立体定向体质子治疗高危肺肿瘤的安全性和有效性。

IF 0.7 Q4 SURGERY Journal of radiosurgery and SBRT Pub Date : 2023-01-01
Matthew T McMillan, Annemarie F Shepherd, Minglei Kang, Liyong Lin, Narek Shaverdian, Abraham J Wu, Daphna Y Gelblum, Nitin Ohri, Stanislav Lazarev, Lee Xu, Arpit M Chhabra, Shaakir Hasan, J Isabelle Choi, Daniel R Gomez, Andreas Rimner, Haibo Lin, Charles B Simone
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引用次数: 0

摘要

目的:立体定向体质子治疗(SBPT)是一种新兴的肺肿瘤治疗策略,旨在将超低分割的优异局部控制优势与质子的物理优势相结合,与光子相比,质子可以减少危及器官(OARs)的积分剂量。然而,迄今为止,很少有数据报道将SBPT分5个或更少的部分用于肺肿瘤。鉴于光子立体定向体放射治疗在遵守OAR剂量限制的情况下难以向高风险肿瘤(即中心/超中心位置、既往野放射、肿瘤大小> 5cm或存在严重肺部合并症)提供消融剂量,我们假设SBPT将是高风险肿瘤患者的有效替代方案。方法和材料:回顾性分析2019年12月至2022年11月在纽约质子中心接受SBPT治疗的29例高危肺癌患者27例。患者被分为三个主要亚组:早期非小细胞肺癌(NSCLC)、局部复发性NSCLC和肺癌或其他组织学的转移性肺癌。使用描述性统计报告患者特征,使用精算方法量化疾病控制率,使用CTCAE v 5.0对毒性进行评分。结果:SBPT最常见的高危指征为肿瘤中心/超中心位置(69.0%)、严重COPD(48.1%)、再照射(44.4%)、显著肺纤维化(22.2%)和肿瘤大小> 5 cm(18.5%)。总的来说,96.6%的肿瘤被处方剂量完全覆盖,而不影响目标覆盖。早期NSCLC、局部复发NSCLC和转移性NSCLC的三年精算率分别为89%、100%和43%。区域控制的三年精算率分别为89%、67%和86%。无远处转移的三年精算生存率分别为79%、100%和0%。2例患者(7.4%)均有临床显著的基线间质性肺疾病和治疗前持续需氧,出现≥2级肺毒性(1例为3级,1例为5级)。没有与食管炎、心脏损伤、气道损伤、肺纤维化、支气管肺出血或臂丛病相关的急性或晚期≥2级毒性。结论:在迄今为止报道的最大规模的质子SBRT研究中,SBPT具有良好的毒性特征,同时是治疗大多数高危肿瘤的有效方法,不需要降低剂量或损害肿瘤覆盖范围,值得进一步研究。
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Safety and efficacy of stereotactic body proton therapy for high-risk lung tumors.

Purpose: Stereotactic body proton therapy (SBPT) is an emerging treatment strategy for lung tumors that aims to combine the excellent local control benefits of ultra-hypofractionation with the physical advantages of protons, which reduce the integral dose to organs at risk (OARs) compared to photons. To date, however, very little data delivering SBPT in 5 or fewer fractions to lung tumors have been reported. Given that photon stereotactic body radiation therapy can struggle to deliver ablative doses to high-risk tumors (i.e., central/ultra-central location, prior in-field radiation, tumor size >5 cm, or the presence of severe pulmonary comorbidities) while adhering to OAR dose constraints, we hypothesized that SBPT would be an effective alternative for patients with high-risk tumors.

Methods and materials: Twenty-seven high-risk patients with 29 lung tumors treated with SBPT at the New York Proton Center between December 2019 and November 2022 were retrospectively identified. Patients were divided into three major subgroups: early-stage non-small cell lung cancer (NSCLC), locally recurrent NSCLC, and metastatic cancer from lung cancer or other histologies. Patient characteristics were reported using descriptive statistics, actuarial methods were used to quantify disease control rates, and toxicities were scored using CTCAE v 5.0.

Results: The most common high-risk indications for SBPT were central/ultra-central tumor location (69.0%), severe COPD (48.1%), reirradiation (44.4%), significant pulmonary fibrosis (22.2%), and large tumor size > 5 cm (18.5%). In total, 96.6% of tumors were fully covered by the prescription dose without compromising target coverage. Three-year actuarial rates of local control for early-stage NSCLC, locally recurrent NSCLC, and metastatic patients were 89%, 100%, and 43%, respectively. Three-year actuarial rates of regional control were 89%, 67%, and 86%. Three-year actuarial rates of distant metastasis-free survival were 79%, 100%, and 0%. Two patients (7.4%), both of whom had clinically significant baseline interstitial lung disease and pre-treatment continuous oxygen demand, experienced grade ≥2 pulmonary toxicity (1 grade 3, 1 grade 5). There were no acute or late grade ≥2 toxicities related to esophagitis, cardiac injury, airway injury, pulmonary fibrosis, bronchopulmonary hemorrhage or brachial plexopathy.

Conclusions: In the largest study of proton SBRT reported to date, SBPT has a favorable toxicity profile while being an effective approach for treating most high-risk tumors without requiring dose de-escalation or compromising tumor coverage and warrants further investigation.

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