含Pemetrexed化學治療於癌症腎功能不全病人嚴重血液毒性風險與療程影響之探討

Kuan-Jen Huang; 黃冠仁

請用此 Handle URI 來引用此文件： http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/78652

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	Kuan-Jen Huang	en
dc.contributor.author	黃冠仁	zh_TW
dc.date.accessioned	2021-07-11T15:09:56Z	-
dc.date.available	2024-07-31
dc.date.copyright	2019-08-28
dc.date.issued	2019
dc.date.submitted	2019-08-12
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dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/78652	-
dc.description.abstract	研究背景對於晚期（advanced）非鱗狀非小細胞肺癌（non-squamous non-small cell lung cancer, NSCLC），若病人不適用標靶治療或免疫治療時，pemetrexed併用platinum的療程組合作為第一線治療，能增加病人存活率並有較低的血液毒性發生率，此療程組合亦是惡性胸膜間皮瘤（malignant pleural mesothelioma, MPM）的藥物治療首選。仿單不建議pemetrexed用於肌酸酐廓清率（Ccr）小於45 mL/min的病人，並且缺乏腎功能調整劑量的資料。雖有許多回溯性研究探討pemetrexed的安全性與腎功能以及相關危險因子的關聯性，然而研究結果不一致且有諸多研究限制。研究目的探討Ccr < 45 mL/min的癌症病人，臨床使用pemetrexed的安全性，比較不同程度腎功能不全者的血液與非血液毒性的發生率，並分析Grade ≥ 3嗜中性球低下的相關危險因子，以及對後續療程的影響。研究方法回溯性世代研究以醫學中心病歷資料進行分析，篩選2014年11月‒2016年11月間使用pemetrexed治療之non-squamous NSCLC與MPM病人，收集涵蓋2008/1‒2018/11期間的臨床資料，包含病人基本資料、抗癌療程處方、相關用藥、實驗檢驗值。白血球低下達最低點（WBC nadir）時，以當次療程周期前的Ccr值作為切點基準分組，比較Ccr < 45 mL/min與 Ccr ≥ 45 mL/min兩組間之Grade ≥ 3嗜中性球低下發生率與對接續療程的影響。此外，以基線（baseline）Ccr值45 mL/min為切點分組，比較兩組間嚴重血液毒性與其他藥物不良反應的發生率，透過次族群分析與敏感度分析驗證結果，並採用Cox比例風險迴歸分析鑑別Grade ≥ 3嗜中性球低下的危險因子。研究終止期間另分析整體療程用藥資料與實驗檢驗值。研究結果從361位病人中篩選出符合研究條件的研究對象共300位。發生所有程度嗜中性球低下者（n=72）之中，Grade ≥ 3嗜中性球低下者的比例於Ccr < 45 mL/min（WBC nadir）組別為（72.2%, 13/18），相較Ccr ≥ 45 mL/min（WBC nadir）組別的比例（31.5%, 17/54）顯著較高（p=0.002）。基線Ccr < 45 mL/min組別（n=30）相較Ccr ≥ 45 mL/min組別（n=270），發生率顯著較高為Grade ≥ 3貧血（23.3% vs. 9.3%, p=0.027）與血清肌酸酐異常增加（36.7% vs. 15.2%, p=0.003），然而，Grade ≥ 3嗜中性球低下發生率無顯著差異（13.3% vs. 9.6%, p=0.52）。基線Ccr < 55 mL/min組別（n=69）相較Ccr ≥ 55 mL/min組別（n=231），顯著高比例發生Grade ≥ 3嗜中性球低下（18.8% vs. 7.4%, p=0.005）、Grade ≥ 3血小板低下（11.6% vs. 3.9%, p=0.029）、血清肌酸酐異常增加（34.8% vs. 12.1%, p< 0.001）與急性腎損傷（5.8% vs. 0.9%, p=0.027）等嚴重血液毒性或腎毒性。研究對象整體而言，Grade ≥ 3嗜中性球低下的危險因子為首次療程前曾發生白血球低下、高血壓、累積療程周期。基線Ccr < 55 mL/min組別，Grade ≥ 3嗜中性球低下相關危險因子為首次療程併用cisplatin（劑量75 mg/m2以下）、累積療程周期大於6次或累積療程周期10次以下、未依據仿單使用vitamin B12；基線Ccr < 45 mL/min組別，併用carboplatin劑量target AUC 5以下可能降低風險。因藥物不良反應終止療程的發生率，基線Ccr < 55 mL/min組別，顯著高於Ccr ≥ 55 mL/min組別（15.9% vs. 5.6%, p=0.010）。研究終止期的血紅素相較基線的數值為低，於基線Ccr < 45 mL/min組別（10.1 g/dL vs. 12.3 g/dL, p < 0.001）與Ccr ≥ 45 mL/min組別（10.8 g/dL vs. 13.0 g/dL, p < 0.001）趨勢相近。結論醫療人員應注意pemetrexed單一使用或併用platinum時，對於基線Ccr < 55 mL/min病人，容易產生Grade ≥ 3嗜中性球低下、Grade ≥ 3血小板低下與腎毒性、容易因為藥物不良反應終止療程，cisplatin之併用與Grade ≥ 3嗜中性球低下風險有關聯性。相較基線Ccr值，以WBC nadir療程周期前Ccr 45 mL/min分組可能更有效偵測到接受pemetrexed治療的病人，是否容易發生Grade ≥ 3嗜中性球低下或白血球低下的警訊，而本研究發現仍待更多研究以佐證。	zh_TW
