O83 Phase 1 study of an anti-CD27 agonist as monotherapy and in combination with pembrolizumab in patients with advanced solid tumors

R. Shapira-Frommer, M. V. Dongen, K. Dobrenkov, E. Chartash, Fang Liu, Claire H. Li, R. Wnek, M. Patel
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引用次数: 5

Abstract

Background MK-5890 is a humanized agonist monoclonal antibody that binds to CD27 to provide a costimulatory signal that enhances T-cell–mediated responses. This first-in-human phase 1 study of MK-5890 evaluated the safety and efficacy of escalating doses of MK-5890 as monotherapy and in combination with pembrolizumab in patients with advanced solid tumors. Methods Key eligibility criteria included histologically or cytologically confirmed advanced solid tumor, measurable disease by RECIST v1.1, and ECOG PS ≤1. MK-5890 was tested alone (dose range, 2-700 mg) or with pembrolizumab (fixed dose, 200 mg). Patients with disease progression following MK-5890 monotherapy were eligible to cross over to combination treatment. The primary objective was safety and tolerability. Objective response rate by investigator per RECIST v1.1 was also evaluated. The database cutoff for this analysis was May 30, 2019. Results Of 44 patients enrolled, 25 received MK-5890 and 19 received MK-5890 plus pembrolizumab; their median age was 59.0 years, 61.4% were female, 47.7% had ECOG PS 1, and 13.6% previously received immune checkpoint inhibitor therapy. In the initial phase, dose-limiting toxicities (DLTs) were reported in 3 patients receiving MK-5890 and 1 patient receiving MK-5890 plus pembrolizumab; all DLTs were associated with infusion-related adverse events. Maximum tolerated dose was defined. Treatment-related adverse events (TRAEs) were reported in 40 patients (90.9%): 22 patients (88.0%) receiving MK-5890 and 18 patients (94.7%) receiving MK-5890 plus pembrolizumab. The most common TRAEs were fatigue (28.0%) and infusion-related reactions (28.0%) with MK-5890 and fatigue (36.8%) and pruritus (31.6%) with MK-5809 plus pembrolizumab. Grade 3-4 TRAEs were reported in 10 patients (22.7%): 6 patients (24.0%) receiving MK-5890 and 4 patients (21.1%) receiving MK-5890 plus pembrolizumab; no grade 5 events were observed. One patient (4.0%) achieved a partial response (PR) with MK-5890 and 1 patient (5.3%) achieved a PR with MK-5890 plus pembrolizumab. Fourteen patients entered the crossover phase to receive MK-5890 plus pembrolizumab. In the crossover phase, no DLTs were reported. TRAEs were reported in 12 patients (85.7%); the most common were pruritus (21.4%), rash (21.4%), and headache (14.3%). One patient (7.1%) reported grade 3-4 TRAEs of increased amylase and increased lipase; no grade 5 events were observed. Two patients (14.3%) achieved a complete response and 2 patients (14.3%) achieved a PR. Conclusions Treatment with MK-5890, alone and in combination with pembrolizumab, demonstrated an acceptable safety profile. Early antitumor activity was observed in patients with advanced solid tumors in both monotherapy and combination therapy arms.
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O83抗cd27激动剂单药和联合派姆单抗治疗晚期实体瘤患者的i期研究
MK-5890是一种人源化激动剂单克隆抗体,可结合CD27提供共刺激信号,增强t细胞介导的应答。MK-5890的第一项人体i期研究评估了逐步增加剂量的MK-5890作为单药治疗和与派姆单抗联合治疗晚期实体瘤患者的安全性和有效性。方法主要入选标准包括组织学或细胞学证实的晚期实体瘤,RECIST v1.1可测量疾病,ECOG PS≤1。MK-5890单独试验(剂量范围,2-700 mg)或与派姆单抗(固定剂量,200 mg)联合试验。MK-5890单药治疗后疾病进展的患者有资格转入联合治疗。主要目标是安全性和耐受性。研究者根据RECIST v1.1的客观缓解率也进行了评估。该分析的数据库截止日期为2019年5月30日。44例入组患者中,25例接受MK-5890治疗,19例接受MK-5890联合派姆单抗治疗;他们的中位年龄为59.0岁,61.4%为女性,47.7%为ECOG ps1, 13.6%以前接受过免疫检查点抑制剂治疗。在初始阶段,3名接受MK-5890治疗的患者和1名接受MK-5890联合派姆单抗治疗的患者报告了剂量限制性毒性(dlt);所有dlt均与输注相关不良事件相关。确定了最大耐受剂量。40例患者(90.9%)报告了治疗相关不良事件(TRAEs): 22例患者(88.0%)接受MK-5890, 18例患者(94.7%)接受MK-5890联合派姆单抗。最常见的trae是MK-5890的疲劳(28.0%)和输液相关反应(28.0%),MK-5809联合派姆单抗的疲劳(36.8%)和瘙痒(31.6%)。10例患者(22.7%)报告了3-4级trae: 6例患者(24.0%)接受MK-5890, 4例患者(21.1%)接受MK-5890联合派姆单抗;未观察到5级事件。1名患者(4.0%)使用MK-5890获得部分缓解(PR), 1名患者(5.3%)使用MK-5890联合派姆单抗获得部分缓解(PR)。14名患者进入交叉期接受MK-5890联合派姆单抗治疗。在交叉阶段,未见dlt的报道。12例(85.7%)出现trae;最常见的是瘙痒(21.4%)、皮疹(21.4%)和头痛(14.3%)。1例患者(7.1%)报告3-4级TRAEs淀粉酶和脂肪酶升高;未观察到5级事件。2例患者(14.3%)获得完全缓解,2例患者(14.3%)获得PR。结论:MK-5890单独治疗和与派姆单抗联合治疗显示出可接受的安全性。单药和联合治疗组在晚期实体瘤患者中均观察到早期抗肿瘤活性。
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Correction: Early disappearance of tumor antigen-reactive T cells from peripheral blood correlates with superior clinical outcomes in melanoma under anti-PD-1 therapy P857 ONM-500 – a novel STING-activating therapeutic nanovaccine platform for cancer immunotherapy P853 Single cell transcriptome analysis identifies unique features in circulating CD8+ T cells that can predict immunotherapy response in melanoma patients O83 Phase 1 study of an anti-CD27 agonist as monotherapy and in combination with pembrolizumab in patients with advanced solid tumors P859 Association of immunopharmacodynamic responses of imprime PGG plus pembrolizumab with clinical benefit in metastatic triple negative breast cancer (TNBC) subjects failing front-line chemotherapy
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