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一项针对永久性前列腺近距离放射治疗患者的病例对照研究中生化结果的详细放射生物学和剂量学分析。

A detailed radiobiological and dosimetric analysis of biochemical outcomes in a case-control study of permanent prostate brachytherapy patients.

作者信息

Butler Wayne M, Stewart Renee R, Merrick Gregory S

机构信息

Schiffier Cancer Center, Wheeling Hospital, 1 Medical Park, Wheeling, West Virginia 26003-6300, USA.

出版信息

Med Phys. 2009 Mar;36(3):776-87. doi: 10.1118/1.3077161.

Abstract

The purpose of this study is to determine dosimetric and radiobiological predictors of biochemical control after recalculation of prostate implant dosimetry using updated AAPM Task Group 43 (TG-43) parameters and the radiobiological parameters recommended by TG-137. All biochemical failures among patients implanted with 125I Or 103Pd sources between 1994 and March 2006 were matched 2:1 with nonfailure controls. The individual matching was by risk group, radionuclide, prescribed dose, and time of implant (one match before and one after the failed patient) resulting in a median follow-up of 10.9 years. Complete dose volume histogram (DVH) data were recalculated for all 55 cases and 110 controls after updating the original source strength by the retrospectively determined ratios of TG-43. Differential DVH data were acquired in 179 increments of prostate volume versus percentage prescribed dose. At each incremental dose level i, the biologically equivalent dose BEDi, equivalent uniform dose EUDi, and tumor control probability TCPi were calculated from the implant dose plus any external beam delivered to the patient. Total BED, EUD, and TCP were then derived from the incremental values for comparison with single point dosimetric quality parameters and DVH-based averages. There was no significant difference between failures and controls in terms of total BED (143 vs 142 Gy), EUD (95 vs 94 Gy), or TCP (0.87 vs 0.89). Conditional logistic regression analysis factored out the matching variables and stratified the cohort into each case and its controls, but no radiobiological parameter was predictive of biochemical failure. However, there was a significant difference between radiobiological parameters of 125I and 103Pd due to less complete coverage of the target volume by the former isotope. The implant BED and TCP were highly correlated with the D90 and natural prescription doses and a series of mean DVH-based doses such as the harmonic mean and expressions of the generalized EUD. In this case-control study of prostate brachytherapy biochemical failures and nonfailures, there were no radiobiological parameters derived from detailed DVH-based analysis that predicted for biochemical control. This may indicate that in our approach, implant dosimetry is at or near the limits of clinically effective dose escalation.

摘要

本研究的目的是,使用更新后的美国医学物理师协会任务组43(TG-43)参数以及TG-137推荐的放射生物学参数,重新计算前列腺植入剂量测定后,确定生化控制的剂量测定和放射生物学预测指标。1994年至2006年3月期间植入125I或103Pd源的患者中所有生化失败病例与无失败对照按2:1进行匹配。个体匹配依据风险组、放射性核素、规定剂量和植入时间(失败患者之前和之后各匹配一例),中位随访时间为10.9年。在根据回顾性确定的TG-43比率更新原始源强度后,对所有55例病例和110例对照重新计算了完整的剂量体积直方图(DVH)数据。以前列腺体积与规定剂量百分比的179个增量获取差异DVH数据。在每个增量剂量水平i,根据植入剂量加上给予患者的任何外照射剂量计算生物学等效剂量BEDi、等效均匀剂量EUDi和肿瘤控制概率TCPi。然后从增量值得出总BED、EUD和TCP,以便与单点剂量测定质量参数和基于DVH的平均值进行比较。在总BED(143对142 Gy)、EUD(95对94 Gy)或TCP(0.87对0.89)方面,失败组与对照组之间无显著差异。条件逻辑回归分析排除了匹配变量,并将队列分层为每个病例及其对照,但没有放射生物学参数可预测生化失败。然而,由于125I对靶区体积的覆盖不如103Pd完全,二者的放射生物学参数存在显著差异。植入BED和TCP与D90、自然处方剂量以及一系列基于DVH平均值的剂量(如调和平均值和广义EUD表达式)高度相关。在这项前列腺近距离治疗生化失败与未失败的病例对照研究中,基于详细DVH分析得出的放射生物学参数均无法预测生化控制情况。这可能表明,在我们的方法中,植入剂量测定已达到或接近临床有效剂量递增的极限。

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