Post-treatment PET/CT for p16-positive oropharynx cancer treated with definitive proton therapy.

IF 1.1 Q3 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

Journal of Clinical Imaging Science Pub Date : 2023-09-29 eCollection Date: 2023-01-01 DOI:10.25259/JCIS_74_2023

Gregory S Alexander, Ariel Eve Pollock, Danielle Arons, Matthew J Ferris, Jason K Molitoris, William F Regine, Matthew E Witek

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引用次数: 0

Abstract

Objectives: Given emerging data suggesting that uncertainty in the relative biologic effectiveness at the distal end of the Bragg peak results in increased mucosal injury in patients with oropharynx cancer receiving adjuvant proton therapy, we evaluated the results of post-treatment positron emission tomography-computed tomography (PET/CT) in patients with p16-positive oropharynx cancer (p16+OPC) treated with definitive intensity-modulated proton therapy (IMPT).

Material and methods: A retrospective cohort study of patients with p16+OPC treated with definitive IMPT between 2016 and 2022 was performed at a single institution. Patients with PET/CT scans within 6 months following completion of IMPT were included in the study. Positive post-treatment scans were defined by a maximum standard uptake values (SUVmax) >4.0 or a <65% reduction in SUVmax in either the primary tumor or lymph node. The Fisher's exact test was used to evaluate factors associated with positive post-treatment PET/ CT values.

Results: Sixty-two patients were included for analysis. Median follow-up was 21 months (range: 3-71 months) with a median time to post-treatment PET/CT of 3 months (range: 2-6 months). Median post-treatment SUVmax of the primary disease and nodal disease was 0 (mean: 0.8, range: 0-7.7) and 0 (mean: 0.7, range: 0-9.5), respectively. Median post-treatment percent reduction in SUVmax for the primary site and lymph node was 100% (mean: 94%, range: 31.3-100%) and 100% (mean: 89%, range: 23-100%), respectively. Eleven patients had a positive post-treatment PET/CT with one biopsy-proven recurrence. Negative and positive predictive values (NPV and PPV) were 98% and 9.1%, respectively. There were no factors associated with positive post-treatment PET/CT.

Conclusion: Similar to patients treated with photon-based radiation therapy, post-treatment PET/CT has a high NPV for patients with p16+OPC treated with definitive proton therapy and should be used to guide patient management. Additional patients and more events are needed to confirm the PPV of a post-treatment PET/CT in this favorable patient cohort.

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p16阳性口咽癌症的治疗后PET/CT经明确质子治疗。

目的：鉴于新出现的数据表明Bragg峰远端相对生物有效性的不确定性导致接受辅助质子治疗的口咽癌症患者的粘膜损伤增加，我们评估了接受明确强度调制质子治疗（IMPT）的p16阳性口咽癌症（p16+OPC）患者的治疗后正电子发射断层扫描计算机断层扫描（PET/CT）结果。材料和方法：2016年至2022年间，在一家机构对接受明确强度调节质子治疗的p16+OPC患者进行了回顾性队列研究。IMPT完成后6个月内进行PET/CT扫描的患者被纳入研究。治疗后阳性扫描由最大标准摄取值（SUVmax）>4.0或a定义。结果：62名患者被纳入分析。中位随访时间为21个月（范围：3-71个月），治疗后PET/CT的中位时间为3个月（时间范围：2-6个月）。原发性疾病和淋巴结疾病的中位治疗后SUVmax分别为0（平均值：0.8，范围：0-7.7）和0（平均数：0.7，范围：0-9.5）。治疗后原发部位和淋巴结SUVmax的中位降低百分比分别为100%（平均：94%，范围：31.3-100%）和100%（平均值：89%，范围：23-100%）。11例患者治疗后PET/CT呈阳性，其中一例活检证实复发。阴性和阳性预测值（NPV和PPV）分别为98%和9.1%。没有与治疗后阳性PET/CT相关的因素。结论：与接受光子放射治疗的患者类似，接受明确质子治疗的p16+OPC患者的治疗后PET/CT具有较高的NPV，应用于指导患者管理。在这个有利的患者队列中，需要更多的患者和更多的事件来确认治疗后PET/CT的PPV。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Clinical Imaging Science RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING-

CiteScore

2.00

自引率

0.00%

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期刊介绍： The Journal of Clinical Imaging Science (JCIS) is an open access peer-reviewed journal committed to publishing high-quality articles in the field of Imaging Science. The journal aims to present Imaging Science and relevant clinical information in an understandable and useful format. The journal is owned and published by the Scientific Scholar. Audience Our audience includes Radiologists, Researchers, Clinicians, medical professionals and students. Review process JCIS has a highly rigorous peer-review process that makes sure that manuscripts are scientifically accurate, relevant, novel and important. Authors disclose all conflicts, affiliations and financial associations such that the published content is not biased.