dc.description.abstract	Background Pemetrexed and platinum combination therapy is first-line treatment for patients with either unresectable malignant pleural mesothelioma (MPM) or advanced non-squamous non-small cell lung cancer (NSCLC) if not suitable for targeted therapy or immunotherapy. Patients with creatinine clearance (Ccr) less than 45 mL/min are not recommended for pemetrexed treatment according to the label. From a few observational studies, there are inconsistent results of whether pemetrexed could be safely used in patients with renal impairment, especially Ccr < 45 mL/min. Objective The study aims at the safety of pemetrexed in cancer patients with Ccr < 45 mL/min, incidence rate of hematologic and non-hematologic toxicities, and the risk factors of Grade ≥ 3 neutropenia as well as impact on regimen of treatment. Methods This cohort study retrospectively collected data from medical records in a medical center. Patients receiving pemetrexed-based regimens for non-squamous NSCLC or MPM from 2014/11‒2016/11 were screened, whose clinical data within the range of 2008/1‒2018/11 were collected. Incidence of Grade ≥ 3 neutropenia and regimen change were compared between patient groups according to the cut-off value of Ccr 45 mL/min prior to the cycle of WBC nadir (Ccr, WBC nadir). Besides, incidence rate of severe hematologic toxicities and other adverse drug events were compared between groups according to baseline Ccr. Subgroup and sensitivity analysis were adopted to examine above findings. Cox regression analysis was used to investigate factors related to Grade ≥ 3 neutropenia. Regimen of treatment and laboratory data at the end of study were analyzed. Results 300 patients in analysis were screened from 361 patients. Proportion of Grade ≥ 3 neutropenia in all-grade neutropenia in patients with Ccr < 45 mL/min (WBC nadir) (2.2%, 13/18) was significantly higher than that in patients with Ccr ≥ 45 mL/min (WBC nadir) (31.5%, 17/54) (p=0.002). Patients with baseline Ccr < 45 mL/min (n=30) had significantly higher rate of Grade ≥ 3 anemia (23.3% vs. 9.3%, p=0.027) and all-grade Scr (serum creatinine) elevation (36.7% vs. 15.2%, p=0.003), compared to those of Ccr ≥ 45 mL/min (n=270). No discrepancy of Grade ≥ 3 neutropenia was found between the two groups. However, patients