The interplay between acute and late toxicity among patients receiving prostate radiotherapy: an individual patient data meta-analysis of six randomised trials

The Lancet Oncology Pub Date : 2025-01-30 DOI:10.1016/s1470-2045(24)00720-4

John Nikitas, Parsa Jamshidian, Alison C Tree, Emma Hall, David Dearnaley, Jeff M Michalski, W Robert Lee, Paul L Nguyen, Howard M Sandler, Charles N Catton, Himanshu R Lukka, Luca Incrocci, Wilma Heemsbergen, Floris J Pos, Soumyajit Roy, Shawn Malone, Eric Horwitz, Jessica Karen Wong, Stefano Arcangeli, Giuseppe Sanguineti, Amar U Kishan

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引用次数: 0

Abstract

Background

The association between acute and late toxicity following prostate radiotherapy has not been well studied using data from multiple randomised clinical trials and fractionation schedules. We aimed to characterise the relationship between acute and late genitourinary and gastrointestinal toxicity among patients receiving conventionally fractionated or moderately hypofractionated prostate radiotherapy.

Methods

This was an individual patient data meta-analysis that identified randomised phase 3 trials of conventionally fractionated or moderately hypofractionated prostate radiotherapy in the Meta-Analysis of Randomized trials in Cancer of the Prostate (MARCAP) Consortium that had individual-level acute and late toxicity data available and were available before Dec 1, 2023. Trials without individual patient data were excluded. Data were provided to MARCAP by study investigators. The associations between acute (≤3 months after radiotherapy) and late (>3 months after radiotherapy) grade 2 or greater genitourinary and gastrointestinal toxicities were assessed using adjusted generalised linear mixed models (adjusted for age, androgen deprivation therapy status, type of radiotherapy, radiation dose, and radiation schedule). In the subset of trials that collected Expanded Prostate Cancer Index Composite quality of life (QOL) evaluations, the association between acute genitourinary and gastrointestinal toxicity and decrements at least twice the minimal clinically important difference (MCID) for urinary and bowel QOL were also evaluated.

Findings

Six of 26 available trials met all the eligibility criteria. 6593 patients were included (conventionally fractionated: n=4248; moderately hypofractionated: n=2345). Median follow-up was 72 months (IQR 61–94). Acute grade 2 or greater genitourinary toxicity was associated with both late grade 2 or greater genitourinary toxicity (odds ratio 2·20 [95% CI 1·88–2·57], p<0·0001) and decrement at least twice the MCID in urinary QOL (1·41 [1·17–1·68], p=0·0002). Acute grade 2 or greater gastrointestinal toxicity was associated with both late grade 2 or greater gastrointestinal toxicity (2·53 [2·07–3·08], p<0·0001) and decrement at least twice the MCID in bowel QOL (1·52 [1·26–1·83], p<0·0001).

Interpretation

Acute toxicity following prostate radiotherapy was statistically significantly associated with late toxicity and with decrement in patient-reported QOL metrics. These data support efforts to evaluate whether interventions that reduce acute toxicity ultimately reduce the risk of late toxicity.

Funding

National Institutes of Health and US Department of Defense.

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接受前列腺放疗的患者急性和晚期毒性之间的相互作用：六项随机试验的个体患者数据荟萃分析

背景：前列腺放射治疗后急性毒性和晚期毒性之间的关系尚未通过多个随机临床试验和分级计划的数据得到很好的研究。我们的目的是描述急性和晚期泌尿生殖系统和胃肠道毒性在接受常规分次或中度低分次前列腺放疗的患者之间的关系。方法：这是一项个体患者数据荟萃分析，在前列腺癌（MARCAP）协会随机试验荟萃分析中确定了常规分割或中度低分割前列腺放疗的随机3期试验，这些试验具有个体水平的急性和晚期毒性数据，并且可在2023年12月1日之前获得。没有个体患者资料的试验被排除在外。研究人员向MARCAP提供了数据。使用调整后的广义线性混合模型（根据年龄、雄激素剥夺治疗状态、放疗类型、放疗剂量和放疗计划进行调整）评估急性（放疗后≤3个月）和晚期（放疗后>；3个月）2级或以上泌尿生殖系统和胃肠道毒性之间的关联。在收集扩展前列腺癌指数综合生活质量（QOL）评估的试验子集中，还评估了急性泌尿生殖系统和胃肠道毒性与泌尿和肠道生活质量最小临床重要差异（MCID）至少两倍的下降之间的关系。结果26项试验中有6项符合所有入选标准。6593例患者被纳入(按常规分类：n=4248；中度低分割：n=2345)。中位随访时间为72个月（IQR 61-94）。急性2级或更严重的泌尿生殖系统毒性与晚期2级或更严重的泌尿生殖系统毒性相关（比值比为2.20 [95% CI 1.88 - 2.57], p= 0.0001），且尿质量中MCID的下降至少为前者的两倍（比值比为1.41 [1.17 - 1.68],p= 0.0002）。急性2级或更大的胃肠道毒性与晚期2级或更大的胃肠道毒性（2.53 [2.07 - 3.08],p< 0.0001）和至少两倍于肠道QOL的MCID （1.52 [1.26 - 1.83], p< 0.0001）相关。前列腺放射治疗后的急性毒性与晚期毒性和患者报告的生活质量指标的下降有统计学意义。这些数据支持评估降低急性毒性的干预措施是否最终降低晚期毒性的风险。资助国家卫生研究院和美国国防部。

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The Lancet Oncology

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