT試驗進行評估,細胞凋亡與細胞內活性氧化物 (reactive oxygen species, ROS) 水平之變化則以流式細胞術進行分析,並進一步利用西方墨點法檢測與ROS調節相關蛋白磷酸化ERK與磷酸化CREB,以DNA保護相關蛋白MTH1之表現變化。
  研究結果顯示,AITC或TC-HT單獨處理僅對PANC-1細胞存活率產生有限抑制效果,然而兩者合併處理可顯著降低細胞存活率,並明顯提升細胞凋亡比例,顯示AITC與TC-HT聯合處理可以增強抑制癌細胞活性之效果。此外,聯合處理組的細胞內ROS水平顯著上升,且其增加幅度高於任何單一處理組,顯示TC-HT可放大AITC所誘發之氧化壓力反應。在蛋白水平的分析方面,AITC搭配TC-HT處理可降低磷酸化ERK與磷酸化CREB的表現量,並伴隨MTH1表現量下降,此結果顯示AITC搭配TC-HT的處理方式可能透過干擾調控氧化壓力之相關訊號路徑與DNA的保護機制,使癌細胞對氧化性損傷更為敏感。
  綜合上述結果,本研究顯示TC-HT可有效增強低劑量AITC對PANC-1細胞之抗癌效應,並指出此聯合處理對於氧化壓力及DNA穩定性調控的干擾可能參與其中。本研究成果提供AITC結合TC-HT之抗癌效果的實驗依據,顯示藉由TC-HT的輔助有望克服AITC於臨床上使用的困難,在胰臟癌的治療上具有潛在應用價值,亦可作為後續相關研究之參考基礎。		zh_TW
dc.description.abstractPancreatic cancer is one of the most aggressive malignancies and is associated with poor prognosis. Due to its high invasiveness and low responsiveness to conventional chemotherapy and radiotherapy, overall survival rates remain persistently low. Therefore, the development of effective adjuvant therapies with less adverse effects remains an important issue in pancreatic cancer research. Allyl isothiocyanate (AITC), a naturally occurring bioactive compound commonly found in cruciferous vegetables, has been reported to exhibit anticancer potential, including the inhibition of cancer cell proliferation and the induction of apoptosis and oxidative stress. However, the application of AITC is limited by its poor solubility and insufficient stability, which restrict its further development as an anticancer therapeutic agent.
In recent years, hyperthermia has been considered a promising adjuvant cancer treatment strategy. Thermal cycling–hyperthermia (TC-HT), proposed by our laboratory, has advantages over conventional hyperthermia treatment, including reduced damage to normal cells, and is thought to enhance therapeutic efficacy by modulating cellular stress responses. However, whether TC-HT can provide synergistic effects with AITC and the underlying molecular mechanisms remain unclear. Therefore, this study aimed to evaluate the anticancer effects of combined TC-HT and AITC treatment on pancreatic cancer cells and to analyze its effects on cell viability, oxidative stress, apoptosis, and the expression of related proteins.
In this study, we used the human pancreatic cancer cell line PANC-1 as an in vitro model. Cells were treated with AITC, TC-HT, or a combination of both treatments to evaluate their entire cancer effects. Cell viability was assessed using the MTT assay, while apoptosis and intracellular reactive oxygen species (ROS) levels were analyzed by flow cytometry. In addition, Western blot analysis was performed to examine the expression levels of ROS-regulating proteins phosphorylated ERK and phosphorylated CREB, and the DNA protective protein MTH1.
The results demonstrated that either AITC or TC-HT exerted only limited inhibitory effects on PANC-1 cell viability. In contrast, the combined treatment significantly reduced cell viability and markedly increased apoptotic cell populations, indicating a synergistic effect between AITC and TC-HT. Moreover, ROS levels were significantly elevated in the combined treatment group, with a greater increase than that observed in either treatment alone, suggesting that TC-HT amplified AITC-induced oxidative stress. At the protein level, the combined treatment reduced the expression of phosphorylated ERK and phosphorylated CREB, accompanied by a decrease in MTH1 expression, implying increased susceptibility of cancer cells to oxidative damage. Collectively, these findings indicate that TC-HT effectively enhances the anticancer effects of low-dose AITC in PANC-1 cells and may help overcome the limitations associated with AITC application.		en
