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  1. NTU Theses and Dissertations Repository
  2. 醫學院
  3. 法醫學科所
請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/54573
完整後設資料紀錄
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dc.contributor.advisor翁德怡(Te-I Weng)
dc.contributor.authorChia-Lien Chiangen
dc.contributor.author江佳蓮zh_TW
dc.date.accessioned2021-06-16T03:05:14Z-
dc.date.available2015-09-25
dc.date.copyright2015-09-25
dc.date.issued2015
dc.date.submitted2015-06-29
dc.identifier.citation1. 台灣南投地方法院。100年度。臺灣南投地方法院刑事判決[重訴字,第6號]。
2. 行政院勞工委員會。2000。行政院勞工委員會採樣分析建議方法,CLA1007,2-氯乙醇。
3. 行政院環境保護署。94年5月。危害性化學物質災害緊急處理手冊。
4. 行政院環境保護署環境檢驗所(NIEA)。99年。水中鹵乙酸與得拉本檢測方法—液相-液相微萃取/氣相層析儀/電子捕捉偵測器法。NIEA W538.51B:中華民國99年11月16日環署檢字第0990103569號公告。
5. 林嘉興。1988。葡萄休眠與催芽技術。葡萄生產技術特刊14:189-196。
6. 詹雅玲。95年。以固相微萃取建立水中三鹵甲烷及鹵乙酸之同步分析方法,中國醫藥大學碩士論文。
7. Armbruster, D. A., M. D. Tillman, L. M. Hubbs, 1994. Limit of detection (LQD)/limit of quantitation (LOQ): comparison of the empirical and the statistical methods exemplified with GC-MS assays of abused drugs. Clin Chem.40(7 Pt 1): 1233-1238.
8. Salih, B. and Ö Çelikbıçak, 2012. Gas Chromatography in plant science, wine technology, toxicology and some specific applications. InTech, chapter 10.
9. Cardador M. J. and M. Gallego, 2012. Development of a method for the quantitation of chloro-, bromo-, and iodoacetic acids in alcoholic beverages.
J Agric Food Chem. 60(3):725-730.
10. Cardador M. J., A. Serrano and M. Gallego, 2008. Simultaneous liquid-liquid microextraction/methylation for the determination of haloacetic acids in drinking waters by headspace gas chromatography. J Chromatogr A.1209(1-2):61-69.
11. Chen Y. T., J. W. Liao and D. Z. Hung, 2010. Protective effects of fomepizole on 2-chloroethanol toxicity. Hum Exp Toxicol. 29(6):507-512.
12. CLSI, 2007. Mass spectrometry in the clinical laboratory: general principles and guidance. CLSI document C50-A. 27(24).
13. Deng J. F., C. C. Yang, W. J. Tsai, J. Ger and ML Wu, 2001. Acute ethylene chlorohydrin poisoning: experience of a poison control center. J Toxicol Clin Toxicol. 39(6):587-593.
14. Deutsche Forschungsgemeinschaft , 2012. 2-Chloroehanol. The MAK Collection for Occupational Health and Safety. Wiley-VCH. (5):65-73.
http://onlinelibrary.wiley.com/doi/10.1002/3527600418.mb10707e0005/pdf
15. Dierker H . and P. G. Brown, 1944. Study of a fatal case of ethylene chlorohydrin poisoning. J Ind Hyg Toxicol. 26:277-279.
16. Tateo F. and M. Bononi, 2006. Determination of ethylene chlorohydrin as marker of spices fumigation with ethylene oxide. J Food Compost Anal. 19:83-87.
17. Ferrari L. A., J. M. Triszcz and L. Giannuzzi, 2006. Kinetics of ethanol degradation in forensic blood samples. Forensic Sci Int. 161(2-3):144-150.
18. George S. E., G. M. Nelson, A. E. Swank, L. R. Brooks, K. Bailey, M. George and A. DeAngelo, 2000. The disinfection by-products dichloro-, dibromo-, and bromochloroacetic acid impact intestinal microflora and metabolism in Fischer 344 rats upon exposure in drinking water. Toxicol Sci. 56(2):282-289.
