首页> 外文期刊>American Journal of Clinical Oncology: Cancer Clinical Trials >High-dose-rate prostate brachytherapy: an excellent accelerated-hypofractionated treatment for favorable prostate cancer.
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High-dose-rate prostate brachytherapy: an excellent accelerated-hypofractionated treatment for favorable prostate cancer.

机译:高剂量率前列腺癌近距离放射疗法:一种出色的加速次分割疗法,可治疗有利的前列腺癌。

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PURPOSE: The radiobiology of prostate cancer appears to favor large fractions. Accelerated hypofractionation treatments may therefore be used to improve the therapeutic ratio, particularly when the doses to rectum and bladder are kept below the prostate dose. The 5-year experience at William Beaumont Hospital (WBH) and the California Endocurietherapy Center (CET) with accelerated-hypofractionated high-dose-rate (HDR) monotherapy in favorable prostate cancer is presented. MATERIALS AND METHODS: Between 1993 and 2004, 454 patients were treated with brachytherapy of which 248 treated with HDR and 206 patients treated with low-dose-rate Palladium (LDR-Pd(1)(3)). The WBH-HDR dose was 38 Gy, in 4 fractions, twice a day. The CET-HDR dose was 42 Gy in 6 fractions in 2 separate implants 1 week apart. The WBH-LDR dose was 120 Gy. RESULTS: Median follow-up was 4.8 years. The 5-year Phoenix biochemical control (BC) was 89%, 91%, and 88% for WBH-LDR, WBH- HDR, and CET-HDR, respectively. The majority of complications were grade 1. HDR was associated with less acute grade 1 to 3 dysuria 60% versus 39%, (P < 0.001), urinary frequency/urgency 90% to58% (P < 0.001), and rectal pain 17% to 6.5% (P < 0.001). Long-term urinary frequency/urgency 54% versus 43%, (P = 0.03) and dysuria 22% versus 15% were less with HDR. The 5-year actuarial impotence rate was 30% for LDR and 20% for HDR (P = 0.23). CONCLUSIONS: Although the same 5-year BC rates were achieved with HDR (248 patients) and LDR (206 patients) monotherapy, HDR brachytherapy was associated with less acute and chronic genitourinary and gastrointestinal toxicities. As another accepted standard of care, accelerated hypofractionated HDR monotherapy is target specific and efficient radiobiologically than EBRT which has many smaller doses per fraction. It could be considered today as the best option in accelerated hypofractionated prostate cancer treatment.
机译:目的:前列腺癌的放射生物学似乎偏爱大部分。因此,加速降血脂治疗可用于提高治疗率,特别是当直肠和膀胱的剂量保持在前列腺剂量以下时。介绍了在威廉·博蒙特医院(WBH)和加利福尼亚内分泌疗法中心(CET)进行加速降分数高剂量率(HDR)单药治疗有益前列腺癌的5年经验。材料与方法:在1993年至2004年之间,有454例患者接受了近距离放射治疗,其中248例接受HDR治疗,206例接受低剂量率钯(LDR-Pd(1)(3))治疗。 WBH-HDR剂量为38 Gy,分4次,每天两次。 CET-HDR剂量为42 Gy,分为2个独立的植入物,间隔1周分6次。 WBH-LDR剂量为120 Gy。结果:中位随访时间为4.8年。 WBH-LDR,WBH-HDR和CET-HDR的5年Phoenix生化控制(BC)分别为89%,91%和88%。大多数并发症为1级。HDR与较少的1至3级急性尿痛相关,分别为60%和39%(P <0.001),尿频/尿急90%至58%(P <0.001)和直肠疼痛17%至6.5%(P <0.001)。 HDR的长期尿频/尿急症的发生率分别为54%和43%(P = 0.03)和排尿困难22%和15%。 LDR的5年精算阳imp率为30%,HDR为20%(P = 0.23)。结论:尽管HDR(248例)和LDR(206例)的单药治疗达到了相同的5年BC率,但HDR近距离放射治疗与较弱的急性和慢性泌尿生殖道和胃肠道毒性有关。作为另一种公认的护理标准,与EBRT相比,加速次分割HDR单一疗法具有比EBRT更高的靶特异性和放射生物学靶点,而EBRT的每部分剂量要小得多。今天,它被认为是加速超分割前列腺癌治疗的最佳选择。

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