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  1. NTU Theses and Dissertations Repository
  2. 公共衛生學院
  3. 公共衛生碩士學位學程
請用此 Handle URI 來引用此文件: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/102053
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dc.contributor.advisor李達宇zh_TW
dc.contributor.advisorTa-Yu Leeen
dc.contributor.author楊艾庭zh_TW
dc.contributor.authorAi-Ting Yangen
dc.date.accessioned2026-03-12T16:14:33Z-
dc.date.available2026-03-13-
dc.date.copyright2026-03-12-
dc.date.issued2026-
dc.date.submitted2026-02-03-
dc.identifier.citation參考文獻
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50. Ong C, Briones J, Lim ZZ, et al. Cost-Effectiveness of Dupilumab and Oral Janus Kinase Inhibitors for the Treatment of Moderate-to-Severe Atopic Dermatitis in Singapore. PharmacoEconomics-Open 2024;8(6):809–822.
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dc.identifier.urihttp://tdr.lib.ntu.edu.tw/jspui/handle/123456789/102053-
dc.description.abstract背景:異位性皮膚炎(Atopic Dermatitis, AD)是一種慢性發炎性皮膚疾病,在台灣盛行率約1.28%,其中 26.7% 為中重度的患者,不少的患者生活品質不佳,同時也對健保造成龐大的醫療支出。傳統治療方式對這些患者的療效往往有限,近年問世的生物製劑和口服小分子鏢靶藥物,為患者帶來全新的治療選擇,包括:Dupilumab(杜避炎)與 JAK 抑制劑(如 Abrocitinib、Baricitinib、Upadacitinib)。本研究從台灣全民健康保險觀點,評估這些新療法相較於最佳支持治療(Best Supportive Care, BSC)之成本效用與財務影響。
方法:本研究之成本效用分析,建構一個結合決策樹與馬可夫模型之混合模型,評估短期與長期(1–20 年)之臨床與經濟結果,參數來源包含臨床試驗療效、健保直接支付的醫療成本,以及 EQ-5D 效用值。所有治療均包含外用類固醇或鈣調磷酸酶抑制劑(Calcineurin)為基礎療法。研究結果以品質調整生命年(QALY)與增量成本效益比(ICER)表示,並以每 QALY 新台幣 200 萬元為支付意願閾值,所有結果均以 3% 折現率計算。亦進行敏感度分析測試模型的穩健性。財務影響分析(Budget Impact Analysis, BIA)則以健保署觀點,估算 2026–2030 年,比較現行之BSC 以及新藥,包括: Dupilumab 與JAK 抑制劑(Upadacitinib、Abrocitinib、
Baricitinib),針對中重度異位性皮膚炎(AD)新療法納入台灣全民健康保險體系後,所產生的財務影響。
結果: 在所有療法中,每日口服 Upadacitinib 30 毫克為最具成本效益選項(11.0782 QALYs;相較於 BSC 其ICER 為NT$1,250,903/QALY),其次為Upadacitinib 15 毫克(NT$1,376,435/QALY)。Dupilumab 在成本效益上遭到排除(被支配),Baricitinib 的 ICER 超出 NT$2,000,000/QALY 閾值。敏感度分析顯示結果具有穩健性,其中療效效用值提升、藥品價格與中止治療率為主要影響因子。財務影響分析預估五年總增額支出達 NT$117 億元,主因為藥費支出,單位病人之年均增額成本由 NT$339,000 下降至 NT$265,000。
結論: 每日服用 Upadacitinib 30 毫克為治療台灣中重度異位性皮膚炎成人患者之最具成本效益選項。然而,其高昂的總體財務衝擊顯示未來須配合合理定價與
給付策略,方能兼顧健保可負擔性與病患可近性。
zh_TW
dc.description.abstractBackground: Atopic dermatitis (AD), a chronic inflammatory skin disease, affects 1.28 of Taiwan’s population, with 26.7% having moderate-to-severe cases, causing significant healthcare costs and quality-of-life impairments. Conventional treatments often fail these patients, necessitating novel therapies like Dupilumab and Janus kinase (JAK) inhibitors (Abrocitinib, Baricitinib, Upadacitinib). This study evaluates the cost-utility and budget impact of these therapies versus best supportive care (BSC) for adults with moderate-to-severe AD from Taiwan’s NHI perspective.
