Response-Adaptive Surgical Timing in neoadjuvant immunotherapy demonstrates enhanced pathologic treatment response in Head and Neck Squamous Cell Carcinoma.

IF 10 1区医学 Q1 ONCOLOGY Clinical Cancer Research Pub Date : 2024-11-25 DOI:10.1158/1078-0432.CCR-24-0037

Eric V Mastrolonardo, Kathryn L Nunes, Pablo Llerena, Anastasia Nikitina, Anastasia Sobol, E Reilly Scott, Madalina Tuluc, Christopher J H Davitt, Jessica Scher, Sruti Tekumalla, Derek Mann, Camilo Henao, Victor Jegede, Stacey Gargano, Larry A Harshyne, Angela Alnemri, Andrey Tyshevich, Vladimir Kushnarev, Madison Chasse, Danielle Sookiasian, Rita Axelrod, Tingting Zhan, Benjamin E Leiby, Matthew Old, Nolan Seim, My G Mahoney, Ubaldo Martinez-Outschoorn, David M Cognetti, Joseph M Curry, George Prendergast, Athanassios Argiris, Andrew P South, Alban J Linnenbach, Jennifer M Johnson, Adam J Luginbuhl

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Abstract

Purpose: We evaluated whether IDO-inhibitor BMS986205 (IDOi) + PD-1 inhibitor nivolumab enhanced T-cell activity and augmented immune-mediated antitumor responses in untreated, resectable HNSCC. We employed response-adaptive surgical timing to identify responders to immunotherapy and enhance their response.

Patients and methods: Patients with HNSCC were 3:1 randomized to receive nivolumab with or without BMS986205 PO daily (NCT03854032). In the combination arm, BMS986205 was initiated 7 days prior to nivolumab. Patients were stratified by HPV status. Response-adaptive surgical timing involved response assessment by radiographic criteria 4 weeks after nivolumab in both arms. Non-responders underwent surgical resection, while responders received 4 more weeks of randomized therapy before surgery. Biomarker analysis utilized pathologic treatment response (pTR) and RNA sequencing.

Results: Forty-two patients were enrolled, and the addition of IDOi to nivolumab did not result in greater rate of radiographic response (p=0.909). Treatment was well-tolerated with only 2 (5%) patients experiencing grade 3 immune-related adverse events. The addition of IDO-inhibitor augmented rates of pTR in patients with high baseline IDO RNA expression (p<0.05). Response-adaptive surgical timing demonstrated reliability in differentiating pathologic responders versus non-responders (p=0.009). A pretreatment NK cell signature, PD-L1 status, and IFN-g expression in the HPV- cohort correlated with response. HPV+ cohort found B-cell and CAF signatures predictive of response/non-response.

Conclusions: Response-adaptive surgical timing enhanced treatment response. IDO-inhibitor BMS986205 augmented pTR in patients with high IDO1-expression in baseline samples, indicating a need for identifying and targeting resistant nodes to immunotherapy. HPV-status-dependent signatures predicting response to immunotherapy in HNSCC warrant further study.

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新辅助免疫疗法中的反应适应性手术时机可增强头颈部鳞状细胞癌的病理治疗反应。

目的：我们评估了IDO抑制剂BMS986205（IDOi）+PD-1抑制剂nivolumab是否能增强未经治疗、可切除的HNSCC患者的T细胞活性并增强免疫介导的抗肿瘤反应。我们采用了反应适应性手术时机来识别免疫疗法的反应者并增强其反应：HNSCC患者按3:1的比例随机接受nivolumab联合或不联合BMS986205每日PO治疗（NCT03854032）。在联合治疗组中，BMS986205在nivolumab治疗前7天开始使用。根据 HPV 状态对患者进行分层。两组患者均在使用 nivolumab 4 周后，根据放射学标准对反应进行评估，确定反应适应性手术时间。无应答者接受手术切除，而有反应者在手术前再接受4周的随机治疗。生物标志物分析采用病理治疗反应（pTR）和RNA测序：42名患者入组，在nivolumab基础上加用IDOi并没有提高放射学反应率（p=0.909）。治疗耐受性良好，仅有2名（5%）患者出现3级免疫相关不良反应。在基线IDO RNA表达较高的患者中，加用IDO抑制剂可提高pTR率（p结论：反应适应性手术时机提高了治疗反应。IDO抑制剂BMS986205提高了基线样本中IDO1高表达患者的pTR，这表明需要识别并针对耐药结节进行免疫治疗。预测HNSCC免疫疗法反应的HPV状态依赖性特征值得进一步研究。

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来源期刊

Clinical Cancer Research 医学-肿瘤学

CiteScore

20.10

自引率

1.70%

发文量

1207

审稿时长

2.1 months

期刊介绍： Clinical Cancer Research is a journal focusing on groundbreaking research in cancer, specifically in the areas where the laboratory and the clinic intersect. Our primary interest lies in clinical trials that investigate novel treatments, accompanied by research on pharmacology, molecular alterations, and biomarkers that can predict response or resistance to these treatments. Furthermore, we prioritize laboratory and animal studies that explore new drugs and targeted agents with the potential to advance to clinical trials. We also encourage research on targetable mechanisms of cancer development, progression, and metastasis.