乳癌病人使用tamoxifen發生子宮相關病變及婦科監測之研究

Wan-Jyun Peng; 彭琬珺

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/78768

完整後設資料紀錄

DC 欄位	值	語言
dc.contributor.advisor	陳燕惠(Yen-Hui Chen)
dc.contributor.author	Wan-Jyun Peng	en
dc.contributor.author	彭琬珺	zh_TW
dc.date.accessioned	2021-07-11T15:17:59Z	-
dc.date.available	2024-08-28
dc.date.copyright	2019-08-28
dc.date.issued	2019
dc.date.submitted	2019-07-17
dc.identifier.citation	Bray F, Ferlay J, Soerjomataram I, et al. Global cancer statistics 2018: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries. CA: A Cancer Journal for Clinicians. 2018;68(6):394-424. 衛生福利部國民健康署. 癌症登記報告. 2018. Davies C, Godwin J, Gray R, et al. Relevance of breast cancer hormone receptors and other factors to the efficacy of adjuvant tamoxifen: patient-level meta-analysis of randomised trials. Lancet. 2011;378(9793):771-784. Davies C, Pan H, Godwin J, et al. Long-term effects of continuing adjuvant tamoxifen to 10 years versus stopping at 5 years after diagnosis of oestrogen receptor-positive breast cancer: ATLAS, a randomised trial. Lancet. 2013;381(9869):805-816. Gray RG, Rea D, Handley K, et al. aTTom: Long-term effects of continuing adjuvant tamoxifen to 10 years versus stopping at 5 years in 6,953 women with early breast cancer. Journal of Clinical Oncology. 2013;31(15_suppl):5-5. Chen JY, Kuo SJ, Liaw YP, et al. Endometrial cancer incidence in breast cancer patients correlating with age and duration of tamoxifen use: a population based study. J Cancer. 2014;5(2):151-155. Committee Opinion No. 601: Tamoxifen and uterine cancer. Obstet Gynecol. 2014;123(6):1394-1397. Tamoxifen and the Endometrium (C-Gyn 12), College Statement. Royal Australian and New Zealand College of Obstetricians and Gynaecologists. 2015. Howlader N NA, Krapcho M, Miller D, et al. SEER Cancer Statistics Review, 1975-2014,. National Cancer Institute. 2017. Bergman L, Beelen MLR, Gallee MPW, et al. Risk and prognosis of endometrial cancer after tamoxifen for breast cancer. The Lancet. 2000;356(9233):881-887. Wickerham DL, Fisher B, Wolmark N, et al. Association of Tamoxifen and Uterine Sarcoma. Journal of Clinical Oncology. 2002;20(11):2758-2760. Chlebowski RT, Schottinger JE, Shi J, et al. Aromatase inhibitors, tamoxifen, and endometrial cancer in breast cancer survivors. Cancer. 2015;121(13):2147-2155. Lee Y, Park YR, Kim HR, et al. Event-free survival following early endometrial events in breast cancer patients treated with anti-hormonal therapy: A nationwide claims data study. Medicine (Baltimore). 2019;98(2):e13976. Matsuo K, Ross MS, Bush SH, et al. Tumor characteristics and survival outcomes of women with tamoxifen-related uterine carcinosarcoma. Gynecologic oncology. 2017;144(2):329-335. Wright JD, Desai VB, Chen L, et al. Utilization of gynecologic services in women with breast cancer receiving hormonal therapy. Am J Obstet Gynecol. 2017(217(1):59.e1-59.e12.).
dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/78768	-
dc.description.abstract	研究背景：Tamoxifen 為 ER/PR(+) 乳癌病人的抗荷爾蒙用藥。有研究顯示使用 tamoxifen 從 5 年延長至 10 年，可以更有效地降低乳癌的復發率及死亡率。治療指引因此建議將 tamoxifen 的服藥期延長至 10 年，但罹患子宮體癌的機率也相對提高。雖曾有研究以台灣健保資料庫分析，發現年齡及 tamoxifen 之服藥期與罹患子宮體癌風險有關，但仍需更多研究探討延長 tamoxifen 之服藥期（超過5年）是否有較高機率罹患子宮體癌。另外有些研究以子宮內膜厚度作為子宮體癌的替代終點，仍存有爭議，因此需更多研究評估使用 tamoxifen 乳癌病人，所接受之例行性婦科監測。研究目的：　 1.分析國內病人使用tamoxifen後，子宮體癌的發生率，並分析相關風險因子，如：年齡、延長tamoxifen服藥期等。 2.分析國內病人使用tamoxifen後，子宮體癌的相關診療資料，如：組織類型等。 3.分析國內病人使用tamoxifen後，接受子宮內膜搔刮術的發生率及其病理結果。研究方法：以臺大醫院的相關資料，進行回溯性世代研究。在臺大醫院癌症登記檔中，確診為原發性乳癌的女性病人，經納入以及排除標準篩選後，共 9,668 人納入，依照所接受之乳癌輔助性荷爾蒙治療，分為只使用過 tamoxifen（以 Tamoxifen-only 簡稱，共 2612 人，27.0%），皆曾使用過 tamoxifen 和 aromatase inhibitor（以 Both 簡稱，共 1754 人，18.1%），只使用過 aromatase inhibitor（以 AI-only 簡稱，共 1536 人，15.9%），未使用過乳癌輔助性荷爾蒙治療（以 Non-user 簡稱，共 3766 人，39.0%），並分析子宮體癌的發生率及相關風險因子。研究結果：在 9,668 位乳癌病人之中，後續被診斷為子宮體癌共有40人，其中 Tamoxifen-only 組的發生率最高（19/2612=0.7%），相較於 AI-only 組（4/1536=0.3%）或 Non-user 組（11/3766=0.3%）。就子宮體癌組織類型而言，Tamoxifen-only組最多為癌瘤（carcinoma）（84.2%），包含子宮內膜腺癌（endometrioid adenocarcinoma）（78.9%），亮細胞腺癌（clear cell adenocarcinoma）（5.3%）；另一類則為肉瘤（sarcoma）（15.8%）包含惡性肉瘤（carcinosarcoma）（10.5%）和基質惡性肉瘤（endometrial stromal sarcoma）（5.3%），其中並沒有一般子宮體癌之肉瘤族群（sarcoma）較常發生的平滑肌肉瘤（leiomyosarcoma）。由 KM 存活曲線顯示，Tamoxifen-only 組相較於其他三組，有顯著較低的無子宮體癌存活率（p=0.038）。由單變項比例風險迴歸分析結果得知，在整體族群中，BMI≥25 kg/m2 、乳小葉原位癌（LCIS）和乳管原位癌（DCIS），皆顯著增加子宮體癌發生風險。由多變項比例風險迴歸分析結果得知，Tamoxifen-only組，相較於Non-user組，有較高的子宮體癌發生風險，且達統計顯著。另外，乳癌診斷年齡50 歲以上及BMI≥25 kg/m2 皆顯著增加子宮體癌發生風險。另將 tamoxifen 開始使用至追蹤結束之間隔時間，以每年做次族群之多變項比例風險迴歸分析，並同時放入年齡≥50歲與 BMI≥25 kg/m2作校正。迴歸分析的結果顯示tamoxifen 在開始使用後4年之內，每一年分層之Tamoxifen only組，相較於Non-user 組皆有顯著增加子宮體癌的風險。於乳癌診斷後接受子宮內膜搔刮術共 507 次，其中最多為 Tamoxifen-only 組（354/507=69.8%），相較於 Both 組（16.4%），Non-user 組（11.0%），以及AI-only 組（2.8%）。病理結果顯示為子宮體癌或內膜增生，最多為 Tamoxifen-only 組（21/354=5.9%），大部分在接受子宮搔刮術前，沒有異常子宮出血（237/354=66.9%），但仍有一定比例之病理結果顯示為子宮體癌或內膜增生(9/354=2.6%)。結論：由多變項比例風險迴歸分析結果得知，Tamoxifen-only 組、乳癌診斷年齡 50 歲以上以及 BMI≥25 kg/m2皆顯著增加子宮體癌發生風險。就子宮體癌組織類型而言，Tamoxifen-only 組雖最多為癌瘤（carcinoma），但另一類肉瘤（sarcoma）較一般子宮體癌族群發生比例高（15.8% 相較於 2~5%）。此外，於乳癌診斷後，接受子宮內膜搔刮術者，Tamoxifen-only 組大部分在接受子宮搔刮術前，沒有異常子宮出血，但仍有一定比例的病理結果顯示為子宮體癌或內膜增生。因此病人在開始使用 tamoxifen，尤其具上述風險因子時，應每年定期接受婦科檢查。	zh_TW
dc.description.abstract	Background: Tamoxifen is an anti-hormonal drug which is commonly used for hormone receptor-positive breast cancer patients. Two randomized controlled trials showed that the extended use of tamoxifen for 10 years, compared to 5 years, significantly reduced the recurrence and mortality of breast cancer. However, the risk of endometrial cancer increased. Few publications examine whether the extended use of tamoxifen (>5 years) have a higher risk of tamoxifen-related uterine events. Since the increase in endometrium thickness is still controversial as a surrogate measure of uterine cancer, studies are needed to evaluate feasible routine gynecologic surveillance in breast cancer