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請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/22804
完整後設資料紀錄
DC 欄位值語言
dc.contributor.advisor鄧哲明
dc.contributor.authorAn-Chi Tsaien
dc.contributor.author蔡岸圻zh_TW
dc.date.accessioned2021-06-08T04:28:50Z-
dc.date.copyright2010-03-12
dc.date.issued2010
dc.date.submitted2010-01-27
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dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/22804-
dc.description.abstract血管新生 (angiogenesis),是指由原來已存在的血管分化形成新血管之一個多重
且複雜的過程。一些疾病,如腫瘤、慢性發炎 (類風濕性關節炎)、糖尿病引起之視
網膜病變等與血管過度增生有關。因此,抑制血管新生可應用於各種因血管增生所
衍生的疾病。在本論文中,將探索具有研發潛力之抗血管新生藥物,並對其作用機
轉進行研究。
本論文的第一個部分主要在探討黃草石斛 (Dendrobrium loddigesii) 莖部萃取
物 moscatilin 對 VEGF 及 bFGF 所引起人類臍靜脈內皮細胞 (Human umbilical
vein endothelial cells;HUVECs) 的生長抑制作用及其可能作用的分子機轉。實驗發
現 moscatilin 能使人類臍靜脈內皮細胞生長產生抑制作用,且其抑制效果和
moscatilin 的濃度呈正相關性。Moscatilin 抑制血管新生是透過阻斷 VEGF 及
bFGF 所引起的 ERK1/2、Akt 和 eNOS 之活化。我們也進行了 in vivo matrigel plug
assay 和腫瘤的異體移植實驗,確認 moscatilin 在體內的抗血管新生效果。綜合以
上實驗證明 moscatilin 是個值得進一步研發的抗血管新生先導藥物。
本論文的第二個部分在探討大爪石斛 (Ephemerantha lonchophylla) 莖部萃取
物 denbinobin 對於第一型類胰島素生長因子 (insulin-like growth factor-1;IGF-1)
所引發血管新生的抑制作用。從體內動物實驗證實 denbinobin 能有效抑制腫瘤細胞
的生長並阻斷 IGF-1 誘發之血管新生作用。此外,denbinobin 也能抑制體外人類臍
靜脈內皮細胞的增生、移行及管柱形成作用。進一步實驗證實 denbinobin 能顯著地
抑制人類臍靜脈內皮細胞中,由 IGF-1 所引起的 IGF-1/IGF-1R 下游相關訊息傳遞
分子 ERK1/2、Akt、mTOR、p70S6K 和 cyclin D1 之活化。因此我們認為 denbinobin
是相當值得未來開發及應用於血管新生相關疾病,例如癌症,的治療上。
本論文的第三個部分在探討 2-phenyl-4 quinolone 類化合物 CHM-1 在體內及
體外模式抑制血管新生的作用機轉。在動物實驗中,CHM-1 可以有效抑制腫瘤的
生長與血管生成。體外試驗也發現 CHM-1 能抑制人類臍靜脈內皮細胞的生長、遷
2
移及管腔形成。進一步實驗證實 CHM-1 能抑制微管蛋白的聚合作用,並透過使細
胞內 p53 蛋白增加,提高 DR5 蛋白質的表現量,而誘發細胞外生性凋亡路徑
(extrinsic apoptotic pathway),最後造成人類臍靜脈內皮細胞的凋亡,達到破壞腫瘤
血管的效果。以上實驗證明 CHM-1 是個具有潛力的抗血管新生先導藥物。
綜合以上所述,本論文主要以抑制血管新生為標的,陸續證實石斛成分
moscatilin 和 denbinobin,以及化學小分子 CHM-1 能顯著地阻斷體外與體內之血
管新生作用,進而治療與血管新生相關的疾病,並發展為具療效之先導藥物。
zh_TW
dc.description.abstractAngiogenesis is a multiple and complex process involving the growth of new blood
vessels from pre-existing vessels. Various pathological conditions, including cancer,
chronic inflammation (e.g. rheumatoid arthritis) and diabetic retinopathy are related to
angiogenesis, thus inhibition of angiogenesis might have implication in various
angiogenesis-mediated disorders. In this thesis, we focused on the discovery of potential
novel antiangiogenic agents, and further investigated the mechanisms of these agents.
The first part is to investigate the anti-proliferation effect and molecular mechanisms
of moscatilin, a bibenzyl derivative from the stem of an India orchid Dendrobrium
loddigesii, on human umbilical vein endothelial cells (HUVECs). We found moscatilin
significantly inhibited HUVECs growth in a concentration-dependent manner. The
antiangiogenic effects of moscatilin are proposed to inhibition of ERK1/2, Akt, and
eNOS signaling pathways. In vivo Matrigel plug assay and tumor xenograft were also
performed to support the potential of moscatilin as an angiognenesis inhibitor for cancer
therapy. Moscatilin is a promising lead compound worthy of further development into a
drug candidate for anti-angiogenesis.
