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請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/76099
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dc.contributor.authorHsiao Yu-Meien
dc.contributor.author蕭玉玫zh_TW
dc.date.accessioned2021-07-01T08:18:03Z-
dc.date.available2021-07-01T08:18:03Z-
dc.date.issued1995
dc.identifier.citationAiken, S. P., McArdle, J. J., Sellin, L. C. Schmidt, J. J. & Weinstein, S. A. (1991). Pre-and post-synaptic effects of a peptide toxin from Trimeresurus wagleri at the rat neuromuscular junction. Pharmacologist 33:186.
Aiken, S. P., Sellin, L. C., Schmidt, J. J., Weinstein, S. A. & McArdle, J. J. (1992). A novel peptide toxin from Trimeresurus wagleri acts pre-and post-synaptically to block transmission at the rat neuromuscular junction. Pharmacology & Toxicology 70: 459.
Applied Biosystems: Introduction to Cleavage Techniques.(1990).
Applied Biosystems: Model 431A User’s Manual. (1992). Version 2.00
Biosym Technologies: Homology User Guide. (1993). Version 2.1
Ellman, G. L. (1958). A colorimetric method for determing low concentrations of mercaptans. Arch. Biochem. Biophys.74:443.
Ellman, G. L. (1959). Tissue sulfhydryl groups. Arch. Biochem. Biophys. 82:70.
Hsieh, W. H., Tsai, M. C., Lee C. Y. & Smith, L. A. (1994). Effects of Waglerin-1, a toxin from Trimeresurus wagleri on the neuromuscular transmission of mouse nerve -muscle pre-parations. Toxicon 32:532.
Lee, C. Y. (1972). Chemistry and pharmacology of polypeptide toxins in snake venoms. Ann. Rev. Pharmacol. 12:265.
Lee, C. Y., Lin, W. W. & Smith, L. A. (1994). A study on the cause of death due to Waglerin-1, a toxin from Trimeresurus wagleri. Toxicon 32:526.
Litchfield, J. T. and Wilcoxon, F. J. (1949). Pharmacol. Exp. Ther. 96:99.
Minton, S. A. (1968). Preliminary observation on the venom of Wagler’s pit viper(Trimeresurus wagleri) Toxicon 6:93.
Schmidt, J. J., Weinstein S. A. & Smith L. A. (1992). Molecular properties and structure-function relationships of lethal peptides from venom of Wagler’s pit viper, Trimeresurus wagleri. Toxicon 30:1027.
Sine, S. M. (1993). Molecular dissection of subunit interfaces in the acetylcholine receptor: Identification of residues that determine curare selectivity. Proc. Natl. Acad. Sci. USA 90:9436.
Smith, M. A. and Hindle, E. (1931). Experiments with the venom of Laticauda, Pseudechis, and Trimeresurus wagleri species. Trans. R. Soc. Trop. Med. Hyg. 25:115.
Tan, N. H. and Tan, C. S. (1989). The enzymatic activities and lethal toxins of Trimeresurus wagleri (Speckled pit viper) venom. Toxicon 27:349.
Weinstein, S. A., Schmidt, J. J., Bernheimer, A. W. and Smith, L. A. (1991). Characterization and amino acid sequences of two lethal peptides isolated from venom of Wagler’s pit viper, Trimeresurus wagleri. Toxicon 29:227.
Williamson M. P. (1994). The structure and function of proline-rich regions in proteins. Biochem. J.297:249.
dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/76099-
dc.description.abstractTrimeresurus wagleri又被稱為斑紋蝮蛇(Speckled pit viper),普遍分佈在東南亞一帶地區,Waglerin-1是牠毒液裡的毒素之-,係由22個氨基酸所組成,其氨基酸序列為:
5 10 15 20
GGKPDLRPCHPPCHYIPRPKPR
其中有一個雙硫鍵。為瞭解其構造與生物活性之間的關係,首先以化學方法合成7個Waglerin-1的類似物來加以探討。
經由固相勝?自動合成儀逐步合成後,所得產物以切除試劑(cleavage reagent)除去所有保護基及樹脂(resin),置於鹼性的醋酸銨(NH4OAc)溶液中(0.05 mg/ml),以逆相高效率液相色層分析法追蹤及分離氧化態的Waglerin-1類似物。
這7個Waglerin-1類似物經氨基酸組成分析及質譜分析無誤後,做生物活性的測定及圓二極光譜分析,參考分子模擬的結果,發現影響這些類似物的毒性之主因可能在於其殘基電荷和/或其側鏈交互作用的被改變。此外,Waglerin-1致毒的活性區域(active site)極有可能就落在分子內雙硫鍵所約束形成的環形區域(loop)內,有待將來合成更多不同的類似物來做進一步的探討。
zh_TW
dc.description.abstractTrimeresurus wagleri. also known as the speckled pit viper, is abundant in south-eastern Asia. Waglerin-1 is one of the two main lethal components of T wagleri venom. The primary sequence of Waglerin-1 has been determined as followed:
5 10 15 20
GGKPDLPPCHPPCHYI PRPKPR
There is an intramolecular disulfide bond within it. In order to understand the relationship between the structure and biological activity of Waglerin-1, a series of Waglerin-1 analogs replaced of the basic residues with Ala were synthesized by the method of automated solid-phase peptide synthesis and air-oxidation. After purification by HPLC, the synthetic Waglerin-1 analogs were characterized by amino acid analysis, ion-electrospray mass spectroscopy, bioassay, and circular dichroism in comparison with synthetic Waglerin-1. Refer to the results of molecular modeling, it suggests that the effect of the replaced charged residues of His-10 and His-14 to the toxicity of Waglerin-1 were most important. In addition, the active Site of Waglerin -1 is probably located in the loop region confined by the intramolecular disulfide bond. In the future, more Wagerin-1 analogs replaced in loop region can be synthesized for advanced study.
en
dc.description.provenanceMade available in DSpace on 2021-07-01T08:18:03Z (GMT). No. of bitstreams: 0
Previous issue date: 1995
en
dc.description.tableofcontents謝誌…………………………………………………………………………i
目錄…………………………………………………………………………iii
表次………………………………………………………………………v
圖次………………………………………………………………………vi
縮寫字表……………………………………………………………………ix
中文摘要…………………………………………………………………xi
英文摘要……………………………………………………………………xiii
一、緒言……………………………………………………………………1
二、儀器與藥品……………………………………………………………7
(一)儀器…………………………………………………………………7
(二)藥品………………………………………………………………11
三、方法………………………………………………………………13
(一) Waglerin-1 類似物的合成…………………………………13
1.固相勝?自動合成法………………………………………………13
2.從HMP resin切下合成完畢的勝?………………………………14
(二)合成的Waglerin-1類似物之純化…………………………16
(三)合成的Waglerin-1類似物之鑑定…………………………18
(四)生物活性(毒性)的測定…………………………………………19
(五)圓二極光譜的測定…………………………………………………21
(六)分子模擬……………………………………………………………22
四、結果與討論……………………………………………………………25
(一) Waglerin-1類似物的合成…………………………………25
(二)合成的Waglerin-1類似物之純化與鑑定…………………27
(三)生物活性一致死劑量的測定……28
(四)圓二極光譜的測定………………31
(五)分子模擬………………………33
五、結論………………………………34
六、參考文獻…………………………36
七、附表………………………………40
八、附圖………………………………43
九、附錄………………77
dc.language.isozh-TW
dc.titleWaglerin-1 類似物之合成、生物活性及結構zh_TW
dc.titleSynthesis,Biological Activity,and Structural Analysis of Waglerin-1 Analogsen
dc.date.schoolyear83-2
dc.description.degree碩士
dc.relation.page83
dc.rights.note未授權
dc.contributor.author-dept生命科學院zh_TW
dc.contributor.author-dept生化科學研究所zh_TW
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