GI-4000是一种表达突变RAS蛋白的重组酵母,用于胰腺癌切除患者的2期随机安慰剂对照佐剂试验。

Journal of Pancreatic Cancer Pub Date : 2021-03-23 eCollection Date: 2021-01-01 DOI:10.1089/pancan.2020.0021
Peter Muscarella, Tanios Bekaii-Saab, Kristi McIntyre, Alexander Rosemurgy, Sharona B Ross, Donald A Richards, William E Fisher, Patrick J Flynn, Alicia Mattson, Claire Coeshott, Heinrich Roder, Joanna Roder, Frank E Harrell, Allen Cohn, Timothy C Rodell, David Apelian
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引用次数: 8

摘要

目的:研究表达四种不同突变RAS蛋白的重组酵母GI-4000在切除的RAS突变胰腺癌患者中的作用。方法:受试者(n = 176)接受GI-4000或安慰剂加吉西他滨治疗。对受试者的肿瘤进行基因分型,以确定与GI-4000产品相匹配的药物。免疫应答通过干扰素-γ (IFNγ) ELISpot检测和调节性T细胞(Treg)频率检测。采用基质辅助激光解吸/电离飞行时间(MALDI-ToF)质谱法对预处理血浆进行回顾性分析,以获得预测GI-4000反应性的蛋白质组学特征。结果:GI-4000耐受性良好,治疗组之间的安全性相当。与安慰剂组相比,GI-4000组显示出相似的中位无复发和总生存期(OS)模式。对于前瞻性定义和分层的R1切除亚组,1年OS有趋势(72% vs 56%), OS有改善(523.5 vs 443.5天[风险比(HR) = 1.06[置信区间(CI): 0.53-2.13], p = 0.872),免疫应答者频率增加(40% vs 8%;p = 0.062), R1 GI-4000免疫应答者与安慰剂相比,159天的OS改善(p = 0.810)。对于R0切除的受试者,gi -4000治疗的受试者未观察到IFNγ反应增加。与安慰剂相比,gi -4000治疗组R0/R1患者Tregs (CD4+/CD45RA+/Foxp3low)降低的频率更高(p = 0.033)。确定了一个蛋白质组学特征,预测GI-4000/吉西他滨的反应,无论切除情况如何。结论:这些结果证明了继续对GI-4000进行分层研究,以确定可能的应答者或与免疫检查点抑制剂或其他免疫调节剂联合使用,这可能提供最佳的抗肿瘤免疫再激活。ClinicalTrials.gov编号:NCT00300950。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Phase 2 Randomized Placebo-Controlled Adjuvant Trial of GI-4000, a Recombinant Yeast Expressing Mutated RAS Proteins in Patients with Resected Pancreas Cancer.

A Phase 2 Randomized Placebo-Controlled Adjuvant Trial of GI-4000, a Recombinant Yeast Expressing Mutated RAS Proteins in Patients with Resected Pancreas Cancer.

A Phase 2 Randomized Placebo-Controlled Adjuvant Trial of GI-4000, a Recombinant Yeast Expressing Mutated RAS Proteins in Patients with Resected Pancreas Cancer.

A Phase 2 Randomized Placebo-Controlled Adjuvant Trial of GI-4000, a Recombinant Yeast Expressing Mutated RAS Proteins in Patients with Resected Pancreas Cancer.

Purpose: GI-4000, a series of recombinant yeast expressing four different mutated RAS proteins, was evaluated in subjects with resected ras-mutated pancreas cancer. Methods: Subjects (n = 176) received GI-4000 or placebo plus gemcitabine. Subjects' tumors were genotyped to identify which matched GI-4000 product to administer. Immune responses were measured by interferon-γ (IFNγ) ELISpot assay and by regulatory T cell (Treg) frequencies on treatment. Pretreatment plasma was retrospectively analyzed by matrix-assisted laser desorption/ionization-time-of-flight (MALDI-ToF) mass spectrometry for proteomic signatures predictive of GI-4000 responsiveness. Results: GI-4000 was well tolerated, with comparable safety findings between treatment groups. The GI-4000 group showed a similar pattern of median recurrence-free and overall survival (OS) compared with placebo. For the prospectively defined and stratified R1 resection subgroup, there was a trend in 1 year OS (72% vs. 56%), an improvement in OS (523.5 vs. 443.5 days [hazard ratio (HR) = 1.06 [confidence interval (CI): 0.53-2.13], p = 0.872), and increased frequency of immune responders (40% vs. 8%; p = 0.062) for GI-4000 versus placebo and a 159-day improvement in OS for R1 GI-4000 immune responders versus placebo (p = 0.810). For R0 resection subjects, no increases in IFNγ responses in GI-4000-treated subjects were observed. A higher frequency of R0/R1 subjects with a reduction in Tregs (CD4+/CD45RA+/Foxp3low) was observed in GI-4000-treated subjects versus placebo (p = 0.033). A proteomic signature was identified that predicted response to GI-4000/gemcitabine regardless of resection status. Conclusion: These results justify continued investigation of GI-4000 in studies stratified for likely responders or in combination with immune check-point inhibitors or other immunomodulators, which may provide optimal reactivation of antitumor immunity. ClinicalTrials.gov Number: NCT00300950.

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