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NARLAL2 剂量递增试验:危及器官分次间变化的剂量学影响。

The NARLAL2 dose escalation trial: dosimetric implications of inter-fractional changes in organs at risk.

机构信息

a Department of Oncology , Aarhus University Hospital , Aarhus C , Denmark.

出版信息

Acta Oncol. 2018 Apr;57(4):473-479. doi: 10.1080/0284186X.2017.1366049. Epub 2017 Aug 23.

Abstract

BACKGROUND

Phase II trials suggested that survival rates for locally advanced lung cancer could be increased by radiotherapy dose escalation. However, results of the phase III RTOG 0617 trial illustrated an imminent risk of treatment-related death. This could be thwarted with strict constraints to organs at risk (OARs) and control of the delivered dose. This study investigates the impact of anatomical changes during radiotherapy on escalated dose distributions used in the Danish NARLAL2 dose escalation trial.

MATERIAL AND METHODS

The phase III NARLAL2 trial randomizes patients between a standard and an escalated treatment plan. In the escalated arm, mean doses up to 95 Gy/33 fractions (tumour) and 74 Gy/33 fractions (lymph nodes) are delivered to the most fluorodeoxyglucose-positron emission tomography (18FDG PET) active regions. The dose distributions are limited by strict constraints to OARs. For a group of 27 patients, a surveillance scan (sCT) was acquired at fraction 11. The original-escalated treatment plans were recalculated on the sCTs and the impact of inter-fractional changes evaluated.

RESULTS

A total of 13 patients (48%) had overdosage of least one OAR. Constraints for the oesophagus, trachea and aorta were violated in 26% of the patients. No overdosage was seen for heart or bronchi. For the connective tissue (all tissue in the mediastinum not identified as OAR or tumour) overdosage was seen in 41% of the patients and for the chest wall in 30% of the patients. The main reason for overdosage was tumour shrinkage.

CONCLUSIONS

Anatomical changes during radiotherapy caused one or more OAR constraint violations for approximately half of the patient cohort. The main cause was tumour shrinkage. For lung cancer radiotherapy dose escalation trials, we recommend incorporation of adaptive radiotherapy strategies.

摘要

背景

Ⅱ期临床试验表明,通过提高放疗剂量可以提高局部晚期肺癌的生存率。然而,Ⅲ期 RTOG 0617 试验的结果表明,存在治疗相关死亡的风险。通过严格限制危及器官(OAR)和控制所给予的剂量,可以避免这种情况。本研究旨在探讨放疗过程中解剖学变化对丹麦 NARLAL2 剂量递增试验中使用的递增剂量分布的影响。

材料和方法

Ⅲ期 NARLAL2 试验将患者随机分为标准治疗组和递增治疗组。在递增组中,高达 95Gy/33 个分次(肿瘤)和 74Gy/33 个分次(淋巴结)的平均剂量被递送至最氟脱氧葡萄糖正电子发射断层扫描(18FDG PET)阳性的区域。剂量分布受到 OAR 严格限制的约束。对 27 例患者中的一组患者在第 11 次分次时进行了监测扫描(sCT)。在 sCT 上重新计算了原始递增治疗计划,并评估了分次间变化的影响。

结果

共有 13 例患者(48%)至少有一个 OAR 出现剂量过高。26%的患者出现食管、气管和主动脉的限制违反。心脏和支气管未见剂量过高。在结缔组织(纵隔中未被确定为 OAR 或肿瘤的所有组织)中,41%的患者出现剂量过高,30%的患者出现胸壁剂量过高。剂量过高的主要原因是肿瘤缩小。

结论

放疗过程中的解剖学变化导致大约一半的患者队列出现一个或多个 OAR 限制违反。主要原因是肿瘤缩小。对于肺癌放疗剂量递增试验,我们建议采用自适应放疗策略。

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