Methods: A hybrid decision tree-Markov model assessed short- and long-term (Years 1–20) outcomes using trial efficacy, NHI costs (2022 NT$), and EQ-5D utilities.Interventions included topical corticosteroids/calcineurin inhibitors. Outcomes were quality-adjusted life-years (QALYs) and incremental cost-effectiveness ratios (ICERs), discounted at 3%, with a NT$2,000,000/QALY threshold. Sensitivity analyses tested robustness. A five-year (2026–2030) budget impact analysis (BIA) included epidemiology and market uptake.
Results: Upadacitinib 30 mg was most cost-effective (11.0782 QALYs, ICER NT$1,250,903/QALY vs BSC), followed by Upadacitinib 15 mg (NT$1,376,435/QALY). Dupilumab was dominated; Baricitinib’s ICERs exceeded NT$2,000,000/QALY. Sensitivity analyses confirmed robustness, with utility gains, medication costs, and discontinuation rates as key drivers. The BIA estimated a NT$117 billion incremental impact, driven by drug costs, with per-patient increments falling from NT$339,000 to NT$265,000.
Conclusion: Upadacitinib 30 mg was the most cost-effective option for moderate-to-severe atopic dermatitis in Taiwan, but its high budget impact underscores the need forstrategic pricing and reimbursement policies to ensure long-term affordability and access.
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dc.description.tableofcontents論文審定書 I
誌謝 II
中文摘要 III
英文摘要 V
第一章 導論 1
第一節 實習單位特色與簡介 1
第二節 研究背景 2
第三節 研究目的與研究問題 4
第二章 文獻回顧 6
第一節 異位性皮膚炎致病機轉 6
第二節 異位性皮膚炎診斷方式 7
一、 診斷方式 7
二、 嚴重程度評估與健保給付條件 9
第三節 異位性皮膚炎治療方式 11
一、 生物製劑臨床試驗療效 13
二、 JAK 抑制劑臨床試驗療效 14
第四節 國內外相關成本效益研究證據 17
第三章 研究方法 21
第一節 成本效用分析 21
一、 PICOS 與模型架構 21
二、 參數來源與變項定義 27
(一) 健康狀態轉移機率 27
(二) 成本參數 31
(三) 效用值參數 35
(四) 使用頻率參數 37
三、 敏感度分析 42
四、 情境分析 42
第二節 財務影響分析 43
一、 參數來源與變項定義 45
(一) 使用人數推估 45
(二) 成本參數 48
(三) 市占率 51
第四章 研究結果 53
第一節 成本效用分析 53
一、 單因子敏感度分析 56
二、 情境分析 80
三、 機率性敏感度分析 83
第二節 財務影響分析 84
第五章 研究限制 89
第六章 政策意涵與結論 90
參考文獻 92
-
dc.language.isozh_TW-
dc.subject成本效用分析-
dc.subject異位性皮膚炎-
dc.subject財務影響分析-
dc.subject杜避炎-
dc.subjectJAK 抑制劑-
dc.subjectcost-utility analysis-
dc.subjectatopic dermatitis-
dc.subjectbudget impact analysis-
dc.subjectdupilumab-
dc.subjectJAK inhibitors-
dc.title臺灣中重度異位性皮膚炎使用杜避炎或口服JAK抑制劑相較於常規治療之成本效用與財務影響分析zh_TW
dc.titleCost-Utility and Budget Impact of Dupilumab or Oral JAK Inhibitors compared with Best Supportive Care for the treatment of Moderate-to-Severe Atopic Dermatitis in Taiwanen
dc.typeThesis-
dc.date.schoolyear114-1-
dc.description.degree碩士-
dc.contributor.oralexamcommittee楊銘欽;高暉涵;丁淑敏zh_TW
dc.contributor.oralexamcommitteeMing-Chin Yang;Hui-Han Kao;Shu-Min Dingen
dc.subject.keyword成本效用分析,異位性皮膚炎財務影響分析杜避炎JAK 抑制劑zh_TW
dc.subject.keywordcost-utility analysis,atopic dermatitisbudget impact analysisdupilumabJAK inhibitorsen
dc.relation.page101-
dc.identifier.doi10.6342/NTU202600545-
dc.rights.note同意授權(全球公開)-
dc.date.accepted2026-02-03-
dc.contributor.author-college公共衛生學院-
dc.contributor.author-dept公共衛生碩士學位學程-
dc.date.embargo-lift2031-02-01-
顯示於系所單位:公共衛生碩士學位學程

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