patients with tamoxifen regimen. Study objectives: 1.To analyze the rates of uterine cancer in patients treated with tamoxifen and to identify the risk factors of tamoxifen-related uterine cancer such as age, extended use of tamoxifen, etc. 2.To evaluate tamoxifen-related uterine cancer characteristics, such as histology, etc. 3.To evaluate the event count and pathological diagnosis in patients proceeding dilatation and curettage (D and C) after tamoxifen use. Methods: This is a retrospective cohort study enrolling female patients diagnosed with breast cancer from the National Taiwan University Hospital cancer register. A total of 9,668 patients who fulfilled inclusion and exclusion criteria were grouped by the treatment with tamoxifen-only (N=2612, 27%), both tamoxifen and aromatase inhibitor (N=1754, 18.1%), aromatase inhibitor-only (N=1536, 18.1%), and non-user (N=3766, 39%) for analyses of incidence rates and risk factors of uterine cancer. Results: In the 9668 breast cancer patients, 40 patients were subsequently diagnosed with uterine cancer. The tamoxifen-only group had higher incidence rate (19/2612, 0.7%) than AI-only or non-user group (4/1536, 0.3% or 11/3766, 0.3%). Uterine cancer in tamoxifen-only group was mostly carcinoma (84.2%), including endometrioid adenocarcinoma (78.9%) and clear cell adenocarcinoma (5.3%), subtyped by histologic classification. Sarcoma was found 15.8%, including carcinosarcoma (10.5%) and endometrial stromal sarcoma (5.3%). None was leiomyosarcoma which had been mostly found in all cause uterine sarcoma. The Kaplan-Meier survival curve showed that tamoxifen-only group had the lowest uterine cancer-free probability among the four groups (p=0.038). BMI≥25 kg/m2, lobular carcinoma in situ (LCIS), ductal carcinoma in situ (DCIS) breast cancer were significant risk factors of uterine cancer in the total population using a univariate cox regression model. Furthermore, the multivariate cox regression model indicated significantly higher risk of uterine cancer in the tamoxifen-only group than the non-user group. Age above 50 years and BMI≥25 kg/m2 also increased the risk of uterine cancer significantly. When patients were stratified with time from tamoxifen treatment to the end of follow-up in one-year intervals, the multivariate cox regression model, adjusted by age above 50 years and BMI above 25 kg/m2, indicated that the uterine cancer risk was higher in the tamoxifen-only group than the non-user group within 4 years of tamoxifen use. The dilatation and curettage (D and C) events were counted 507 in all patients after breast cancer diagnosis. The tamoxifen-only group contributed to the total event mostly (354/507, 69.8%), compared to the both group (16.4%), non-user group (11.0%) and AI-only group (2.8%). The tamoxifen-only group had the highest event count of either uterine cancer or endometrial hyperplasia (21/354, 5.9%) among the four groups. Two