Levendag P C, Schmitz P I, Jansen P P, Senan S, Eijkenboom W M, Sipkema D, Meeuwis C A, Kolkman-Deurloo I K, Visser A G
Department of Radiation Oncology, Dr. Daniel den Hoed Cancer Center/University Hospital Rotterdam-Dijkzigt, The Netherlands.
Int J Radiat Oncol Biol Phys. 1997 Jun 1;38(3):497-506. doi: 10.1016/s0360-3016(97)00046-1.
Fractionated high-dose-rate (fr.HDR) and pulsed-dose-rate (PDR) brachytherapy (BT) regimens, which simulate classical continuous low-dose-rate (LDR) interstitial radiation therapy (IRT) schedules, have been developed for clinical use. This article reports the initial results using these novel schedules in squamous cell carcinoma (SCC) of the tonsillar fossa (TF) and/or soft palate (SP).
Between 1990 and 1994, 38 patients with TF and SP tumors (5 T1, 22 T2, 10 T3, and 1 T4) were treated by fr.HDR or PDR brachytherapy, either alone or in combination with external irradiation (ERT). Half of the patients were treated with fr.HDR, which entailed twice-daily fractions of > or = 3 Gy. The other 19 patients were administered PDR, which consisted of pulses of < or = 2 Gy delivered 4-8 times/day. The median cumulative dose of IRT +/- ERT series was 66 Gy (range 55-73). The results in these patients treated by brachytherapy were compared to 72 patients with similar tumors treated in our institute with curative intent, using ERT alone. The median cumulative dose of ERT-only series was 70 Gy (range 40-77).
Excellent locoregional control was achieved with the use of IRT +/- ERT, with only 13% (5 of 38) developing local failure, and salvage surgery being possible in three of the latter (60%). Neither BT scheme (fr.HDR vs. PDR) nor tumor site (TF vs. SP) significantly influenced local control rates. The type and severity of the side effects observed are comparable to those reported in the literature for LDR-IRT. These results contrast sharply with our ERT-only series, in which 39% of patients (28 of 72) developed local failure, with surgical salvage being possible only in three patients (11%). Taking the data set of 110 patients, in a univariate analysis IRT, T stage, N stage, overall treatment time (OTT), and BEDcor10 (biological effective dose with a correction for the OTT) were significant prognostic factors for local relapse-free survival (LRFS) and overall survival (OS) at 3 years. Using Cox proportional hazard analysis, only T stage and BEDcor10 remained significant for LRFS (p < 0.001 and 0.008, respectively), as well as for OS (p < 0.001 and 0.003, respectively). With regard to the current (IRT) and historical (ERT) series, for the LRFS at 3 years, dose-response relationships were established, significant, however, only for the BEDcor10 (p = 0.03).
The 3-year LRFS of approximately 90% for TF and SP tumors reported here is comparable with the best results in the literature, particularly given the fact that 30% of the patients (11 of 38) presented with T3/4 tumors. When compared with our historical (ERT-only) controls, the patients treated with IRT had superior local control. A dose-response relationship was established for the BEDcor10.
已开发出分次高剂量率(fr.HDR)和脉冲剂量率(PDR)近距离放射治疗(BT)方案,用于模拟经典的连续低剂量率(LDR)组织间放射治疗(IRT)方案,以供临床使用。本文报告了在扁桃体窝(TF)和/或软腭(SP)鳞状细胞癌(SCC)中使用这些新方案的初步结果。
1990年至1994年间,38例TF和SP肿瘤患者(5例T1、22例T2、10例T3和1例T4)接受了fr.HDR或PDR近距离放射治疗,单独使用或与外照射(ERT)联合使用。一半患者接受fr.HDR治疗,即每天两次,每次剂量≥3 Gy。另外19例患者接受PDR治疗,即每天4 - 8次,每次剂量≤2 Gy。IRT±ERT系列的中位累积剂量为66 Gy(范围55 - 73)。将这些接受近距离放射治疗的患者的结果与我院72例有治愈意向、仅接受ERT治疗的类似肿瘤患者的结果进行比较。仅接受ERT系列的中位累积剂量为70 Gy(范围40 - 77)。
使用IRT±ERT实现了出色的局部区域控制,仅13%(38例中的5例)出现局部失败,其中3例(60%)可行挽救性手术。两种BT方案(fr.HDR与PDR)以及肿瘤部位(TF与SP)均未对局部控制率产生显著影响。观察到的副作用类型和严重程度与文献中报道的LDR - IRT的情况相当。这些结果与我们仅接受ERT的系列形成鲜明对比,在该系列中,39%的患者(72例中的28例)出现局部失败,仅3例患者(11%)可行手术挽救。在对110例患者的数据集进行单因素分析时,IRT、T分期、N分期、总治疗时间(OTT)以及BEDcor10(校正OTT后的生物等效剂量)是3年局部无复发生存率(LRFS)和总生存率(OS)的显著预后因素。使用Cox比例风险分析,仅T分期和BEDcor10对LRFS仍具有显著性(分别为p < 0.001和0.008),对OS也具有显著性(分别为p < 0.001和0.003)。关于当前(IRT)和历史(ERT)系列,对于3年的LRFS,建立了剂量反应关系,但仅BEDcor10具有显著性(p = 0.03)。
本文报道的TF和SP肿瘤3年LRFS约为90%,与文献中的最佳结果相当,特别是考虑到30%的患者(38例中的11例)为T3/4期肿瘤。与我们的历史(仅ERT)对照组相比,接受IRT治疗的患者具有更好的局部控制。为BEDcor10建立了剂量反应关系。
