顺铂禁忌症患者局部晚期头颈癌放疗联合西妥昔单抗或达伐单抗(NRG-HN004):一项开放标签、多中心、平行组、随机的 2/3 期试验

Loren K Mell, Pedro A Torres-Saavedra, Stuart J Wong, Julie A Kish, Steven S Chang, Richard C Jordan, Tian Liu, Minh Tam Truong, Eric W Winquist, Vinita Takiar, Trisha Wise-Draper, Jared R Robbins, Cristina P Rodriguez, Musaddiq J Awan, Beth M Beadle, Christina Henson, Samir Narayan, Sharon A Spencer, Steven Powell, Neal Dunlap, Quynh-Thu Le
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引用次数: 0

摘要

背景在顺铂禁忌症的情况下,局部区域晚期头颈部鳞状细胞癌(HNSCC)患者的治疗存在争议。方法NRG-HN004是一项开放标签、多中心、平行组、随机、2/3期试验,在北美的89个学术和社区医疗中心进行。符合条件的患者年龄在18岁或18岁以上,患有美国癌症联合委员会第8版III-IVB期p16阴性HNSCC或I-III期p16阳性口咽癌或不明原发癌,且有顺铂禁忌症(东部合作肿瘤学组[ECOG]表现状态2、肾功能或听力受损、周围神经病变、年龄至少70岁且有中度或重度合并症,或年龄小于70岁且有重度合并症)。患者通过包块随机化(6的倍数)被随机分配(2:1)至静脉注射杜瓦鲁单抗1500毫克(放疗前2周开始)或静脉注射西妥昔单抗400毫克/平方米(放疗前1周开始)或静脉注射西妥昔单抗250毫克/平方米(放疗前1周开始),然后从放疗第1周开始每周注射250毫克/平方米(8个周期),同时接受调强放疗(70 Gy,35次/分,7周)。分层因素包括肿瘤和结节分期、ECOG表现状态和合并症、原发部位和p16状态。二期研究的主要终点是意向治疗人群的无进展生存期。在无进展生存期信息为50%时进行了一次预设的中期无用性分析。如果观察到的危险比为1-0或更高,且西妥昔单抗更有利,则将考虑提前停止治疗。延长随访分析为事后分析。该试验已在ClinicalTrials.gov注册,编号为NCT03258554,目前已结束报名。研究结果在10名患者的安全先导试验后,2期试验从2019年3月12日到2021年7月30日共招募了190名患者,其中186名患者被随机分配(123名患者接受度伐单抗治疗,63名患者接受西妥昔单抗治疗)。中位年龄为72岁(IQR 64-77),30名(16%)患者为女性,156名(84%)患者为男性。在进行中期无效性分析后,2期试验于2021年7月30日暂停,并于2022年9月1日永久结束。该试验的 3 期部分没有进行。在中位随访2-3年(IQR 1-9-3-1)的延长随访中(数据截止日期为2023年7月31日;事后分析),durvalumab组的2年无进展生存率为50-6%(95% CI 41-5-59-8),而西妥昔单抗组为63-7%(51-3-76-1)(危险比1-33 [95% CI 0-84-2-12];P=0-89)。两组的不良事件相似。最常见的3-4级不良事件是吞咽困难(119例杜瓦单抗组患者中26例[22%] vs 61例西妥昔单抗组患者中18例[30%])、淋巴细胞减少症(33例[28%] vs 20例[33%])和口腔黏膜炎(13例[11%] vs 11例[18%])。杜瓦鲁单抗组和西妥昔单抗组分别有4名(3%)和1名(2%)患者死于与治疗相关的不良事件(杜瓦鲁单抗组患者死于未注明原因的死亡、喉头水肿、肺部感染和呼吸衰竭,西妥昔单抗组患者死于未注明原因的猝死)。需要进一步的试验来确定这一人群的治疗标准。资金来源美国国家癌症研究所和阿斯利康公司。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Radiotherapy with cetuximab or durvalumab for locoregionally advanced head and neck cancer in patients with a contraindication to cisplatin (NRG-HN004): an open-label, multicentre, parallel-group, randomised, phase 2/3 trial

Background

Management of patients with locoregionally advanced head and neck squamous cell carcinoma (HNSCC) when cisplatin is contraindicated is controversial. We aimed to assess whether radiotherapy with concurrent and adjuvant durvalumab would improve outcomes compared with radiotherapy with cetuximab.

Methods

NRG-HN004 was designed as an open-label, multicentre, parallel-group, randomised, phase 2/3 trial with safety lead-in conducted at 89 academic and community medical centres in North America. Eligible patients were aged 18 years or older with American Joint Committee on Cancer 8th edition stage III–IVB p16-negative HNSCC or unfavourable stage I–III p16-positive oropharyngeal or unknown primary carcinoma, who had a contraindication to cisplatin (Eastern Cooperative Oncology Group [ECOG] performance status 2, renal or hearing impairment, peripheral neuropathy, aged at least 70 years with moderate or severe comorbidity, or aged younger than 70 years with severe comorbidity). Patients were randomly assigned (2:1) by permuted block randomisation (multiples of 6) to intravenous durvalumab 1500 mg starting 2 weeks before radiotherapy then every 4 weeks starting week 2 of radiotherapy (seven cycles) or intravenous cetuximab 400 mg/m2 1 week before radiotherapy then 250 mg/m2 weekly beginning week 1 of radiotherapy (eight cycles), with intensity-modulated radiotherapy (70 Gy in 35 fractions over 7 weeks). Stratification factors were tumour and nodal stage, ECOG performance status and comorbidity, and primary site and p16 status. The phase 2 primary endpoint was progression-free survival in the intention-to-treat population. There was one prespecified interim futility analysis at 50% of progression-free survival information. If the observed hazard ratio was 1·0 or more, favouring cetuximab, early stopping would be considered. Extended follow-up analysis was post hoc. This trial is registered with ClinicalTrials.gov, NCT03258554, and is closed to enrolment.

Findings

Following a ten-patient safety lead-in, the phase 2 trial enrolled 190 patients from March 12, 2019, to July 30, 2021, 186 of whom were randomly assigned (123 to durvalumab and 63 to cetuximab). Median age was 72 years (IQR 64–77), 30 (16%) patients were women and 156 (84%) were men. Phase 2 accrual was suspended in July 30, 2021, following an interim futility analysis, and permanently closed in Sept 1, 2022. The phase 3 part of the trial was not conducted. At a median follow-up of 2·3 years (IQR 1·9–3·1) for the extended follow-up (data cutoff July 31, 2023; post-hoc analysis), 2-year progression-free survival was 50·6% (95% CI 41·5–59·8) in the durvalumab group versus 63·7% (51·3–76·1) in the cetuximab group (hazard ratio 1·33 [95% CI 0·84–2·12]; p=0·89). Adverse events were similar in both groups. The most common grade 3–4 adverse events were dysphagia (26 [22%] of 119 patients in the durvalumab group vs 18 [30%] of 61 patients in the cetuximab group), lymphopenia (33 [28%] vs 20 [33%]), and oral mucositis (13 [11%] vs 11 [18%]). Four (3%) patients in the durvalumab group and one (2%) in the cetuximab group died from treatment-related adverse events (death not otherwise specified, laryngeal oedema, lung infection, and respiratory failure in the durvalumab group and sudden death not otherwise specified in the cetuximab group).

Interpretation

Our findings suggest that durvalumab did not improve outcomes compared with cetuximab in patients with HNSCC with contraindications to cisplatin. Further trials are needed to define the standard of care for this population.

Funding

US National Cancer Institute and AstraZeneca.
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