首页> 外文期刊>Frontiers in Oncology >Combined Long-Term Androgen Deprivation and Pelvic Radiotherapy in the Post-operative Management of Pathologically Defined High-Risk Prostate Cancer Patients: Results of the Prospective Phase II McGill 0913 Study
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Combined Long-Term Androgen Deprivation and Pelvic Radiotherapy in the Post-operative Management of Pathologically Defined High-Risk Prostate Cancer Patients: Results of the Prospective Phase II McGill 0913 Study

机译:组合长期雄激素剥夺和骨盆放疗在病理定义的高风险前列腺癌症患者的术后管理中:预期阶段的结果II麦吉尔0913研究

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Purpose: Following radical prostatectomy, prostate bed radiotherapy (PBRT) has been combined with either long-term androgen deprivation therapy (LT-ADT) or short-term ADT with pelvic lymph node radiotherapy (PLNRT) to provide an oncological benefit in randomized trials. McGill 0913 was designed to characterize the efficacy of combining PBRT, PLNRT, and LT-ADT. It is the first study to do so prospectively. Methods: In a single arm phase II trial conduced from 2010 to 2016, 46 post-prostatectomy prostate cancer patients at a high-risk for relapse (pathological Gleason 8+ or T3) were assessed for treatment with combined LT-ADT (24 months), PBRT, and PLNRT. Patients received PLNRT and PBRT (44 Gy in 22 fractions) followed by a PBRT boost (22 Gy in 11 fractions). The primary endpoint was progression-free survival (PFS). Toxicity and quality of life (QoL) were evaluated using CTCAE V3.0 and EQ-5D-3L questionnaires, respectively. Results: Among the 43 patients were treated as per protocol, median PSA was 0.30 μg/L. On surgical pathology, 51% had positive margins, 40% had Gleason 8+ disease, 42% had seminal vesicle involvement, and 19% had lymph node involvement. At a median follow-up of 5.2 years, there were no deaths or clinical progression. At 5 years, PFS was 78.0% (95% Confidence Interval 63.7–95.5%). Not including erectile dysfunction, patients experienced: 14% grade 2 endocrine toxicity while on ADT, one incident of long-term gynecomastia, 5% grade 2 acute urinary toxicity, 5% grade 2 late Urinary toxicity, and 24% long-term hypogonadism. No comparison between the average or minimum self-reported QoL at baseline, during ADT, nor after ADT demonstrated a statistically significant difference. Conclusions: Combining PBRT, PLNRT, and LT-ADT had an acceptable PFS in patients with significant post-operative risk factors for recurrence. While therapy was well-tolerated, long-term hypogonadism was a substantial risk. Further investigations are needed to determine if this combination is beneficial. Trial registration: NCT01255891.
机译:目的:遵循自由基前列腺切除术,前列腺床放射疗法(PBRT)与长期雄激素剥夺治疗(LT-ADT)或短期ADT与盆腔淋巴结放射疗法(PLNRT)组合,以提供随机试验中的肿瘤效益。 McGill 0913旨在表征组合PBRT,PLNRT和LT-ADT的疗效。这是第一次进行这么前瞻性的研究。方法:在2010年至2016年的单一ARM期II试验中,评估了46例前列腺切除术前列腺癌患者,以较高的复发(病理肠胃胺8+或T3)进行评估,用于用综合(24个月)治疗,pbrt和plnrt。患者接受PLNRT和PBRT(22个级分中的44 GY),然后是PBRT升压(11分数中的22μm)。主要终点是无进展的存活率(PFS)。使用CTCAE V3.0和EQ-5D-3L问卷评估毒性和寿命质量(QOL)。结果:43例患者在议定方案治疗中,中位数PSA为0.30μg/升。在手术病理学上,51%具有阳性边距,40%有Glason 8+疾病,42%具有雄性囊泡的参与,19%有淋巴结参与。在5.2年的中位随访,没有死亡或临床进展。 5年来,PFS为78.0%(95%置信区间63.7-95.5%)。不含勃起功能障碍,经历了勃起功能障碍:14%级内分泌毒性,同时在ADT上,一道长期的膀胱肿瘤,5%急性尿毒毒性,5%患者晚期泌尿毒性,24%的长期性低因素。在ADT期间,基线的平均值或最小自我报告的QoL之间没有比较,ADT在ADT之后表现出统计学显着差异。结论:组合PBRT,PLNRT和LT-ADT在患有显着的患者危险因素的患者中具有可接受的PFS。虽然治疗耐受良好,但长期的性腺性腺是大量风险。需要进一步调查来确定这种组合是否有益。试验注册:NCT01255891。

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