P858 An open-label, multi-center trial of INO-5401 and INO-9012 delivered by electroporation (EP) in combination with cemiplimab in subjects with newly-diagnosed glioblastoma (GBM)

J. Skolnik, D. Reardon, S. Brem, A. Desai, S. Bagley, Sylvia C. Kurz, M. I. Fuente, S. Nagpal, M. Welch, B. Sacchetta, Sarah K Bartra, A. Bredlau, I. Lowy, K. Kraynyak, M. Morrow, T. McMullan, J. Boyer
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引用次数: 1

Abstract

Background GBM is one of the most deadly cancers and treatment is surgery, followed by radiation (RT) and temozolomide (TMZ) daily during RT followed by cycles of TMZ for select patients.1 New immunotherapies, such as checkpoint inhibition, may benefit patients with GBM. T cell-enabling therapies, in combination with checkpoint inhibition, may improve overall survival (OS). In this study, a novel antigen-specific T cell-generating therapy, INO-5401 (synthetic DNA plasmids encoding for human telomerase [hTERT], Wilms Tumor-1 [WT-1] and prostate specific membrane antigen [PSMA]), plus INO-9012 (synthetic DNA plasmid encoding for IL-12), with the PD-1 checkpoint inhibitor, cemiplimab, was given to patients with newly-diagnosed GBM to evaluate tolerability, immunogenicity and clinical efficacy of the combination. Methods Phase I/II, single arm, two cohort study (A: MGMT Promoter Unmethylated, B: MGMT Promoter Methylated). The primary objective is to evaluate the safety of INO-5401 and INO-9012 followed by EP with CELLECTRA® 2000 in combination with cemiplimab. Secondary objectives include the evaluation of preliminary clinical efficacy and immunogenicity. Treatment is with 9 mg INO-5401 with 1 mg INO-9012 every three weeks (Q3W) for four doses, then Q9W; and cemiplimab (350 mg IV Q3W). RT is given as 40 Gy over three weeks; TMZ is given concurrent with radiation (Cohorts A and B), followed by maintenance TMZ (Cohort B). Results 52 patients were enrolled onto this study; 32 in Cohort A and 20 in Cohort B. 18 were women (35%) and 47 were white (90%). The median age was 60 years (range 19-78 years). The most common Grade ≥3 adverse events were elevations in alanine or aspartate aminotransferase (ALT/AST; 5 patients), and tumor inflammation/edema (5 patients); there was one Grade 5 unrelated event of urosepsis. The only related SAE reported in more than one patient was pyrexia. 22 patients (42%) reported immune-related AEs, with the most common being elevations in ALT or AST (8 patients), and were reported most commonly within the first nine weeks of treatment. The safety profile was consistent with that of patients with GBM and of checkpoint inhibitors. ELISpot assessments performed to date demonstrated the majority of patients have T cell responses to INO-5401. PFS6 was 75% (95% CI 56.6, 88.5) in Cohort A (preliminary; Cohort B pending). Conclusions INO-5401 + INO-9012 with cemiplimab has an acceptable safety profile, is immunogenic and is potentially efficacious in patients with newly-diagnosed GBM. This combination is promising; survival results will be updated next year. Trial Registration NCT03491683. Ethics Approval This study was approved by New York University institution’s Ethics Board; approval number i17-00764. References Stupp R, et al. (2009). Lancet Oncology 10(5): 459–466.
一项开放标签、多中心试验:INO-5401和INO-9012通过电穿孔(EP)联合西米单抗治疗新诊断的胶质母细胞瘤(GBM)患者
GBM是最致命的癌症之一,治疗方法是手术,然后是放疗(RT)和替莫唑胺(TMZ),在放疗期间每天,然后选择患者进行TMZ周期治疗新的免疫疗法,如检查点抑制,可能使GBM患者受益。T细胞激活疗法,结合检查点抑制,可能提高总生存率(OS)。本研究采用新型抗原特异性T细胞生成疗法INO-5401(编码人类端粒酶[hTERT]、Wilms Tumor-1 [WT-1]和前列腺特异性膜抗原[PSMA]的合成DNA质粒)和INO-9012(编码IL-12的合成DNA质粒)联合PD-1检查点抑制剂cemiplimab,对新诊断的GBM患者进行耐受性、免疫原性和临床疗效评价。方法I/II期,单臂,双队列研究(A: MGMT启动子未甲基化,B: MGMT启动子甲基化)。主要目的是评估INO-5401和INO-9012的安全性,随后是EP与CELLECTRA®2000联合用药。次要目的包括初步临床疗效和免疫原性评价。治疗方法是每三周使用9mg INO-5401和1mg INO-9012 (Q3W),共四次,然后是Q9W;和西米单抗(350mg IV Q3W)。三周内给予40 Gy的RT;TMZ与放疗同时给予(队列A和B),随后给予维持TMZ(队列B)。结果52例患者纳入本研究;A组32例,b组20例,女性18例(35%),白人47例(90%)。中位年龄为60岁(范围19-78岁)。最常见的≥3级不良事件是丙氨酸或天冬氨酸转氨酶(ALT/AST;肿瘤炎症/水肿(5例);有1例5级尿脓毒症无关事件。在一个以上的患者中报告的唯一相关SAE是发热。22名患者(42%)报告了免疫相关的不良反应,最常见的是ALT或AST升高(8名患者),最常见于治疗的前9周。安全性与GBM患者和检查点抑制剂一致。迄今为止进行的ELISpot评估显示,大多数患者对INO-5401有T细胞应答。队列A中PFS6为75% (95% CI 56.6, 88.5)(初步;B队列待定)。结论INO-5401 + INO-9012联合头孢米单抗具有可接受的安全性,具有免疫原性,对新诊断的GBM患者可能有效。这种组合是有希望的;生存结果将于明年更新。试验注册编号NCT03491683。本研究经纽约大学伦理委员会批准;批准号i17-00764。参考文献Stupp R等(2009)。中华医学杂志,10(5):459-466。
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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