全脑放射治疗部分留发技术的可行性研究

Narelle Williams, F. Boyle, A. Hong, Hsien Chan, E. Paton, Kerryn Miller, Z. Moutrie, Sinead Mulrennan, Bianca Karle, Gerald B Fobarty
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引用次数: 1

摘要

全脑放疗(WBRT)是一种常见的治疗实体瘤脑转移的姑息性治疗方法。传统上,当有头发的头皮皮肤接受全剂量时,它与相反的外侧野一起给予,导致完全脱发。体积调节电弧疗法(VMAT)可以在对较大转移灶同时进行综合增强(SIB)的同时,将对关键结构(如海马)的剂量降至最低。本可行性研究旨在验证以下假设:使用VMAT保发WBRT方案减少头皮剂量,可在治疗后四周保留头皮毛发并减少脱发,而不影响治疗后三个月的疾病控制。方法:毛发稀疏研究(01.07 WBRTMel子研究SS01.13)是一项由研究者发起的前瞻性可行性研究。制定了VMAT保发WBRT方案,将对头皮的剂量限制在15个分数的16格雷(Gy)。主要目的是通过CTCAE v4和临床医生和患者的感知来测量RT后4周的脱发率。生活质量(QoL)在基线、治疗后1个月和3个月进行评估,使用经过验证的工具,包括欧洲癌症研究和治疗组织(EORTC)生活质量问卷(QLQ-C15-PAL+4)以及与头发有关的四个附加问题,视觉模拟量表(VAS)测量脱发严重程度的感知,以及总化疗引起的脱发困扰量表(CADS)。结果:9例黑色素瘤(6例)、乳腺癌(2例)和肺癌(1例)脑转移患者入组于澳大利亚乌鸦巢的Mater Sydney医院。4周时,5例患者可评估:4例报告中度脱发(CTCAE v4 2级),1例报告轻度脱发(CTCAE v4 1级)。5例患者均佩戴假发或围巾以掩盖脱发。任何程度的脱发都会影响生活质量。与完全脱发相比,通常在常规WBRT中发现的脱发减少并没有转化为生活质量的平均改善。在患者继续研究期间,没有出现症状性颅内疾病进展。两名患者在3个月时进行了MRI检查,均有证据表明,在接受处方WBRT剂量的体积内,疾病发生了颅内进展。从收集的数据来看,VMAT保发WBRT似乎耐受性良好。结论:VMAT保发WBRT在WBRT后4周部分保留了头皮毛发,并且在研究期间不影响症状性疾病控制。治疗肿瘤学家观察到,与传统的WBRT相比,头发长得更快,并且联合细胞毒性化疗对rt诱导的脱发有附加作用。然而,该研究并不是最佳的,因为数据收集受到患者可用性的阻碍。患者群体过于不适,无法按照协议进行随访。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Whole brain radiotherapy with partial hair-sparing technique-a feasibility study
Introduction: Whole brain radiotherapy (WBRT) is a common palliative treatment for brain metastases from solid tumours. Traditionally, it is given with opposed lateral fields causing total alopecia as hair-bearing scalp skin receives the full dose. Volumetric modulated arc therapy (VMAT) can deliver WBRT with a simultaneous integrated boost (SIB) to larger metastases whilst minimising dose to critical structures such as the hippocampus. This feasibility study aimed to test the hypothesis that a reduced dose to the scalp using a VMAT hair-sparing WBRT protocol would spare scalp hair and reduce alopecia at four weeks post treatment without compromising disease control at three months. Methods: The Hair Spare study (01.07 WBRTMel sub-study SS01.13) was an investigator-initiated, prospective feasibility study. A VMAT hair-sparing WBRT protocol was developed to limit the dose to the scalp to 16 Gray (Gy) in 15 fractions. The primary objective was the rate of alopecia at 4 weeks post RT as measured by CTCAE v4 and clinician and patient perception. Quality of life (QoL) was assessed at baseline, one month and three months post treatment with validated instruments including European Organisation for Research and Treatment of Cancer (EORTC) QoL Questionnaire (QLQ-C15-PAL+4) plus four additional questions specifically relating to hair, a visual analogue scale (VAS) to measure the perception of hair loss severity, and the total Chemotherapy-Induced Alopecia Distress Scale (CADS). Results: Nine patients with brain metastases from melanoma (6), breast (2) and lung (1) cancer were enrolled at the Mater Sydney Hospital, Crows Nest, Australia. At 4 weeks, 5 patients were evaluable: 4 reported moderate alopecia (CTCAE v4 Grade 2) and 1 reported mild alopecia (CTCAE v4 Grade 1). All 5 wore wigs or scarves to hide hair loss. Any amount of hair loss impacted QoL. Reduced hair loss compared to complete alopecia, as usually found with conventional WBRT, did not translate to a mean improvement in QoL. There was no symptomatic intracranial progression of disease while the patients remained on study. Two patients had MRI at 3 months, and both had evidence of intracranial progression of disease within the volume that had received prescription WBRT dose. From the data collected it seems that VMAT hair-sparing WBRT was well-tolerated. Conclusion: VMAT hair-sparing WBRT partially spared scalp hair at four weeks post WBRT and did not compromise symptomatic disease control during the study. The treating oncologists observed that the hair grew back quicker than with conventional WBRT, and that combined cytotoxic chemotherapy was additive to RT-induced alopecia. However, the study was not optimal in that data collection was hampered by patient availability. The patient population was too unwell to be followed up according to the protocol.
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