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首页> 外文期刊>International Journal of Radiation Oncology, Biology, Physics >Risk of long-term complications after TFG-beta1-guided very-high-dose thoracic radiotherapy.
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Risk of long-term complications after TFG-beta1-guided very-high-dose thoracic radiotherapy.

机译:TFG-beta1指导的超大剂量胸腔放疗后长期并发症的风险。

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摘要

To report the incidence of late complications in long-term survivors of very-high-dose thoracic radiotherapy (RT) treated on a prospective clinical trial.Patients with locally advanced or medically inoperable non-small-cell lung cancer received three-dimensional conformal RT to the primary tumor and radiographically involved lymph nodes to a dose of 73.6 Gy at 1.6 Gy twice daily. If the plasma transforming growth factor-beta1 (TGF-beta1) level was normal after 73.6 Gy, additional twice-daily RT was delivered to successively higher total doses until the maximal tolerated dose was reached. Patients within a given dose level were followed for 6 months before escalation to the next dose level was permitted. Late complications were defined according to Radiation Therapy Oncology Group/European Organization for Research and Treatment of Cancer criteria.Thirty-eight patients were enrolled between 1996 and 1999. Twenty-four patients were not eligible for radiation dose escalation beyond 73.6 Gy because of persistently abnormal TGF-beta1 levels. Fourteen patients received dose escalation (80 Gy in 8; 86.4 Gy in 6). Grade 3 or greater late complications occurred in 4 of 24, 1 of 8, and 2 of 6 patients treated to 73.6, 80, and 86.4 Gy, respectively. The corresponding patient numbers with late Grade 4-5 toxicity were 3 of 24, 0 of 6, and 0 of 8. Overall, 7 (18%) of the 38 patients developed Grade 3-5 late toxicity. Nonpulmonary complications predominated (4 of 7). Five (71%) of seven serious complications developed within 11 months after RT; however, the remaining two complications (29%) occurred very late (at 43 and 62 months). The 5-year actuarial risk of late Grade 3-5 complications was 33%.Long-term survivors of very-high-dose RT for non-small-cell lung cancer have a significant risk of severe treatment-related complications. At these high dose levels, the predominant toxicity may no longer be pulmonary. All Grade 4-5 complications occurred in patients whose dose was limited to 73.6 Gy because of a persistently elevated TGF-beta1. Thus, persistently elevated plasma TGF-beta1 levels toward the end of RT may identify patients at greatest risk of severe complications.
机译:在前瞻性临床试验中报道超高剂量胸腔放疗(RT)长期幸存者晚期并发症的发生率局部晚期或医学上无法手术的非小细胞肺癌患者接受了三维共形RT每天两次,以1.6 Gy的剂量将原发肿瘤和放射学累及的淋巴结转移至73.6 Gy。如果在73.6 Gy后血浆转化生长因子-β1(TGF-β1)水平正常,则将每天两次的RT依次给药至更高的总剂量,直至达到最大耐受剂量。在给定剂量水平内的患者接受随访6个月,然后才允许升级至下一个剂量水平。根据放射治疗肿瘤学小组/欧洲癌症研究和治疗组织的标准定义了晚期并发症。1996年至1999年间招募了38例患者。由于持续异常,有24例患者不符合超过73.6 Gy的放射剂量升级标准。 TGF-beta1水平。十四名患者接受了剂量递增(8 Gy为80 Gy; 6 Gy为86.4 Gy)。在分别接受73.6、80和86.4 Gy治疗的24名患者中,有24名患者中有4名发生了3级或更高级别的晚期并发症,在8名患者中有2名发生了。相应的具有4-5级晚期毒性的患者人数为24中的3名,6级的0和8级的0。总体上,38例患者中有7名(18%)发展为3-5级晚期毒性。非肺部并发症占主导地位(7/4)。放疗后11个月内发生了7例严重并发症中的5例(占71%);然而,其余两个并发症(29%)发生的时间很晚(分别在43和62个月)。 3-5级晚期并发症的5年精算风险是33%。非小细胞肺癌超高剂量RT的长期幸存者有严重的与治疗相关的并发症的风险。在这些高剂量水平下,主要的毒性可能不再是肺部的。由于TGF-β1持续升高,所有4-5级并发症发生在剂量限于73.6 Gy的患者中。因此,在RT结束时血浆TGF-β1水平持续升高可能会确定患有严重并发症的风险最高的患者。

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