The Role of ATF3 in Prodigiosin-induced Apoptosis

碩士 === 國立中興大學 === 生物醫學研究所 === 98 === Prodigiosin (PG) has been identified as a new and potential anti-cancer drug in a variety of studies. However, the precise targets of PG-induced apoptosis are still uncovered, and therefore identification of the target is the main focus in this study. By analyzin...

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Main Authors: Yu-Ta Peng, 彭昱達
Other Authors: Chia-Che Chang
Format: Others
Language:zh-TW
Published: 2010
Online Access:http://ndltd.ncl.edu.tw/handle/44417388543847912917
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spelling ndltd-TW-098NCHU51140082016-12-25T04:10:42Z http://ndltd.ncl.edu.tw/handle/44417388543847912917 The Role of ATF3 in Prodigiosin-induced Apoptosis ATF3 在 Prodigiosin 誘發之細胞凋亡中所扮演的角色 Yu-Ta Peng 彭昱達 碩士 國立中興大學 生物醫學研究所 98 Prodigiosin (PG) has been identified as a new and potential anti-cancer drug in a variety of studies. However, the precise targets of PG-induced apoptosis are still uncovered, and therefore identification of the target is the main focus in this study. By analyzing data from microarray, we found activating transcription factor 3 (ATF3) showed an obvious difference in expression. The results from quantitative real-time RT-PCR analysis and immunoblot analysis on a number of different kinds of cancer cell lines indicated that ATF3 can be highly induced by PG. Further analysis revealed that PG can activate the human ATF3 promoter, and c-Jun N-terminal kinase (JNK) signaling pathway is involved in the up-regulation of ATF3 by PG. Additionally, PG treatment was shown to induce endoplasmic reticulum (ER) stress. Finally, PG-induced apoptosis was significantly reduced by silencing ATF3. Together, these data indicated that PG activates JNK signaling to up-regulates ATF3, which in turn contributes to the induction of apoptosis, partly through ER stress. In conclusion, ATF3 not only plays an important role in PG-induced apoptosis, but also acts a novel molecular taget of PG. Chia-Che Chang 張嘉哲 2010 學位論文 ; thesis 48 zh-TW
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description 碩士 === 國立中興大學 === 生物醫學研究所 === 98 === Prodigiosin (PG) has been identified as a new and potential anti-cancer drug in a variety of studies. However, the precise targets of PG-induced apoptosis are still uncovered, and therefore identification of the target is the main focus in this study. By analyzing data from microarray, we found activating transcription factor 3 (ATF3) showed an obvious difference in expression. The results from quantitative real-time RT-PCR analysis and immunoblot analysis on a number of different kinds of cancer cell lines indicated that ATF3 can be highly induced by PG. Further analysis revealed that PG can activate the human ATF3 promoter, and c-Jun N-terminal kinase (JNK) signaling pathway is involved in the up-regulation of ATF3 by PG. Additionally, PG treatment was shown to induce endoplasmic reticulum (ER) stress. Finally, PG-induced apoptosis was significantly reduced by silencing ATF3. Together, these data indicated that PG activates JNK signaling to up-regulates ATF3, which in turn contributes to the induction of apoptosis, partly through ER stress. In conclusion, ATF3 not only plays an important role in PG-induced apoptosis, but also acts a novel molecular taget of PG.
author2 Chia-Che Chang
author_facet Chia-Che Chang
Yu-Ta Peng
彭昱達
author Yu-Ta Peng
彭昱達
spellingShingle Yu-Ta Peng
彭昱達
The Role of ATF3 in Prodigiosin-induced Apoptosis
author_sort Yu-Ta Peng
title The Role of ATF3 in Prodigiosin-induced Apoptosis
title_short The Role of ATF3 in Prodigiosin-induced Apoptosis
title_full The Role of ATF3 in Prodigiosin-induced Apoptosis
title_fullStr The Role of ATF3 in Prodigiosin-induced Apoptosis
title_full_unstemmed The Role of ATF3 in Prodigiosin-induced Apoptosis
title_sort role of atf3 in prodigiosin-induced apoptosis
publishDate 2010
url http://ndltd.ncl.edu.tw/handle/44417388543847912917
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