dc.description.provenanceSubmitted by admin ntu (admin@lib.ntu.edu.tw) on 2026-02-26T16:48:30Z
No. of bitstreams: 0		en
dc.description.provenanceMade available in DSpace on 2026-02-26T16:48:30Z (GMT). No. of bitstreams: 0en
dc.description.tableofcontents口試委員會審定書 i
誌謝 ii
摘要 iii
ABSTRACT v
目 次 vii
圖 次 x
第一章 緒論與文獻回顧 1
1.1 胰臟癌簡介 1
1.2 活性氧化物質 (reactive oxygen species, ROS) 簡介 2
1.3 ERK / CREB訊息傳遞路徑與癌細胞存活調控 2
1.4 MTH1與氧化損傷防禦機制 3
1.5 細胞凋亡 (apoptosis) 簡介 3
1.6 藥物簡介:異硫氰酸烯丙酯 (allyl isothiocyanate, AITC) 4
1.7 傳統熱療法與循環加熱簡介 6
1.8 藥物與熱療法的結合 6
第二章 實驗材料與方法 8
2.1 細胞株的冷凍保存與培養 8
2.1.1 細胞培養液 8
2.1.2 細胞株的解凍復甦 8
2.1.3 細胞株的繼代培養 9
2.1.4 細胞株的冷凍保存 10
2.2 細胞之藥物與加熱處理 10
2.2.1 細胞的分盤 10
2.2.2 藥物的處理 10
2.2.3 TC-HT處理方式 11
2.3 MTT assay測量細胞存活率 12
2.4 西方墨點法 (western blot) 的原理與測定 12
2.4.1 蛋白質的萃取 13
2.4.2 蛋白質濃度的定量分析 13
2.4.3 蛋白質前處理 14
2.4.4 電泳膠片製作 14
2.4.5 樣品上樣與電泳 15
2.4.6 蛋白質轉印 15
2.4.7 封閉轉印膜 (blocking) 15
2.4.8 抗體反應與冷光顯影 16
2.5 流式細胞術測定細胞狀態 16
2.5.1 細胞內ROS檢測 16
2.5.2 細胞凋亡程度檢測 17
2.6 統計分析 (statistical analysis) 18
第三章 實驗結果與討論 19
3.1 AITC與TC-HT對PANC-1細胞生長影響 19
3.1.1 AITC與TC-HT對PANC-1細胞活性影響 19
3.1.2 AITC與TC-HT對PANC-1細胞株型態 (morphology) 影響 21
3.2 以流式細胞儀測定PANC-1細胞株狀態 21
3.2.1 AITC與TC-HT對於PANC-1細胞內的細胞凋亡之影響 21
3.2.2 AITC與TC-HT造成PANC-1細胞內的ROS水平提升 22
3.3 ERK / CREB路徑之活化程度在AITC與TC-HT聯合處理下的變化 24
3.3.1 磷酸化ERK蛋白水平在AITC與TC-HT聯合處理下的變化 24
3.3.2 p-CREB蛋白水平在AITC與TC-HT聯合處理下的變化 25
3.4 PANC-1細胞中的DNA保護機制在AITC與TC-HT聯合處理下的變化 26
3.4.1 MTH1蛋白水平在AITC與TC-HT聯合處理下的變化 26
3.5 AITC搭配TC-HT對PANC-1細胞影響的機制討論 27
第四章 總結 29
REFERENCE 31		-
dc.language.isozh_TW-
dc.subject異硫氰酸烯丙酯 (AITC)-
dc.subject熱刺激-
dc.subject胰臟癌-
dc.subject活性氧化物質 (Reactive oxygen species, ROS)-
dc.subject細胞凋亡-
dc.subjectallyl isothiocyanate-
dc.subjecthyperthermia-
dc.subjectpancreatic cancer-
dc.subjectReactive oxygen species (ROS)-
dc.subjectcell apoptosis-
dc.title循環加熱增強異硫氰酸烯丙酯AITC對人類胰臟癌細胞的抗癌作用zh_TW
dc.titleThermal Cycling Hyperthermia Enhances the Anticancer Effect of Allyl isothiocyanate on PANC-1 cellsen
dc.typeThesis-
dc.date.schoolyear114-1-
dc.description.degree碩士-
dc.contributor.oralexamcommittee温進德;呂世正zh_TW
dc.contributor.oralexamcommitteeJin-Der Wen;Shr-Jeng Leuen
dc.subject.keyword異硫氰酸烯丙酯 (AITC),熱刺激胰臟癌活性氧化物質 (Reactive oxygen species, ROS)細胞凋亡zh_TW
dc.subject.keywordallyl isothiocyanate,hyperthermiapancreatic cancerReactive oxygen species (ROS)cell apoptosisen
dc.relation.page37-
dc.identifier.doi10.6342/NTU202600644-
dc.rights.note未授權-
dc.date.accepted2026-02-08-
dc.contributor.author-college理學院-
dc.contributor.author-dept應用物理研究所-
dc.date.embargo-liftN/A-
顯示於系所單位:應用物理研究所

文件中的檔案:
檔案 大小格式 
ntu-114-1.pdf
  未授權公開取用 		1.37 MBAdobe PDF
顯示文件簡單紀錄


系統中的文件,除了特別指名其著作權條款之外,均受到著作權保護,並且保留所有的權利。

社群連結
聯絡資訊
10617臺北市大安區羅斯福路四段1號
No.1 Sec.4, Roosevelt Rd., Taipei, Taiwan, R.O.C. 106
Tel: (02)33662353
Email: ntuetds@ntu.edu.tw
意見箱
相關連結
館藏目錄
國內圖書館整合查詢 MetaCat
臺大學術典藏 NTU Scholars
臺大圖書館數位典藏館
本站聲明
© NTU Library All Rights Reserved