Symptomatic Pneumonitis With Durvalumab After Concurrent Chemoradiotherapy in Unresectable Stage III NSCLC

Johan F. Vansteenkiste MD, PhD , Jarushka Naidoo MB, BCH, MHS , Corinne Faivre-Finn MD, PhD , Mustafa Özgüroğlu MD , Augusto Villegas MD , Davey Daniel MD , Shuji Murakami MD , Rina Hui M.B.B.S., PhD , Ki Hyeong Lee MD , Byoung Chul Cho MD, PhD , Kaoru Kubota MD, PhD , Helen Broadhurst MSc , Catherine Wadsworth BVSc , Michael Newton PharmD , Piruntha Thiyagarajah MD , Scott J. Antonia MD
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Abstract

Introduction

In the placebo-controlled, phase 3 PACIFIC trial, durvalumab significantly prolonged progression-free survival (PFS) (p < 0.0001) and overall survival (OS) (p = 0.00251) in patients with unresectable stage III NSCLC and no progression after platinum-based concurrent chemoradiotherapy (cCRT). Pneumonitis or radiation pneumonitis (PRP) was common in both arms. We report exploratory analyses evaluating the association of symptomatic (grade ≥2) PRP (G2+PRP) with baseline factors and clinical outcomes.

Methods

Patients with WHO performance status of 0 or 1 were randomized (2:1) to 12 months of durvalumab or placebo, 1 to 42 days after cCRT. Associations between baseline factors and on-study G2+PRP in durvalumab-treated patients were investigated using univariate and multivariate logistic regression. PFS and OS were analyzed using Cox proportional hazards models adjusted for time-dependent G2+PRP plus covariates for randomization stratification factors without and with additional baseline factors.

Results

On-study G2+PRP occurred in 94 of 475 (19.8%) and 33 of 234 patients (14.1%) on durvalumab and placebo, respectively (median follow-up, 25.2 mo); grade greater than or equal to 3 PRP was uncommon (4.6% and 4.7%, respectively). Time to onset and resolution of G2+PRP was similar with durvalumab and placebo. Univariate and multivariate analyses identified patients treated in Asia, those with stage IIIA disease, those with performance status of 1, and those who had not received induction chemotherapy as having a higher risk of G2+PRP. PFS and OS benefit favoring durvalumab versus placebo was maintained regardless of time-dependent G2+PRP.

Conclusions

Factors associated with higher risk of G2+PRP with durvalumab after cCRT were identified. Clinical benefit was maintained regardless of on-study G2+PRP, suggesting the risk of this event should not deter the use of durvalumab in eligible patients with unresectable stage III NSCLC.

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不可切除的 III 期非小细胞肺癌患者同时接受化放疗后使用 Durvalumab 会引发症状性肺炎
简介:在安慰剂对照的3期PACIFIC试验中,对于不可切除的III期NSCLC患者和铂类药物同期化放疗(cCRT)后无进展的患者,durvalumab可显著延长无进展生存期(PFS)(p < 0.0001)和总生存期(OS)(p = 0.00251)。肺炎或放射性肺炎(PRP)在两组中都很常见。我们报告了探索性分析,评估了无症状(≥2级)PRP(G2+PRP)与基线因素和临床结果之间的关系。方法将WHO表现状态为0或1级的患者随机(2:1)分配到12个月的durvalumab或安慰剂治疗,治疗时间为cCRT后1到42天。采用单变量和多变量逻辑回归分析了durvalumab治疗患者的基线因素与研究中G2+PRP之间的关系。使用Cox比例危险模型分析了PFS和OS,该模型调整了时间依赖性G2+PRP以及随机分层因素的协变量(无额外基线因素和有额外基线因素)。结果接受durvalumab和安慰剂治疗的475例患者中分别有94例(19.8%)和234例患者中分别有33例(14.1%)发生了研究中G2+PRP(中位随访25.2个月);大于或等于3级的PRP并不常见(分别为4.6%和4.7%)。Durvalumab和安慰剂的G2+PRP发生和缓解时间相似。通过单变量和多变量分析发现,在亚洲接受治疗的患者、IIIA期患者、表现状态为1级的患者以及未接受诱导化疗的患者发生G2+PRP的风险较高。无论G2+PRP的时间依赖性如何,杜伐单抗相对于安慰剂的PFS和OS获益均得以维持。无论研究中G2+PRP的情况如何,临床获益都能保持不变,这表明这一事件的风险不应阻碍符合条件的不可切除的III期NSCLC患者使用durvalumab。
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来源期刊
CiteScore
4.20
自引率
0.00%
发文量
145
审稿时长
19 weeks
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