異位性皮膚炎聚角蛋白微絲基因之新生兒篩檢與遺傳諮詢

Yu-Hui Wu; 吳昱慧

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/77004

完整後設資料紀錄

DC 欄位	值	語言
dc.contributor.advisor	林芯予(Shin-Yu Lin)
dc.contributor.author	Yu-Hui Wu	en
dc.contributor.author	吳昱慧	zh_TW
dc.date.accessioned	2021-07-10T21:43:04Z	-
dc.date.available	2021-07-10T21:43:04Z	-
dc.date.copyright	2020-09-10
dc.date.issued	2020
dc.date.submitted	2020-07-30
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dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/77004	-
dc.description.abstract	異位性皮膚炎（Atopic Dermatitis, AD）依過往文獻統計，全球總體盛行率約9.6%-20%，根據台灣健保資料庫（NHI）2000年至2007年的統計，國人盛行率約6.7%。造成此疾病的最大原因，據以往研究顯示有約70%-85%為聚角蛋白微絲基因（Filaggrin gene, FLG gene）變異所引起，此基因變異會導致皮膚屏障（Skin barrier）功能缺損，保濕能力下降，進一步引發過敏原侵入，使得免疫功能失調，造成異位性皮膚炎發生。現行檢測與病程發展，是患者臨床症狀嚴重進而尋求專業醫師協助，後續透過臨床診斷並給予治療與用藥；如能在疾病誘發前進行基因檢測，並在衛教諮詢與專業醫師協助下提早預防勝於治療，本次研究將透過追蹤統計進一步探討，諮詢衛教的介入降低異位性皮膚炎被誘發的可能性；並藉此統計台灣盛行率建立資料庫與高低風險族群比例，基因型與臨床症狀的關聯性，並透過基因找出台灣族群的常見點位。本次研究依據過去國內外文獻所提及之FLG基因突變點位，從中挑選20個突變點位進行實驗，收案時間2015年至2020年03月份共8,076個新生兒；透過研究結果顯示，台灣異位性皮膚炎新生兒患者有65.8%為FLG基因異常，而台灣族群的盛行率為39.3%，透過檢測得知前三名常見點位分別是c.1432C>T/c.1432C>T佔79.4%、c.12064A>T佔9.7%、以及c.3321delA佔6.6%，後續透過衛教諮詢的介入之下，降低63.3%新生兒成為異位性皮膚炎患者。此研究得知，透過基因檢測、臨床診斷、衛教諮詢，可降低異位性皮膚炎發病率，也讓未來高風險族群之新生兒把傷害降到最低。	zh_TW
dc.description.abstract	According to the statistics from previous studies, the global prevalence of atopic dermatitis (AD) is around 9.6% to 20%. The statistics drawn from Taiwan’s National Health Insurance (NHI) Database revealed that the prevalence of AD in Taiwan was 6.7% from 2000 to 2007. With regard to the primary cause of the disease, previous studies have demonstrated that 70% to 85% of cases are caused by mutations of the filaggrin (FLG) gene. Such mutations result in skin barrier dysfunction and reduced water-holding capacity, thereby exposing the skin to allergens and causing immunity system disorders and AD. With respect to the testing and course of AD, current standards call for patients with serious clinical symptoms to seek professional assistance from physicians and receive treatment and medications based on their clinical diagnosis results. AD can be prevented if genetic testing is performed before the onset of the disease and assistance is provided through health consultations and physician visits. This study aimed to explore the possibility of reducing the likelihood of the onset of AD by tracking the statistics of AD and implementing health consultation interventions. In so doing, the statistical data can be used to establish a database covering the prevalence of AD in Taiwan and the percentage of high-risk groups, uncover the association between genotypes and clinical symptoms, and determine the common points of mutations among ethnic groups in Taiwan. 20 points of FLG mutations reported in local and overseas studies were selected for the experiments performed in this study. The participants were 8,076 neonates enrolled from 2015 to March 2020. The results demonstrated that 65.8% of the neonates in Taiwan had FLG gene abnormalities, while the prevalence of AD in Taiwan was 39.3%. The test results showed that the three most common points of mutation were c.1432C>T/c.1432C>T (which accounted for 79.4%), c.12064A>T (9.7%), and c.3321delA (6.6%). By means of subsequent health consultation interventions, AD was reduced among 63.3% of the neonates. Based on the results of this study, genetic testing, clinical diagnosis, and health consultation are effective means for reducing the incidence of atopic dermatitis and for minimizing injuries among high-risk neonates.	en
