斑馬魚顆粒蛋白前體調控肝臟再生之機制

Keng-Yu Chiang; 江耕宇

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/63542

完整後設資料紀錄

DC 欄位	值	語言
dc.contributor.advisor	吳金洌
dc.contributor.author	Keng-Yu Chiang	en
dc.contributor.author	江耕宇	zh_TW
dc.date.accessioned	2021-06-16T17:13:46Z	-
dc.date.available	2017-08-20
dc.date.copyright	2012-08-20
dc.date.issued	2012
dc.date.submitted	2012-08-20
dc.identifier.citation	Bell, A., Q. Chen, et al. (1999). 'The five amino acid-deleted isoform of hepatocyte growth factor promotes carcinogenesis in transgenic mice.' Oncogene 18(4): 887-895. Benvenuti, S. and P. M. Comoglio (2007). 'The MET receptor tyrosine kinase in invasion and metastasis.' J Cell Physiol 213(2): 316-325. Bohm, F., U. A. Kohler, et al. (2010). 'Regulation of liver regeneration by growth factors and cytokines.' EMBO Mol Med 2(8): 294-305. Borowiak, M., A. N. Garratt, et al. (2004). 'Met provides essential signals for liver regeneration.' Proc Natl Acad Sci U S A 101(29): 10608-10613. Cadieux, B., B. P. Chitramuthu, et al. (2005). 'The zebrafish progranulin gene family and antisense transcripts.' BMC Genomics 6: 156. Factor, V. M., D. Seo, et al. (2010). 'Loss of c-Met disrupts gene expression program required for G2/M progression during liver regeneration in mice.' PLoS One 5(9). Huh, C. G., V. M. Factor, et al. (2004). 'Hepatocyte growth factor/c-met signaling pathway is required for efficient liver regeneration and repair.' Proc Natl Acad Sci U S A 101(13): 4477-4482. Kinkel, M. D., S. C. Eames, et al. (2010). 'Intraperitoneal injection into adult zebrafish.' J Vis Exp(42). Li, Y. H., M. H. Chen, et al. (2010). 'Progranulin A-mediated MET signaling is essential for liver morphogenesis in zebrafish.' J Biol Chem 285(52): 41001-41009. Matsuo, T., S. Yamaguchi, et al. (2003). 'Control mechanism of the circadian clock for timing of cell division in vivo.' Science 302(5643): 255-259. Michalopoulos, G. K. (2007). 'Liver regeneration.' J Cell Physiol 213(2): 286-300. Morello, D., A. Lavenu, et al. (1990). 'Differential regulation and expression of jun, c-fos and c-myc proto-oncogenes during mouse liver regeneration and after inhibition of protein synthesis.' Oncogene 5(10): 1511-1519. Poss, K. D., M. T. Keating, et al. (2003). 'Tales of regeneration in zebrafish.' Dev Dyn 226(2): 202-210. Sadler, K. C., K. N. Krahn, et al. (2007). 'Liver growth in the embryo and during liver regeneration in zebrafish requires the cell cycle regulator, uhrf1.' Proc Natl Acad Sci U S A 104(5): 1570-1575. Schibler, U. (2003). 'Circadian rhythms. Liver regeneration clocks on.' Science 302(5643): 234-235. Shankaran, S. S., A. Capell, et al. (2008). 'Missense mutations in the progranulin gene linked to frontotemporal lobar degeneration with ubiquitin-immunoreactive inclusions reduce progranulin production and secretion.' J Biol Chem 283(3): 1744-1753. Stolz, D. B., W. M. Mars, et al. (1999). 'Growth factor signal transduction immediately after two-thirds partial hepatectomy in the rat.' Cancer Res 59(16): 3954-3960. Taub, R. (2004). 'Liver regeneration: from myth to mechanism.' Nat Rev Mol Cell Biol 5(10): 836-847. Weglarz, T. C. and E. P. Sandgren (2000). 'Timing of hepatocyte entry into DNA synthesis after partial hepatectomy is cell autonomous.' Proc Natl Acad Sci U S A 97(23): 12595-12600.
dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/63542	-
dc.description.abstract	肝臟的生長除了於胚胎發育階段，另可發生於肝臟受到損傷時所啟動的肝臟再生機制。本實驗室先前的研究指出，顆粒蛋白前體藉由調控肝細胞生長因子接受器訊息傳遞路徑進而影響肝細胞生長。顆粒蛋白前體為一種具有多功能性的分泌性醣蛋白，已知參與在細胞生長、傷口癒合、腫瘤形成、發炎反應、神經發育及在神經退化性疾病等方面並扮演重要的角色。本研究欲探究顆粒蛋白前體參與在肝臟再生中所扮演之角色，使顆粒蛋白前體在肝臟生長發育的調控功能更完整。我們選用斑馬魚建立肝臟再生的模式魚種，將肝臟專一性表現螢光的成魚進行部分肝切除手術，觀察顆粒蛋白前體是否會參與在肝臟再生中。利用定量聚合酶連鎖反應的結果顯示，在肝臟受到損傷後，此顆粒蛋白前體的訊息核糖核酸表現量及細胞週期、細胞增生相關基因群會伴隨肝臟再生的過程而被誘發表現。為了探究顆粒蛋白前體A 型在斑馬魚肝臟再生中的調控功能。我們分別利用基因功能失活及增益方法探究之。我們的實驗結果顯示，顆粒蛋白前體A 型失活的斑馬魚在部分的肝臟切除手術之後，肝臟表現出較弱的肝臟再生的恢復能力，造成此結果的原因是細胞週期相關的基因延遲的表現，且細胞增生相關的基因表現受到了抑制，這些受影響的基因表現在肝臟切除受術後三十六小時可明顯的觀察到。在另一方面，我們肝臟專一性增益表現顆粒蛋白前體A 型的斑馬魚，在部分的肝臟切除手術後，肝臟表現較快的肝臟再生的恢復能力。因此，我們推斷斑馬魚顆粒蛋白前體A 型藉由調控肝細胞生長因子接受器訊息傳遞路徑對肝臟再生是必須的。	zh_TW
dc.description.abstract	Physiologic liver growth not only occurs in embryonic development, but also in the liver regeneration process that was activated after liver injury. According to our previous research, it indicated that progranulin could modulate MET, the receptor of hepatocyte growth factor, signaling to regulate liver growth. Progranulin is a multifunctional secreted glycoprotein. It has been known that plays a critical role in cell growth, wound healing, tumorigenesis, inflammation response, neurodevelopment, and neurodegeneration. This research would study the regulatory role of progranulin that involve in liver regeneration. We established a liver regeneration model after partial hepatectomy in liver-specific fluorescent adult zebrafish. The result of quantitative-PCR showed that mRNA expression of progranulin, cell cyele and proliferation related genes were induced after partial hepatectomy. To study the functional progranulin A in liver regeneration. We use the loss of function and gain of function assay. In our grnA morphant showed a weak recovery with delayed cell cycle related gene and suppressed cell proliferation related gene that specifically at 36 hours after partial heapatectomy. On the other side, in our liver specific grnA over expression transgenic zebrafish showed a faster recovery than wild-type zebrafish after partial hepatectomy. In conclusion, grnA mediate met signaling is required for liver regeneration.	en
