Timing of Radiation Pneumonitis in Patients with Stage 3 Non-Small-Cell Lung Cancer Receiving Consolidation Durvalumab after Chemoradiation

IF 1.8 4区医学 Q3 HEALTH CARE SCIENCES & SERVICES European Journal of Cancer Care Pub Date : 2024-04-27 DOI:10.1155/2024/5886423

Melinda Mushonga, Alexander Louie, Susanna Cheng, May N. Tsao, Wee Loon Ong, Patrick Cheung, Ian Poon, L. Zhang, Yee C. Ung

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Abstract

Purpose. Consolidation with durvalumab is standard of care in the management of unresectable stage 3 non-small-cell lung cancer (NSCLC) postchemoradiation, and pneumonitis is an independent potential treatment complication of both treatment strategies. This study seeks to determine the timing of radiation pneumonitis (RP) by receipt of durvalumab. In addition, we reviewed the preventative strategies guided by pathophysiology of pneumonitis. Methods. We identified patients with unresectable Stage 3 NSCLC who developed grade ≥2 RP after chemoradiotherapy. Time-to-RP was defined from date of completion of radiotherapy to date of radiological diagnosis of RP and accompanying clinical symptoms. Early RP was defined as RP within 2 months of completion of radiotherapy. Differences in time-to-RP by receipt of durvalumab were evaluated using Wilcoxon rank-sum test. Differences in those who had early vs late RP by receipt of durvalumab was evaluated using Fisher’s exact test. Logistic regression was used to evaluate patient and treatment factors associated with early RP. Results. Of the 144 patients with Stage 3 NSCLC who had definitive chemoradiotherapy, 31 (22%) developed grade ≥2 RP and were included in the study. There was one patient with grade 5 RP. The median age of the cohort was 67 years (range 41–87). The mean lung dose, V5Gy, and V20Gy were 15.8Gy (SD = 1.56), 60.14% (SD 2.73), and 29.96% (SD 1.82), respectively. Twelve (39%) patients received durvalumab. The median time-to-RP was 3.4 months (range: 1.7–7.2) and 2.3 months (range: 0.6–9.6) in patients who had durvalumab and no durvalumab, respectively (P = 0.01). 83% (10/12) of patients who had durvalumab and 58% (11/19) of patients who did not have durvalumab had late RP (P = 0.14). No other patient and treatment factors were associated with early RP. Conclusion. Patients on durvalumab may have late-onset RP; therefore, further studies with larger cohort of patients and development of new predictive models that incorporate evolving management are needed should preventative strategies of RP be considered in routine clinical practice.

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化疗后接受 Durvalumab 巩固治疗的 3 期非小细胞肺癌患者发生放射性肺炎的时间安排

研究目的在治疗化疗后不可切除的3期非小细胞肺癌（NSCLC）时，使用杜伐单抗进行巩固治疗是标准疗法，而肺炎是这两种治疗策略的独立潜在并发症。本研究旨在确定接受杜伐单抗治疗后出现放射性肺炎（RP）的时间。此外，我们还回顾了以肺炎病理生理学为指导的预防策略。方法我们确定了化疗后出现≥2级RP的不可切除的3期NSCLC患者。RP发生时间的定义是从放疗结束之日到RP经放射学诊断并伴有临床症状之日。早期RP定义为放疗结束后2个月内的RP。使用Wilcoxon秩和检验评估接受度伐卢单抗后RP发生时间的差异。使用费舍尔精确检验评估了接受德伐卢单抗后早期与晚期RP患者的差异。采用 Logistic 回归评估与早期 RP 相关的患者和治疗因素。结果。在144名接受了明确放化疗的3期NSCLC患者中，有31人（22%）出现了≥2级RP，并被纳入研究。有一名患者出现了 5 级 RP。组群的中位年龄为67岁（41-87岁）。平均肺剂量、V5Gy 和 V20Gy 分别为 15.8Gy (SD = 1.56)、60.14% (SD 2.73) 和 29.96% (SD 1.82)。12名患者（39%）接受了杜伐单抗治疗。使用德伐卢单抗和未使用德伐卢单抗患者的中位复发时间分别为 3.4 个月（范围：1.7-7.2）和 2.3 个月（范围：0.6-9.6）（P = 0.01）。83%（10/12）接受过度伐卢单抗治疗的患者和58%（11/19）未接受过度伐卢单抗治疗的患者出现了晚期RP（P = 0.14）。其他患者和治疗因素均与早期 RP 无关。结论。使用度伐卢单抗的患者可能会出现晚发RP；因此，如果常规临床实践中考虑采用RP预防策略，则需要对更大的患者群进行进一步研究，并开发新的预测模型，将不断变化的管理纳入其中。

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

European Journal of Cancer Care 医学-康复医学

CiteScore

4.00

自引率

4.80%

发文量

213

审稿时长

3 months

期刊介绍： The European Journal of Cancer Care aims to encourage comprehensive, multiprofessional cancer care across Europe and internationally. It publishes original research reports, literature reviews, guest editorials, letters to the Editor and special features on current issues affecting the care of cancer patients. The Editor welcomes contributions which result from team working or collaboration between different health and social care providers, service users, patient groups and the voluntary sector in the areas of: - Primary, secondary and tertiary care for cancer patients - Multidisciplinary and service-user involvement in cancer care - Rehabilitation, supportive, palliative and end of life care for cancer patients - Policy, service development and healthcare evaluation in cancer care - Psychosocial interventions for patients and family members - International perspectives on cancer care