使用 MRI 引导的 HDR 近距离治疗(HDR)或整合的 VMAT(IB-VMAT)推量进行局部前列腺癌的肿瘤靶向剂量递增:剂量学、毒性和健康相关生活质量。
Tumor-targeted dose escalation for localized prostate cancer using MR-guided HDR brachytherapy (HDR) or integrated VMAT (IB-VMAT) boost: Dosimetry, toxicity and health related quality of life.
机构信息
Princess Margaret Cancer Center, University Health Network, Toronto, Canada; Department of Radiation Oncology, University of Toronto, Canada; Hospital Clinico San Carlos, Madrid, Spain.
Princess Margaret Cancer Center, University Health Network, Toronto, Canada.
出版信息
Radiother Oncol. 2020 Aug;149:240-245. doi: 10.1016/j.radonc.2020.05.029. Epub 2020 May 22.
PURPOSE
To report dosimetry, preliminary toxicity and health-related quality of life (HRQoL) outcomes of tumor-targeted dose-escalation delivered by integrated boost volumetric arc therapy (IB-VMAT) or MR-guided HDR brachytherapy (HDR) boost for prostate cancer.
MATERIALS AND METHODS
Patients diagnosed with localized prostate cancer, with at least 1 identifiable intraprostatic lesion on multiparametric MRI (mpMRI) were enrolled in a prospective non-randomized phase II study. All patients received VMAT to the prostate alone (76 Gy in 38 fractions) plus a GTV boost: IB-VMAT (95 Gy in 38 fractions) or MR-guided HDR (10 Gy single fraction). GTV was delineated on mpMRI and deformably registered to planning CT scans. Comparative dosimetry using EQD2 assuming α/β 3 Gy was performed. Toxicity and health-related quality of life data (HRQoL) data were collected using CTCAE v.4.0, International Prostate Symptom Score (IPSS) and the Expanded Prostate Index Composite (EPIC).
RESULTS
Forty patients received IB-VMAT and 40 HDR boost. Organs at risk and target minimal doses were comparable between the two arms. HDR achieved higher mean and maximal tumor doses (p < 0.05). Median follow-up was 31 months (range 25-48); Acute grade G2 genitourinary (GU) toxicity was 30% and 37.5% in IB-VMAT and HDR boost, while gastrointestinal (GI) toxicity was 7.5% and 10%, respectively. Three patients developed acute G3 events, two GU toxicity (one IB-VMAT and one HDR boost) and one GI (IB-VMAT). Late G2 GU toxicity was 25% and 17.5% in the IB-VMAT and HDR boost arm and G2 GI was 5% and 7.5%, respectively. Two patients, both on the IB-VMAT arm, developed late G3 toxicity: one GI and one GU. No statistically significant difference was found in HRQoL between radiotherapy techniques (p > 0.2). Urinary and bowel HRQoL domains in both groups declined significantly by week 6 of treatment in both arms (p < 0.05) and recovered baseline scores at 6 months.
CONCLUSION
Intraprostatic tumor dose escalation using IB-VMAT or MR-guided HDR boost achieved comparable OAR dosimetry, toxicity and HRQOL outcomes, but higher mean and maximal tumor dose were achieved with the HDR technique. Further follow-up will determine long-term outcomes including disease control.
目的
报告通过容积弧形调强放疗(VMAT)的肿瘤靶向剂量递增的剂量学、初步毒性和健康相关生活质量(HRQoL)结果,以及使用磁共振引导高剂量率近距离治疗(HDR)推量治疗前列腺癌的结果。
材料和方法
本前瞻性非随机 2 期研究纳入了至少在多参数磁共振成像(mpMRI)上有 1 个前列腺内可识别病变的局限性前列腺癌患者。所有患者均接受前列腺 VMAT 治疗(76 Gy 分 38 次)加 GTV 推量:VMAT 推量(95 Gy 分 38 次)或磁共振引导 HDR(10 Gy 单次)。GTV 在 mpMRI 上勾画,并在计划 CT 扫描上进行可变形配准。使用 EQD2(假设 α/β 为 3 Gy)进行比较剂量学。使用 CTCAE v.4.0、国际前列腺症状评分(IPSS)和前列腺指数综合评分(EPIC)收集毒性和健康相关生活质量(HRQoL)数据。
结果
40 例患者接受了 VMAT 推量治疗,40 例患者接受了 HDR 推量治疗。2 组的危及器官和靶区最小剂量相当。HDR 达到了更高的平均和最大肿瘤剂量(p<0.05)。中位随访时间为 31 个月(范围 25-48 个月);IB-VMAT 和 HDR 推量组急性 2 级泌尿生殖系统(GU)毒性发生率分别为 30%和 37.5%,胃肠道(GI)毒性发生率分别为 7.5%和 10%。3 例患者发生急性 3 级事件,2 例 GU 毒性(1 例 IB-VMAT,1 例 HDR 推量),1 例 GI 毒性(IB-VMAT)。IB-VMAT 和 HDR 推量组的晚期 2 级 GU 毒性发生率分别为 25%和 17.5%,晚期 2 级 GI 毒性发生率分别为 5%和 7.5%。2 例患者(均在 IB-VMAT 组)发生晚期 3 级毒性:1 例 GI 毒性,1 例 GU 毒性。放射治疗技术之间在 HRQoL 方面无统计学差异(p>0.2)。2 组患者在治疗第 6 周时泌尿和肠道 HRQoL 域均显著下降(p<0.05),6 个月时恢复至基线水平。
结论
使用 IB-VMAT 或磁共振引导 HDR 推量进行前列腺内肿瘤剂量递增,可获得相当的 OAR 剂量学、毒性和 HRQoL 结果,但 HDR 技术可达到更高的平均和最大肿瘤剂量。进一步随访将确定包括疾病控制在内的长期结果。
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