dc.description.provenance	Made available in DSpace on 2021-06-16T17:13:46Z (GMT). No. of bitstreams: 1 ntu-101-R99b45017-1.pdf: 1371256 bytes, checksum: e237c8333cd91fe0c37a0ef947455d0b (MD5) Previous issue date: 2012	en
dc.description.tableofcontents	口試論文審定書............................................................................................................. I 謝辭 ...............................................................................................................................II 摘要 .............................................................................................................................. III Abstract ....................................................................................................................... IV Table of Content............................................................................................................V List of Figures ............................................................................................................VII List of Tables ............................................................................................................... IX Chapter 1: Introduction................................................................................................1 1.1 The Mechanism of Liver Regeneration ......................................................... 1 1.2 Known Factors Involved in The Liver Regeneration ................................... 1 1.3 Zebrafish as a Disease and Developmental Animal Model .......................... 3 1.4 Progranulin is Essential For Hepatocyte Proliferation ................................ 4 Chapter 2: Material and Method .................................................................................6 2.1 Fish Strains ....................................................................................................... 6 2.2 Morpholino Design .......................................................................................... 6 2.3 Morpholino Intraperitoneal Injection into Adult Zebrafish ....................... 6 2.4 Partial Hepatectomy ........................................................................................ 7 2.5 Quantitative RT-PCR...................................................................................... 7 VI Chapter 3: Results ......................................................................................................... 9 3.1 Establishment of Liver Regeneration Model in Tg(fabp10:EGFP) Adult Zebrafish ..........................................................................................................9 3.2 The Gene Expression of Cell Cycle and Cell Proliferation Related Gene..9 3.3 grnA Morphant Shows the Delayed Recovery of Zebrafish Liver............10 3.4 grnA Morphant Decreases the Expression of Cell Cycle and Cell Proliferation Related Gene in Zebrafish Liver Regeneration ................... 11 3.5 grnA Morphant Modulate the Met Expression Involve in Delayed Zebrafish Liver Regeneration ...................................................................... 11 3.6 The Study of Functional Progranulin in Liver Regeneration with Gain-of-Function ...........................................................................................12 Chapter 4: Discussion..................................................................................................13 Reference ......................................................................................................................16
dc.language.iso	zh-TW
dc.subject	斑馬魚	zh_TW
dc.subject	顆粒蛋白前體	zh_TW
dc.subject	肝細胞生長因子接受器	zh_TW
dc.subject	部分肝臟切除手術	zh_TW
dc.subject	肝臟再生	zh_TW
dc.subject	Partial Hepatectomy	en
dc.subject	Zebrafish	en
dc.subject	Met	en
dc.subject	Progranulin	en
dc.subject	Liver Regeneration	en
dc.title	斑馬魚顆粒蛋白前體調控肝臟再生之機制	zh_TW
dc.title	Progranulin is Required for Liver Regeneration in The Partial Hepatectomized Zebrafish	en
dc.type	Thesis
dc.date.schoolyear	100-2
dc.description.degree	碩士
dc.contributor.oralexamcommittee	陳志毅,龔紘毅
dc.subject.keyword	斑馬魚,顆粒蛋白前體,肝細胞生長因子接受器,部分肝臟切除手術,肝臟再生,	zh_TW
dc.subject.keyword	Zebrafish,Progranulin,Met,Partial Hepatectomy,Liver Regeneration,	en
dc.relation.page	31
dc.rights.note	有償授權
dc.date.accepted	2012-08-20
dc.contributor.author-college	生命科學院	zh_TW
dc.contributor.author-dept	漁業科學研究所	zh_TW
顯示於系所單位：	漁業科學研究所

文件中的檔案：

檔案	大小	格式
ntu-101-1.pdf 未授權公開取用	1.34 MB	Adobe 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。