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将生物学因素纳入放射性肝病平行结构正常组织并发症概率模型。

Inclusion of biological factors in parallel-architecture normal-tissue complication probability model for radiation-induced liver disease.

作者信息

Cheng Jason Chia-Hsien, Liu Hua-Shan, Wu Jian-Kuen, Chung Hsiao-Wen, Jan Gwo-Jen

机构信息

Department of Electrical Engineering, National Taiwan University, No. 1 Sec. 4 Roosevelt Road, Taipei 106, Taiwan.

出版信息

Int J Radiat Oncol Biol Phys. 2005 Jul 15;62(4):1150-6. doi: 10.1016/j.ijrobp.2004.12.031.

Abstract

PURPOSE

To include biologic factors in parallel-architecture normal-tissue complication probability (NTCP) model for radiation-induced liver disease (RILD) after three-dimensional conformal radiotherapy (3D-CRT) for gastric or hepatic cancer.

METHODS AND MATERIALS

A total of 151 patients (89 with hepatocellular carcinoma and 62 with gastric cancer) who received 3D-CRT to the liver were included (isocenter dose range 33.0 to 66.0 Gy; mean 48.0 Gy). RILD was defined as grade 3 or higher liver toxicity according to Common Toxicity Criteria Version 2.0 of the National Cancer Institute within 4 months after 3D-CRT. Possible correlations of patient-related or dosimetric factors with RILD were tested. Maximum-likelihood analysis estimated NTCP model parameters for group and subgroups. Goodness-of-fit analysis estimated deviance of NTCP model parameters between subgroups.

RESULTS

RILD developed in 25 patients. Hepatitis B virus carrier status (p < 0.001) was the only significant independent factor. The 4 parallel NTCP model parameters, mean functional reserve (V(50)), width of functional reserve distribution (sigma), dose damage to 50% of liver subunits (D(50)), and slope parameter for subunit dose-response (k), were respectively, 0.54, 0.14, 50 Gy, 0.18 (group); 0.53, 0.07, 50 Gy, 4.6 x 10(-7) (carriers); 0.59, 0.12, 25 Gy, 59.8 (noncarriers). In carrier-state subgroups, goodness-of-fit deviance with 1 subgroup's parameter set would have been worse in the other group. Across subgroups, patients with RILD all had liver fraction damage (f) greater than 0.4 compared with wider distribution for the whole group.

CONCLUSIONS

RILD is described with a parallel-architecture NTCP model for HBV carriers and noncarriers with a threshold effect greater than 0.4. The main difference is in slope parameter for subunit dose-response.

摘要

目的

将生物学因素纳入用于胃癌或肝癌三维适形放疗(3D-CRT)后放射性肝病(RILD)的平行结构正常组织并发症概率(NTCP)模型。

方法和材料

纳入151例接受肝脏3D-CRT的患者(89例肝细胞癌患者和62例胃癌患者)(等中心剂量范围33.0至66.0 Gy;平均48.0 Gy)。根据美国国立癌症研究所《通用毒性标准》第2.0版,将RILD定义为3D-CRT后4个月内3级或更高等级的肝毒性。测试了患者相关因素或剂量学因素与RILD的可能相关性。最大似然分析估计了组和亚组的NTCP模型参数。拟合优度分析估计了亚组之间NTCP模型参数的偏差。

结果

25例患者发生RILD。乙肝病毒携带者状态(p < 0.001)是唯一显著的独立因素。4个平行的NTCP模型参数,平均功能储备(V(50))、功能储备分布宽度(sigma)、50%肝脏亚单位的剂量损伤(D(50))以及亚单位剂量反应的斜率参数(k),分别为0.54、0.14、50 Gy、0.18(组);0.53、0.07、50 Gy、4.6×10(-7)(携带者);0.59、0.12、25 Gy、59.8(非携带者)。在携带者状态亚组中,使用一个亚组的参数集时,另一组的拟合优度偏差会更差。在所有亚组中,与整个组更广泛的分布相比,发生RILD的患者肝脏部分损伤(f)均大于0.4。

结论

对于乙肝病毒携带者和非携带者,RILD可通过具有大于0.4的阈值效应的平行结构NTCP模型来描述。主要差异在于亚单位剂量反应的斜率参数。

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