19. Goldblatt M. W.and W. E. Chiesman, 1944. Toxic Effects of Ethylene Chlorohydrin. Br J Ind Med. 1(4):207-223.
20. Kato J, T Dote, H Shimizu, Y Shimbo, M Fujihara and K Kono, 2006. Lethal acute lung injury and hypoglycemia after subcutaneous administration of monochloroacetic acid. Toxicol Ind Health .22(5):203-209.
21. Kolb B. and L. S. Ettre, 2005. Static headspace-gas chromatography: theory and pratice, 2nd ED, Wiley.
22. Johnson M. K., 1975. Letter: Ethylene chlorohydrin intoxication. Arch Dis Child. 50(3):250.
23. NCCLS, 2002. Gas Chromatography/Mass Spectrometry (GC/MS) confirmation of durgs; approved guideline. NCCLS document C43-A. 22(22).
24. Needleman S. B. and R. W. Romberg, 1990. Limits of linearity and detection for some drugs of abuse. J Anal Toxicol. 14(1):34-38.
25. NIOSH, 1994. NIOSH Manual of analytical methods, 1th ed. Method 2513.
26. Sakai A, H Shimizu, K Kono and E Furuya, 2005. Monochloroacetic acid inhibits liver gluconeogenesis by inactivating glyceraldehyde-3-phosphate dehydrogenase. Chem Res Toxicol. 18(2):277-282.
27. Sigma-Aldrich, 2012. MSDS of 2-chloroethanol
http://www.sigmaaldrich.com/MSDS/MSDS/DisplayMSDSPage.do?country=TW&language=en&productNumber=48085&brand=SUPELCO&PageToGoToURL=http%3A%2F%2Fwww.sigmaaldrich.com%2Fcatalog%2Fsearch%3Fterm%3D2-chloroethanol%26interface%3DAll%26N%3D0%26mode%3Dmatch%2520partialmax%26lang%3Den%26region%3DTW%26focus%3Dproduct
28. U.S.EPA, 2006. Volatile organic compounds by gas chromatography/mass spectrometry (GC/MS). US Environmental Protection Agency Method 8260C, revision 3.
29. U.S.EPA, 2003. Determination of Haloacetic Acid and Dalapon in Drinking Water by Liquid-Lquid Microextraction, Derivatization, and Gas Chromatography with Electron Capture Detector. Method 552.3.
30. Urbansky ET, 2000. Techniques and methods for the determination of haloacetic acids in potable water. J Environ Monit. 2(4):285-291.
31. Van Rillaer W. G. and H. Beenaert, 1982. Determination of residual ethylene chlorohydrin (ECH) in fumigated foodstuffs by glass capillary gas chromatography. Z Lebensm Unters Forsch. 175:175-178.
32. Wasfi I. A., A. H. Al-Awadhi, Z. N. Al-Hatali, F. J. Al-Rayami and N. A. Al Katheeri, 2004. Rapid and sensitive static headspace gas chromatography-mass spectrometry method for the analysis of ethanol and abused inhalants in blood. J Chromatogr B Analyt Technol Biomed Life Sci. 799(2):331-336.
dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/54573-
dc.description.abstract2-氯乙醇(CAS 107-07-3)是台灣農民常用於葡萄催芽之用的試劑,雖因毒性強烈被禁用,但因比49 %氰滿素效果較佳且費用便宜,還是常被農民非法使用,因此常有誤食或工作接觸造成意外中毒的事件。民國100年南投縣發生因感情糾紛而使用2-氯乙醇毒殺,造成4人死亡的謀殺案件,從屍體中檢測出2-氯乙醇成為重要的法庭證據。
因2-氯乙醇並非一般常規篩檢毒物,目前並沒有標準方法可以檢測血中濃度,因此我們使用HS-GC/MS系統並以1-pentanol為內標準品建立全血中2-氯乙醇的檢測方法,此方法利用選擇性離子方法以定量(m/z 31)與定性離子(m/z 49, 80)測得2-氯乙醇之偵測極限為1 μg/mL,定量極限為5 μg/mL,靈敏度佳且線性關係良好(在5-200 μg/mL之間可得r2=0.999)、易於操作。
為得知其穩定度,以EDTA抗凝固劑管採取10位自願者血液,將血液檢體每組配製10 μg/mL與100 μg/mL二種濃度,分二組分別置於室溫及4℃二種不同儲存溫度的環境下儲存,觀察不同時間點對於2-氯乙醇穩定度之影響。結果顯示10 μg/mL濃度2-氯乙醇於血液檢體中從第0週到第12週不論是儲存於4℃或室溫條件下都沒有明顯下降趨勢,4℃平均為10.6 μg/mL (SD 0.86),室溫平均為10.5 μg/mL (SD 0.62);100 μg/mL濃度2-氯乙醇血液檢體則是在4℃儲存條件下沒有明顯下降(平均93.6 μg/mL,SD 5.37),但儲存於室溫的檢體從第0週到第6週都還保持穩定,但第9週起就降低到78.3 μg/mL,第12週則為83.4 μg/mL。
2-氯乙醇的代謝途徑為經酒精脫氫酶氧化成為氯乙醛後,再經乙醛脫氫酶代謝為氯乙酸。為證實2-氯乙醇中毒,除2-氯乙醇外尚須檢驗其代謝物氯乙酸的濃度,參考檢測水質中氯乙酸方法,同時考慮時間與操作簡易性,挑選以液相-液相微萃取法/甲基化,在室溫下震盪三分鐘即可萃取氯乙酸,同時將氯乙酸衍生為甲基化酯類以HS-GC/MS偵測,並同時偵測2-氯乙醇。於本實驗方法中可同時於水中驗出這二種物質,但血液檢體,還有其LOD、LOQ、衍化率等均需再進一步評估。
zh_TW
dc.description.abstract2-chloroethanol (2-CE, ethylene chlorohydrin, CAS 107-07-3) is a chemical once widely used in hastening grape vine sprouting among Taiwanese farmers. Due to its severe toxicity upon acute exposure, such use of 2-CE is now prohibited in Taiwan. However, because of its superior potency and cheaper price compared to 49% cyanamide, 2-CE is still being illegally used by some farmers, so cases of poisoning due to accidental ingestions or occupational exposures were reported from time to time. In 2011, a man murdered his ex-girlfriend with 2-CE due to an emotional entanglement in Nantou County; four persons died in this case, and the detection of 2-CE from the corpses was an important forensic evidence.
To date, there are no standardized methods for the detection and quantification of 2-CE in human blood, because it is not a routinely-screened toxin. We developed a sensitive and specific method by employing static headspace gas chromatography with mass spectrometry (HS-GC/MS) for the quantitative determination of 2-CE in whole blood sample using 1-pentanol as internal standard. It was performed using selected ion monitoring (SIM) with quantitative ion (m/z 31) and qualitative ion (m/z 49, 80). We found that the method produced results with good linearity (r2=0.999, in the concentration range of 5-200 μg/mL), is sensitive (with the limit of detection and the limit of quantitation as 1 μg/mL and 5 μg/mL, respectively), and is easy to operate.
To evaluate the stability of 2-CE, whole human blood samples were taken from 10 volunteers (with EDTA added as anticoagulant), and two different concentrations of 2-CE solutions (10 μg/mL and 100 μg/mL) were prepared from each sample. They were further divided into two groups, with one group stored at 4℃ and another stored at room temperature until analyzed in triplicate by headspace gas chromatography-mass spectrometry (HS-GC/MS). After twelve weeks, the result showed that there were no significant alterations in the concentrations of the 10 μg/mL 2-CE solutions, whether stored at 4℃ (average 10.6 μg/mL with SD 0.86) or room temperature (average 10.5 μg/mL with SD 0.62). In the 100 μg/mL 2-CE solutions, no significant alterations of the concentrations were noticed when stored at 4℃ (average 93.6 μg/mL with SD 5.37); however, when stored at room temperature, it decreased significantly to 78.3 μg/mL in the 9th week and to 83.4 μg/mL in the 12th week.
