Objective: To explore the efficacy of adjusting the dose of imatinib dose in the context of therapeutic drug monitoring (TDM) in patients with gastrointestinal stromal tumors (GISTs) who are receiving adjuvant therapy after complete resection of their tumors. Methods: This was a descriptive study. Inclusion criteria were (1) complete surgical resection with a pathological diagnosis of GIST, (2) postoperative adjuvant therapy with imatinib and dosage adjustment, (3) multiple TDM of imatinib, and (4) complete clinical, pathological, and follow-up data. The data of 70 patients with GISTs treated at Union Hospital, Tongji Medical College, Huazhong University of Science and Technology between January 2015 and December 2023 were collected retrospectively. The study cohort comprised 15 (21.4%) men and 55 (78.6%) women of median age 60 years (range: 25-82). Of the eligible patients, 49 (70.0%) were at high-risk, 14 (20.0%) at intermediate-risk, six (8.6%) at low-risk, and one (1.4%) at very low risk. Patients were followed up by the gastrointestinal stromal tumor clinic every 2-3 months and their plasma concentrations of imatinib were checked. The dose was adjusted to 300 mg/d or 200 mg/d depending on whether they had had ≥ grade III adverse reactions, and whether the first plasma concentration of imatinib was ≥ 1,500 μg/L or between the expected range of 760 μg/L-1,100 μg/L. Studied indicators included adverse reactions, quality of life before and after dose adjustment, and overall survival and recurrence-free survival (RFS) after dose adjustment. Results: Before dose adjustment, all 70 patients received 400 mg of imatinib daily, with initial TDM values of 1,900 ± 568 μg/L, for a median duration of 8.3 months. After dose adjustment, 60 patients received 300 mg daily, with a TDM of 1,216 ± 350 μg/L, whereas 10 received 200 mg daily, with a TDM of 1,023 ± 269 μg/L. The median duration of treatment after dose adjustment was 23.4 months. Compared with those whose dosages were not adjusted, the incidence of bone marrow suppression was significantly lower (74.3% [52/70] vs. 51.4% [36/70], χ2=9.202, P=0.010); as were the incidences of edema (95.7% [67/70] vs. 50.0% [35/70], χ2=40.526, P<0.001); skin reactions (70.0% [49/70] vs. 32.9% [23/70), χ2=22.495, P<0.001); and gastrointestinal reactions (38.6% [27/70] vs. 10.0% [7/70], χ2=15.899, P<0.001) in those whose dosages were adjusted. The average total scores for physical health before and after dose adjustment were 76 ± 5 and 88 ± 4, respectively; whereas the mental health scores were 75 ± 6 and 89 ± 4, respectively. The median follow-up period was 36 months (range 6-126). During the first 3 years of follow-up, five high-risk patients with non-gastric GISTs developed recurrences. The 3-year overall survival rate was 100%, and the 3-year RFS rate was 92.8%, high-risk patients having a 3-year RFS rate of 89.8%. Conclusion: The adverse reactions and quality of life of GIST patients with severe adverse reactions to adjuvant imatinib therapy after complete resection can be mitigated by appropriately reducing the dosage of imatinib under the guidance of TDM.
目的: 探究血药浓度监测指导下伊马替尼减量治疗胃肠间质瘤完整切除术后辅助治疗患者的疗效。 方法: 采用描述性观察性研究方法。纳入标准:(1)手术完整切除且病理诊断为胃肠间质瘤;(2)术后行伊马替尼辅助治疗且存在剂量调整;(3)多次行伊马替尼血药浓度监测;(4)临床病理资料及随访资料完整。回顾性收集2015年1月至2023年12月于华中科技大学同济医学院附属协和医院就诊的70例胃肠间质瘤病例资料。男性15例(21.4%),女性55例(78.6%);中位年龄60(25~82)岁;高危患者49例(70.0%),中危患者14例(20.0%),低危患者6例(8.6%),1例(1.4%)患者行伊马替尼术前治疗。患者每2~3个月至胃肠间质瘤专病门诊复查血药浓度。基于血药浓度监测下,综合患者不良反应是否≥Ⅲ级、首次血药谷浓度是否≥1 500 μg/L以及是否在血药浓度期望区间(760~1 100 μg/L),将剂量调整为300 mg/d或200 mg/d。观察指标包括剂量调整前后本组患者的不良反应、生活质量情况、以及剂量调整后总体生存期(OS)和无复发生存期(RFS)。 结果: 剂量调整前,70例患者每日服药剂量均为400 mg,首次血药谷浓度水平为(1 900±568)μg/L,剂量调整前服药时长中位数为8.3个月。剂量调整后,60例患者每日服用剂量为300 mg,血药谷浓度水平为(1 216±350)μg/L;10例患者服用剂量为200 mg,血药谷浓度水平为(1 023±269)μg/L,剂量调整后服药中位时长为23.4个月。伊马替尼剂量调整后,全组患者骨髓抑制减少[74.3%(52/70)比51.4%(36/70),χ2=9.202,P=0.010];水肿减少[95.7%(67/70)比50.0%(35/70),χ2=40.526,P<0.001];皮肤反应减少[70.0%(49/70)比32.9%(23/70),χ2=22.495,P<0.001];消化道反应减少[38.6%(27/70)比10.0%(7/70),χ2=15.899,P<0.001],差异均有统计学意义(均P<0.05)。剂量调整前后患者躯体健康总测量评分分别为(76±5)和(88±4)分,心理健康总测量评分分别为(75±6)和(89±4)分。全组患者中位随访36(6~126)个月,共有5例高危非胃原发胃肠间质瘤在3年内复发,全组3年OS为100%,3年RFS为92.8%,高危患者3年RFS为89.8%。 结论: 针对完整切除术后行伊马替尼辅助治疗且不良反应严重的胃肠间质瘤患者,在血药浓度监测指导下适当调低服药剂量,有助于减轻患者不良反应,改善患者生活质量。.