Early On-Treatment Assessment of T Cells, Cytokines, and Tumor DNA with Adaptively Dosed Nivolumab + Ipilimumab: Final Results from the Phase 2 ADAPT-IT Study.

IF 10 1区医学 Q1 ONCOLOGY

Clinical Cancer Research Pub Date : 2024-08-15 DOI:10.1158/1078-0432.CCR-23-3643

James W Smithy, Hannah L Kalvin, Fiona D Ehrich, Ronak Shah, Matthew Adamow, Vladislav Raber, Collen A Maher, Jenna Kleman, Deborah A G McIntyre, Alexander N Shoushtari, Allison Betof Warner, Margaret K Callahan, Parisa Momtaz, Omar Eton, Suresh Nair, Jedd D Wolchok, Paul B Chapman, Michael F Berger, Katherine S Panageas, Michael A Postow

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引用次数: 0

Abstract

Purpose: The Adaptively Dosed ImmunoTherapy Trial (ADAPT-IT;NCT03122522) investigated adaptive ipilimumab discontinuation in melanoma based on early radiographic assessment. Initial findings indicated similar effectiveness compared with conventional nivolumab-ipilimumab (nivo-ipi). Exploratory biomarker analyses and final clinical results are now reported.

Patients and methods: Patients with unresectable melanoma received two doses of nivo-ipi. Radiographic assessment at Week 6 informed continuation of ipilimumab before nivolumab maintenance. The primary endpoint was overall response rate at Week 12. Plasma was assayed for circulating tumor DNA and 10 cytokines using a multiplex immunoassay. Flow cytometry of peripheral blood mononuclear cells was performed with an 11-color panel.

Results: Among the treated patients, expansion of proliferating T-cell populations was observed in responders and nonresponders. Baseline IL6 levels were low in patients achieving an objective radiographic response (median 1.30 vs. 2.86 pg/mL; P = 0.025). High baseline IL6 levels were associated with short progression-free survival [PFS; HR = 1.24, 95% confidence interval (CI), 1.01-1.52; P = 0.041]. At Week 6, patients with response had lower average tumor variant allele fractions than nonresponders (median 0.000 vs. 0.019; P = 0.014). Greater increases in average variant allele fractions from baseline to Week 6 correlated with short PFS (HR = 1.11, 95% CI, 1.01-1.21; P = 0.023). Week 12 overall response rate was 47% (95% CI, 35%-59%) with a median follow-up of 34 months among survivors. Median PFS was 21 months (95% CI, 10-not reached); 76% of responses (95% CI, 64%-91%) persisted at 36 months.

Conclusions: Adaptively dosed nivo-ipi responses are durable and resemble historical data for conventional nivo-ipi. Baseline IL6 and circulating tumor DNA changes during treatment warrant further study as biomarkers of nivo-ipi response.

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使用适应性剂量的 nivolumab + ipilimumab 对 T 细胞、细胞因子和肿瘤 DNA 进行早期治疗评估：ADAPT-IT 二期研究的最终结果。

目的：ADAPT-IT（NCT03122522）研究了基于早期放射学评估的黑色素瘤适应性伊匹单抗停药。初步研究结果表明，与传统的nivolumab-ipilimumab（nivo-ipi）相比，其疗效相似。现报告探索性生物标志物分析和最终临床结果：无法切除的黑色素瘤患者接受了两种剂量的nivo-ipi治疗。在第6周进行的放射学评估告知患者在尼夫单抗维持治疗前继续使用伊匹单抗。主要终点是第12周时的总反应率（ORR）。使用多重免疫测定法检测血浆中的循环肿瘤DNA（ctDNA）和10种细胞因子。外周血单核细胞流式细胞仪采用 11 色板进行检测：结果：在接受治疗的患者中，应答者和非应答者都观察到增殖 T 细胞群的扩增。获得客观放射学反应的患者的基线 IL-6 水平较低（中位数为 1.30 vs 2.86 pg/mL；P=0.025）。较高的基线IL-6水平与较短的无进展生存期（PFS；危险比（HR）=1.24，95% CI：1.01-1.52；P=0.041）相关。第6周时，与无应答患者相比，有应答患者的平均肿瘤变异等位基因分数（VAF）更低（中位数为0.000 v 0.019；P=0.014）。从基线到第6周，平均VAF的增幅越大，PFS越短（HR=1.11，95% CI：1.01-1.21；p=0.023）。第12周的ORR为47%（95% CI：35-59%），幸存者的中位随访时间为34个月。中位PFS为21个月（95% CI:10-未达到）；76%的反应（95% CI:64%-91%）持续36个月：结论：自适应剂量的nivo-ipi反应是持久的，与传统nivo-ipi的历史数据相似。治疗期间基线IL-6和ctDNA的变化作为nivo-ipi反应的生物标志物值得进一步研究。

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

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.

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