2-chloroethanol has been assumed to be metabolized to chloroacetaldehyde (CAA) via alcohol dehydrogenase, and then to chloroacetae (CA) by aldehyde dehydrogenase. Both 2-CE and its metabolites should be detected in order to prove that it’s indeed 2-CE poisoning. Looking to the method of determining CA concentration in water for inspiration, we developed a simple and quick way that combines simultaneous liquid-liquid microextraction/methylation and HS-GC/MS for quantification of CA and 2-CE concentrations. Methylation and derivatization were completed in 3 minutes by shaking at room temperature. The methyl ester derivatives and the organic phase were completely volatilized by static headspace technique, and then analyzed by GC/MS. It seems that the concentrations of CA and 2-CE could be simultaneously determined in water, but further evaluations of LOD, LOQ, linearity and yield rate of the method in blood samples are still needed.
en
dc.description.provenanceMade available in DSpace on 2021-06-16T03:05:14Z (GMT). No. of bitstreams: 1
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Previous issue date: 2015
en
dc.description.tableofcontents口試委員會審定書 i
目 錄 ii
圖 目 錄 iii
表 目 錄 iv
誌謝 v
中文摘要 vi
English Summary vii
第一章 緒論 1
1.1. 題目定義 1
1.2. 研究動機 1
1.3. 文獻綜覽 4
1.3.1. 2-氯乙醇 4
1.3.2. 代謝物氯乙酸 7
第二章 材料與方法 9
2.1. 實驗材料 9
2.2. 實驗儀器設備 10
2.3. 2-氯乙醇實驗方法 10
2.4. 氯乙酸與2-氯乙醇同步分析之實驗方法 11
第三章 2-氯乙醇實驗結果 14
3.1. 實驗條件設定 14
3.2. 實驗確效 21
3.3. 檢體分析 34
3.3.1. 儲存於4℃之2-氯乙醇穩定度測試 34
3.3.2. 儲存於室溫之2-氯乙醇穩定度測試 34
第四章 氯乙酸實驗結果 42
第五章 討論 48
5.1. 2-氯乙醇方法建立 48
5.2. 2-氯乙醇穩定性 51
5.3. 同步偵測2-氯乙醇與其代謝物氯乙酸的可行性 52
參考文獻 53
dc.language.isozh-TW
dc.subject氯乙酸zh_TW
dc.subject人類全血zh_TW
dc.subject穩定度zh_TW
dc.subject2-氯乙醇zh_TW
dc.subject氣相層析質譜儀zh_TW
dc.subject氯乙酸zh_TW
dc.subject人類全血zh_TW
dc.subject穩定度zh_TW
dc.subject2-氯乙醇zh_TW
dc.subject氣相層析質譜儀zh_TW
dc.subjectHS-GC/MSen
dc.subject2-chloroethanolen
dc.subjectstabilityen
dc.subjecthuman whole blooden
dc.subjectchloroacetic aciden
dc.subjectHS-GC/MSen
dc.subject2-chloroethanolen
dc.subjectstabilityen
dc.subjecthuman whole blooden
dc.subjectchloroacetic aciden
dc.title2-氯乙醇於全血中的穩定度測試zh_TW
dc.titleThe Stability of 2-Chloroethanol in whole blooden
dc.typeThesis
dc.date.schoolyear103-2
dc.description.degree碩士
dc.contributor.oralexamcommittee彭福佐,洪東榮
dc.subject.keyword氣相層析質譜儀,2-氯乙醇,穩定度,人類全血,氯乙酸,zh_TW
dc.subject.keywordHS-GC/MS,2-chloroethanol,stability,human whole blood,chloroacetic acid,en
dc.relation.page55
dc.rights.note有償授權
dc.date.accepted2015-06-29
dc.contributor.author-college醫學院zh_TW
dc.contributor.author-dept法醫學研究所zh_TW
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