Reis Ferreira Miguel, Khan Atia, Thomas Karen, Truelove Lesley, McNair Helen, Gao Annie, Parker Chris C, Huddart Robert, Bidmead Margaret, Eeles Ros, Khoo Vincent, van As Nicholas J, Hansen Vibeke N, Dearnaley David P
Division of Radiotherapy and Imaging, Institute of Cancer Research, London, United Kingdom; Urology Unit, Royal Marsden NHS Foundation Trust, London, United Kingdom.
Research Data Management and Statistics Unit, Royal Marsden NHS Foundation Trust, London, United Kingdom.
Int J Radiat Oncol Biol Phys. 2017 Dec 1;99(5):1234-1242. doi: 10.1016/j.ijrobp.2017.07.041. Epub 2017 Aug 2.
To investigate the feasibility of dose escalation and hypofractionation of pelvic lymph node intensity modulated radiation therapy (PLN-IMRT) in prostate cancer (PCa).
In a phase 1/2 study, patients with advanced localized PCa were sequentially treated with 70 to 74 Gy to the prostate and dose-escalating PLN-IMRT at doses of 50 Gy (cohort 1), 55 Gy (cohort 2), and 60 Gy (cohort 3) in 35 to 37 fractions. Two hypofractionated cohorts received 60 Gy to the prostate and 47 Gy to PLN in 20 fractions over 4 weeks (cohort 4) and 5 weeks (cohort 5). All patients received long-course androgen deprivation therapy. Primary outcome was late Radiation Therapy Oncology Group toxicity at 2 years after radiation therapy for all cohorts. Secondary outcomes were acute and late toxicity using other clinician/patient-reported instruments and treatment efficacy.
Between August 9, 2000, and June 9, 2010, 447 patients were enrolled. Median follow-up was 90 months. The 2-year rates of grade 2+ bowel/bladder toxicity were as follows: cohort 1, 8.3%/4.2% (95% confidence interval 2.2%-29.4%/0.6%-26.1%); cohort 2, 8.9%/5.9% (4.1%-18.7%/2.3%-15.0%); cohort 3, 13.2%/2.9% (8.6%-20.2%/1.1%-7.7%); cohort 4, 16.4%/4.8% (9.2%-28.4%/1.6%-14.3%); cohort 5, 12.2%/7.3% (7.6%-19.5%/3.9%-13.6%). Prevalence of bowel and bladder toxicity seemed to be stable over time. Other scales mirrored these results. The biochemical/clinical failure-free rate was 71% (66%-75%) at 5 years for the whole group, with pelvic lymph node control in 94% of patients.
This study shows the safety and tolerability of PLN-IMRT. Ongoing and planned phase 3 studies will need to demonstrate an increase in efficacy using PLN-IMRT to offset the small increase in bowel side effects compared with prostate-only IMRT.
探讨前列腺癌(PCa)盆腔淋巴结调强放射治疗(PLN-IMRT)剂量递增及大分割放疗的可行性。
在一项1/2期研究中,晚期局限性PCa患者先接受70至74 Gy的前列腺照射,然后依次接受剂量递增的PLN-IMRT,剂量分别为50 Gy(队列1)、55 Gy(队列2)和60 Gy(队列3),分35至37次分割。两个大分割队列在4周(队列4)和5周(队列5)内分20次给予前列腺60 Gy和PLN 47 Gy。所有患者均接受长期雄激素剥夺治疗。主要结局是所有队列放疗后2年的晚期放射肿瘤学组毒性。次要结局是使用其他临床医生/患者报告的工具评估的急性和晚期毒性以及治疗效果。
2000年8月9日至2010年6月9日期间,共纳入447例患者。中位随访时间为90个月。2级及以上肠道/膀胱毒性的2年发生率如下:队列1,8.3%/4.2%(95%置信区间2.2%-29.4%/0.6%-26.1%);队列2,8.9%/5.9%(4.1%-18.7%/2.3%-15.0%);队列3,13.2%/2.9%(8.6%-20.2%/1.1%-7.7%);队列4,16.4%/4.8%(9.2%-28.4%/1.6%-14.3%);队列5,12.2%/7.3%(7.6%-19.5%/3.9%-13.6%)。肠道和膀胱毒性的发生率似乎随时间稳定。其他量表也反映了这些结果。全组5年生化/临床无失败率为71%(66%-75%),94%的患者盆腔淋巴结得到控制。
本研究显示了PLN-IMRT的安全性和耐受性。正在进行和计划中的3期研究需要证明,与仅前列腺IMRT相比,使用PLN-IMRT可提高疗效,以抵消肠道副作用的小幅增加。
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