third of the tamoxifen-only patients had no abnormal uterine bleeding before D and C (237/354, 66.9%) with positive rate of uterine cancer or endometrial hyperplasia as much as 2.6% (9/354). Conclusion: The tamoxifen-only group vs non-user group, age above 50 years and BMI≥25 kg/m2 increased the risk for uterine cancer significantly. Most uterine cancer in tamoxifen-only group was histologically classified as carcinoma while the sarcoma rate was higher than all cause uterine cancer population (15.8% vs 2-3%). Positive rate of uterine cancer or endometrial hyperplasia was as much as 2.6% in the tamoxifen-only patients without abnormal uterine bleeding before D and C. It indicates that routine gynecological check is an important follow-up in breast cancer patients with tamoxifen treatment.	en
dc.description.provenance	Made available in DSpace on 2021-07-11T15:17:59Z (GMT). No. of bitstreams: 1 ntu-108-R06451005-1.pdf: 1377054 bytes, checksum: 97c70a9846c0e1fd7d6f2b61575fc265 (MD5) Previous issue date: 2019	en
dc.description.tableofcontents	中文摘要 I 英文摘要 IV 表目錄 IX 圖目錄 X 縮寫對照表 XI 第 1 章緒論 1 1. 1 乳癌與子宮體癌的流行病學 1 1. 2 使用 tamoxifen 與發生子宮體癌的相關性 3 1. 3 使用 tamoxifen 病人定期接受婦科檢查 4 1. 4 研究目的 5 第 2 章研究方法與材料 6 2. 1 研究材料 6 2. 2 研究族群與架構 6 2. 2. 1 納入與排除條件 6 2. 2. 2 研究期間定義 7 2. 2. 3 研究族群之分組 7 2. 3 研究族群相關資料之收集 8 2. 4 統計分析 11 2. 4. 1 研究族群之描述性統計 11 2. 4. 2 研究族群之組間差異 11 2. 4. 3 存活分析（Kaplan-Meier survival curve） 11 2. 4. 4 比例風險迴歸分析（Cox proportional hazard regression） 12 2. 4. 5 統計軟體 12 第 3 章研究結果 13 3. 1 研究族群之建立 13 3. 2 研究族群之背景資料敘述 14 3. 2. 1 病人相關基本資料 14 3. 2. 2 乳癌相關診療資料 15 3. 3 子宮體癌之相關診療資料 24 3. 4 無子宮體癌存活曲線 31 3. 5 整體族群子宮體癌之相關風險因子 33 3. 5. 1 整體族群之單變項比例風險迴歸分析 33 3. 5. 2 整體族群之多變項比例風險迴歸分析 34 3. 6 Tamoxifen開始使用至追蹤結束間隔時間之次族群分析 38 3. 6. 1 Tamoxifen-only組之背景資料敘述 38 3. 6. 2 次族群之多變項比例風險迴歸分析 38 3. 7 接受子宮內膜搔刮術之發生率及病理結果 41 第 4 章討論 44 4. 1 研究族群之背景資料分析 44 4. 2 子宮體癌之相關診療資料 46 4. 3 子宮體癌之相關風險因子 47 4. 4 接受子宮內膜搔刮術之發生率及病理結果 49 4. 5 研究限制 50 4. 6 研究優勢 51 第 5 章結論與未來展望 52 參考文獻 53 附錄 55
dc.language.iso	zh-TW
dc.subject	乳癌	zh_TW
dc.subject	子宮體癌	zh_TW
dc.subject	tamoxifen	zh_TW
dc.subject	危險因子	zh_TW
dc.subject	uterine cancer	en
dc.subject	tamoxifen	en
dc.subject	risk factor	en
dc.subject	breast cancer	en
dc.title	乳癌病人使用tamoxifen發生子宮相關病變及婦科監測之研究	zh_TW
dc.title	Tamoxifen-related Uterine Events and Gynecologic Surveillance in Breast Cancer Patients	en
dc.type	Thesis
dc.date.schoolyear	107-2
dc.description.degree	碩士
dc.contributor.coadvisor	魏凌鴻(Lin-Hung Wei)
dc.contributor.oralexamcommittee	張文君(Wen-Chun Chang),林季宏(Ching-Hung Lin)
dc.subject.keyword	tamoxifen,子宮體癌,乳癌,危險因子,	zh_TW
dc.subject.keyword	tamoxifen,uterine cancer,breast cancer,risk factor,	en
dc.relation.page	63
dc.identifier.doi	10.6342/NTU201901486
dc.rights.note	有償授權
dc.date.accepted	2019-07-18
dc.contributor.author-college	醫學院	zh_TW
dc.contributor.author-dept	臨床藥學研究所	zh_TW
dc.date.embargo-lift	2024-08-28	-
顯示於系所單位：	臨床藥學研究所

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