The second part is aimed to evaluate the roles of denbinobin, a phenanthraquinone
derivative present in the stems of Ephemerantha lonchophylla, in suppressing the
IGF-1-induced angiogenesis and elucidating the underlying molecular mechanisms.
Denbinobin inhibited tumor growth and IGF-1-induced angiogenesis in vivo.
Additionally, denbinobin also suppressed IGF-1-induced HUVECs proliferation,
migration and tube formation in vitro. We further found that denbinobin caused more
efficient inhibition of IGF-1-induced activation of IGF-1R and its downstream signaling
targets, including ERK, Akt, mTOR, p70S6K, 4EBP, and cyclin D1. Our findings
suggest that denbinobin could be a potential therapeutic agent against angiogenesisrelated
diseases, such as cancer.
The third part is to study the antiangiogenic activity and mechanism of CHM-1, a
2-phenyl-4 quinolone derivative, in vitro and in vivo. Results of animal models indicated
4
that CHM-1 inhibited tumor growth and induced vascular shutdown within tumor.
CHM-1 also suppressed the proliferation, migration and tube formation of HUVECs in
vitro. Besides, CHM-1 inhibited microtubule assembly as well as upregulated the
expression of p53, DR5. Then, apoptosis executed by an extrinsic apoptotic pathway.
Taken together, we suggest CHM-1 has potential to be an antivascular and antitumor
therapeutic lead compound.
In conclusion, the aim of this study is to examine the anti-angiogenetic effects of
moscatilin, denbinobin and CHM-1. We found that these agents can inhibit angiogenesis
in vitro and in vivo. We suggest that moscatilin, denbinobin and CHM-1 have potential to
be a lead compound for treating angiogenesis-dependent diseases such as cancer.
en
dc.description.provenanceMade available in DSpace on 2021-06-08T04:28:50Z (GMT). No. of bitstreams: 1
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Previous issue date: 2010
en
dc.description.tableofcontents目錄
縮寫表················································································································· i
中文摘要············································································································· 1
英文摘要············································································································· 3
第一章
第一節 研究動機與目的············································································ 5
第二節 文獻回顧························································································ 7
第二章 實驗材料與方法···················································································· 37
第一節 實驗材料························································································ 37
第二節 實驗方法························································································ 39
第三章 Moscatilin 於體內及體外抑制腫瘤之血管新生及生長
中文摘要······································································································ 50
英文摘要······································································································ 51
第一節 緒言································································································ 52
第二節 材料與方法···················································································· 53
第三節 結果································································································ 54
第四節 討論································································································ 57
第四章 Denbinobin 經由阻斷第一型類胰島素生長因子接受體之訊息傳遞而抑制血
管新生及腫瘤生長
中文摘要······································································································ 70
英文摘要······································································································ 71
第一節 緒言································································································ 72
第二節 材料與方法···················································································· 73
第三節 結果································································································ 74
第四節 討論································································································ 77
第五章 CHM-1 透過調控 p53/DR5 途徑而引起人類臍靜脈內皮細胞的凋亡作用
中文摘要······································································································ 92
英文摘要······································································································ 93
第一節 緒言································································································ 94
第二節 材料與方法···················································································· 95
第三節 結果································································································ 96
第四節 討論································································································ 101
總結與展望········································································································· 115
參考文獻············································································································· 118
著作····················································································································· 129
dc.language.isozh-TW
dc.subject血管新生zh_TW
dc.subject癌症zh_TW
dc.subjectangiogenesisen
dc.subjectcanceren
dc.title抗癌藥物 Moscatilin, Denbinobin 與 CHM-1對於血管新生抑制作用機轉之探討zh_TW
dc.titleInvestigation of Anti-angiogenic Mechanism of
Moscatilin, Denbinobin and CHM-1
en
dc.typeThesis
dc.date.schoolyear98-1
dc.description.degree博士
dc.contributor.oralexamcommittee黃德富,楊春茂,顏茂雄,林建煌,顧記華
dc.subject.keyword癌症,血管新生,zh_TW
dc.subject.keywordcancer,angiogenesis,en
dc.relation.page129
dc.rights.note未授權
dc.date.accepted2010-01-27
dc.contributor.author-college醫學院zh_TW
dc.contributor.author-dept藥理學研究所zh_TW
顯示於系所單位:藥理學科所

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