with baseline Ccr < 55 mL/min (n=69) had significantly higher rate of severe hematologic toxicities and renal toxicity compared to those of Ccr ≥ 55 mL/min (n=231), such as Grade ≥ 3 neutropenia (18.8% vs. 7.4%, p=0.005), Grade ≥ 3 thrombocytopenia (11.6% vs. 3.9%, p=0.029), all-grade SCr elevation (34.8% vs. 12.1%, p< 0.001) and acute kidney injury (5.8% vs. 0.9%, p=0.027). Those risk factors significantly associated with Grade ≥ 3 neutropenia include previous neutropenia before start-up of pemetrexed treatment, hypertension, and number of treatment cycles; nevertheless, cumulative dose of pemetrexed is of significantly lower risk. As for patients with baseline Ccr < 55 mL/min, those risk factors significantly associated with Grade ≥ 3 neutropenia include combined cisplatin use in the first treatment cycle, number of treatment cycles longer than 6 or below 10, off-label or never use of vitamin B12; in contrast, patients with baseline Ccr < 45 mL/min had significantly lower risk when initial dose of carboplatin is below 5 AUC. Incidence of treatment discontinuation by adverse drug event was higher in patients with baseline Ccr < 55 mL/min, compared to those of Ccr ≥ 55 mL/min (15.9% vs. 5.6%, p=0.01). At the end of study, median hemoglobin was significantly lowered than the value at baseline, which was both seen in patients with baseline Ccr < 45 mL/min (10.1 g/dL vs. 12.3 g/dL, p<0.001) and those of Ccr ≥ 45 mL/min (10.8 g/dL vs. 13.0 g/dL, p<0.001). Conclusion Cautions are required in that patients with baseline Ccr < 55 mL/min receiving pemetrexed-based regimens either single agent or combined with platinum are prone to severe hematologic toxicities, renal toxicity, and treatment discontinuation by adverse drug events; moreover, combined with cisplatin is significantly associated with Grade ≥ 3 neutropenia. Ccr < 45 mL/min (WBC nadir), compared to the value at baseline, may be better to distinguish victims of Grade ≥ 3 neutropenia or leukopenia, though further studies are needed.	en
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dc.description.tableofcontents	中文摘要 I Abstract III 目錄 V 表目錄 VIII 圖目錄 X 縮寫對照表 XI 第1章前言 1 第2章文獻探討 2 2.1 非鱗狀非小細胞肺癌 2 2.1.1非鱗狀非小細胞肺癌之流行病學 2 2.1.2 非小細胞肺癌之治療方式 2 2.1.3 非鱗狀非小細胞肺癌之治療原則 3 2.2惡性胸膜間皮瘤 4 2.2.1惡性胸膜間皮瘤之流行病學 4 2.2.2惡性胸膜間皮瘤之治療 4 2.3 Pemetrexed藥品概述 5 2.3.1作用機制 5 2.3.2適應症 5 2.3.3藥品動態學性質 6 2.4 Pemetrexed相關藥物不良反應 8 2.4.1常見藥物不良反應 8 2.4.2常見造成治療終止或延後的藥物不良反應 9 2.5嚴重血液毒性 9 2.5.1嚴重血液毒性發生率 9 2.5.2預防性用藥 10 