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dc.description.tableofcontents	口試委員審定書………………………………………………………………………..i 致謝…………………………………………………………………………………….ii 中文摘要………………………………………………………………………………iii 英文摘要..……………………………………………………………………………..iv 目錄..…………………………………………………………………………………..vi 第一章、緒論…………………………………………………………………………...1 1.1前言……………….………………………………………………………………...1 1.2瞭解異位性皮膚炎…….…………………………………………………………...1 1.2.1患者臨床4大主要症狀………………………………………………………..1 1.3臨床診斷標準……….……………………………………………………………...3 1.4嚴重程度分級-用藥與治療……………..………………………………………….3 1.5全球流行病學………………….…………………………………………………...4 1.6社會與經濟影響……….…………………………………………………………...6 1.7皮膚功能與基因作用機制…….…………………………………………………...7 1.8聚角蛋白微絲基因……………………….…………………………………….…..8 1.9突變點位檢測………………………………………………………………………9 1.10建立革新全面防護…….………………………………………………………….9 1.11研究動機與目的……….………………………………………………………...10 第二章、研究方法與材料……………………………………………………..……..11 2.1研究對象……….………………………………………………………………….11 2.2研究方法…….………………………………………………………………….…11 2.2.1檢體類別……….………………………………………………………….….11 2.2.1.1血液……….………………………………………………………….……11 2.2.1.2臍帶血…….……………………………………………………………….11 2.2.1.3口腔黏膜細胞….………………………………………………………….11 2.2.1.4血片……………….……………………………………………………….11 2.2.2 DNA萃取…………………………………………………………………….11 2.2.2.1TANBead………….………………………………………………………..11 2.2.2.2Qiagen….…………………………………………………………………..13 2.2.3引子對設計……………………………………………………….…………..14 2.2.4聚合酶鏈鎖反應實驗….……………………………………………………..14 2.2.5膠體電泳……………….……………………………………………………..15 2.2.6 PCR產物純化-管式純化…………………………………………………….16 2.2.7核酸定序分析………………………………………………………………...17 2.3統計研究…………………………………………………………………………..17 2.3.1第一個統計研究設計…………….…………………………………………..17 2.3.1.1設計目的性………………………………………………………………..17 2.3.2第二個統計研究設計…………………….…………………………………..17 2.3.2.1設計目的性…………….………………………………………………….18 2.3.3第三個統計研究設計…….…………………………………………………..18 2.3.3.1設計目的性……….……………………………………………………….18 第三章、結果…………………………………………………………………………19 3.1第一個研究統計.………………………………………………………………….19 3.1.1統計目的………………………………………………………………..…… 19 3.1.2異位性皮膚炎新生兒-FLG基因檢測統計結果……………………….……19 3.1.3異位性皮膚炎新生兒-FLG基因突變點位分佈……………………….……19 3.2第二個研究統計……………………………………………………………….….20 3.2.1統計目的……………………………………………………………….……..20 3.2.2一般新生兒-總年度收件量統計與地區統計趨勢……………………….….20 3.2.3一般新生兒-FLG基因高風險盛行率及地區分佈……………………….….20 3.2.4一般新生兒-FLG基因突變點位分佈趨勢………….………………….…....21 3.3第三個研究統計…………………………………………………………………..22 3.3.1統計目的…………………………………………………………….………..22 3.3.2 FLG基因高風險新生兒-高風險比例與追蹤狀況………………………….22 3.3.3 FLG基因高風險新生兒-衛教後確診比例………………………………….22 第四章、討論與未來展望……………………………………………………………24 4.1基因檢測、臨床診斷、衛教諮詢三者關聯性…………………………………..24 4.2台灣族群FLG基因突變點位統計與國外資訊比較…………………………….24 4.3異位性皮膚炎FLG基因各國家發生率與常見點位分佈……………………….25 4.4 c.1432點位臨床意義之探討……………………………………………………..26 4.5衛教資訊…………………………………………………………………………..26 4.6未來展望….……………………………………………………………………….27 第五章、結論………………………………………………………………………….28 參考文獻………………………………………………………………………………30 附錄…………………………………………………………………………………... 43
dc.language.iso	zh-TW
dc.subject	衛教諮詢	zh_TW
dc.subject	異位性皮膚炎	zh_TW
dc.subject	聚角蛋白微絲基因	zh_TW
dc.subject	皮膚屏障	zh_TW
dc.subject	盛行率	zh_TW
dc.subject	高風險族群	zh_TW
dc.subject	突變點位	zh_TW
dc.subject	台灣族群	zh_TW
dc.subject	基因檢測	zh_TW
dc.subject	臨床診斷	zh_TW
dc.subject	point of mutation	en
dc.subject	atopic dermatitis	en
dc.subject	filaggrin gene	en
dc.subject	skin barrier	en
dc.subject	prevalence	en
dc.subject	high-risk groups	en
dc.subject	health consultation	en
dc.subject	clinical diagnosis	en
dc.subject	genetic testing	en
dc.subject	ethnic groups in Taiwan	en
dc.title	異位性皮膚炎聚角蛋白微絲基因之新生兒篩檢與遺傳諮詢	zh_TW
dc.title	Neonatal screening and genetic counseling for filaggrin gene in atopic dermatitis	en
dc.type	Thesis
dc.date.schoolyear	108-2
dc.description.degree	碩士
dc.contributor.oralexamcommittee	李建南(Chien-Nan Lee),蘇怡寧(Yi-Ning Su)
dc.subject.keyword	異位性皮膚炎,聚角蛋白微絲基因,皮膚屏障,盛行率,高風險族群,突變點位,台灣族群,基因檢測,臨床診斷,衛教諮詢,	zh_TW
dc.subject.keyword	atopic dermatitis,filaggrin gene,skin barrier,prevalence,high-risk groups,point of mutation,ethnic groups in Taiwan,genetic testing,clinical diagnosis,health consultation,	en
dc.relation.page	70
dc.identifier.doi	10.6342/NTU202001892
dc.rights.note	未授權
dc.date.accepted	2020-07-30
dc.contributor.author-college	醫學院	zh_TW
dc.contributor.author-dept	分子醫學研究所	zh_TW
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