2.5.3臨床處置與療程調整 10 2.6 Pemetrexed與嚴重血液毒性相關危險因子 11 2.6.1腎功能不全 11 2.6.2抗癌藥品組合 12 2.6.3劑量與療程周期 12 2.6.4併用藥 12 第3章研究目的 13 第4章研究方法 14 4.1研究架構 14 4.1.1研究對象篩選 14 4.1.2研究期間定義 15 4.1.3研究收集資料 15 4.1.4研究目標定義 17 4.1.5 研究對象分組 17 4.1.6 Grade ≥ 3嗜中性球低下之危險因子 17 4.1.7 次族群分析 18 4.1.8 敏感度分析 18 4.2 統計分析 18 4.2.1描述性統計分析 18 4.2.2 Cox比例風險迴歸分析 19 4.3.3 統計軟體 20 第5章研究結果 21 5.1 研究對象篩選流程 21 5.2 研究對象之基本特性與用藥資料 22 5.2.1基本特性資料 24 5.2.2用藥資料 25 5.3 白血球低下達最低點療程周期分析 26 5.3.1 主要研究目標分析 26 5.3.2 發生Grade ≥ 3嗜中性球低下之病人特性與療程分析 26 5.3.3 發生Grade ≥ 3嗜中性球低下對於療程的影響 29 5.3.4腎功能惡化並發生Grade ≥ 3嗜中性球低下病人描述性分析 30 5.4 Grade ≥ 3嗜中性球低下之危險因子分析 31 5.4.1 單變項比例風險迴歸分析 31 5.4.2 多變項比例風險迴歸分析 31 5.5基本特性與用藥資料-以基線Ccr 45 mL/min分組 32 5.5.1基本特性與用藥資料 32 5.5.2 Pemetrexed於不同療程藥品組合之劑量分析 34 5.6 療程相關藥物不良反應-以基線Ccr 45 mL/min分組 35 5.6.1 嚴重血液毒性發生率 35 5.6.2 其他實驗數值相關藥物不良反應 36 5.6.3 臨床症狀相關藥物不良反應 37 5.7 次族群分析 38 5.7.1 Grade ≥ 3嗜中性球低下危險因子分析-基線Ccr 45 mL/min分組 38 5.7.2 Grade ≥ 3嗜中性球低下發生有無之次族群分析 40 5.8 敏感度分析 41 5.8.1 主要研究目標分析-以基線Ccr 55 mL/min分組 41 5.8.2其他實驗數值相關藥物不良反應-以基線Ccr 55 mL/min分組 41 5.8.3實驗數值相關藥物不良反應-以基線Ccr 45-54 mL/min分三組 42 5.8.4 Grade ≥ 3嗜中性球低下危險因子分析-基線Ccr 55 mL/min分組 45 5.9 研究終止期整體療程與實驗檢驗數值分析 47 5.9.1整體療程分析 47 5.9.2實驗檢驗數值分析 48 第6章討論 49 6.1 研究對象之基本特性與用藥資料 49 6.1.1 基本特性與用藥資料 49 6.1.2 目標族群與對照族群之基本特性與用藥資料 50 6.1.3 Pemetrexed於不同療程藥品組合之劑量 51 6.2 Grade ≥ 3嗜中性球低下危險因子探討 51 6.2.1 腎功能不全–以WBC nadir療程周期前Ccr分組 51 6.2.2 腎功能不全–以基線Ccr分組 52 6.2.3 抗癌藥品組合 54 6.2.4劑量 55 6.2.5療程周期 55 6.2.6併用藥 56 6.2.7其他危險因子 57 6.3 發生Grade ≥ 3嗜中性球低下對於療程的影響 58 6.4其他pemetrexed相關藥物不良反應 58 6.4.1 其他嚴重血液毒性 58 6.4.2 其他實驗數值相關藥物不良反應 60 6.4.3臨床症狀相關藥物不良反應 61 6.5 療程終止原因探討 61 6.5.1療程終止的常見原因 61 6.5.2終止療程的常見藥物不良反應 62 6.5.3 研究終止期實驗檢驗數值分析 62 6.6研究限制與優勢 63 6.6.1研究限制 63 6.6.2研究優勢 64 第7章結論與建議 65 參考文獻 66 附錄 73
dc.language.iso	zh-TW
dc.title	含Pemetrexed化學治療於癌症腎功能不全病人嚴重血液毒性風險與療程影響之探討	zh_TW
dc.title	Risk of Severe Hematologic Toxicities and Impact of Pemetrexed-based Regimens on Cancer Patients with Renal Impairment	en
dc.type	Thesis
dc.date.schoolyear	107-2
dc.description.degree	碩士
dc.contributor.coadvisor	何?芳(Yunn-Fang Ho)
dc.contributor.oralexamcommittee	羅英(Yin Lo),林家齊,黃政文
dc.subject.keyword	Pemetrexed,腎功能不全,血液毒性,危險因子,肌酸酐廓清率,	zh_TW
dc.subject.keyword	Pemetrexed,renal impairment,hematologic toxicity,risk factor,creatinine clearance,	en
dc.relation.page	81
dc.identifier.doi	10.6342/NTU201902627
dc.rights.note	有償授權
dc.date.accepted	2019-08-12
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	2024-07-31	-
顯示於系所單位：	臨床藥學研究所

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