在1期剂量扩大队列中,OX40 (PF-04518600)和4-1BB (utomilumab)激动抗体联合治疗黑色素瘤和非小细胞肺癌的结果

A. Chiappori, John A Thompson, F. Eskens, J. Spano, T. Doi, O. Hamid, A. Diab, N. Rizvi, S. Hu-Lieskovan, W. Ros, Jacob S. Thomas, A. Forgie, Wenjing Yang, K. Liao, Ray Li, Farhad Kazazi, J. Chou, A. E. Khoueiry
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Efficacy, safety, and the association of baseline and pharmacodynamic biomarkers with efficacy were examined. Methods In this expansion cohort, patients with locally advanced/metastatic melanoma (n=10) and NSCLC (n=20) who progressed on prior anti-PD1/PD-L1 treatment and/or anti CTLA4 treatment (melanoma only) were enrolled. Patients received OX40 antibody 30 mg IV every 2wks in combination with uto 20 mg IV every 28d. Tumor assessments were performed every 8wks using RECIST1.1. Paired biopsy samples collected at baseline and 6wks were analyzed by immunohistochemistry and RNA sequencing to evaluate the pharmacodynamic effects of the OX40 antibody in combination with uto. Whole blood samples were collected longitudinally, from which DNA was extracted and submitted for high-throughput sequencing of the T cell receptor β-chain. Results One patient with NSCLC achieved a confirmed and ongoing partial response lasting at least 6 months; Based on analyses of a subset of baseline biopsies, this patient’s tumor had the lowest FOXP3 expression. A total of 7 (70%) melanoma patients and 7 (35%) NSCLC patients achieved a best overall response of stable disease (SD). The median duration of SD was 16.3 weeks (melanoma: 16.0 weeks; NSCLC: 24.1 weeks), for a disease control rate of 50%. Among patients with a defined response, paired biopsy analyses showed that the greatest increase in CD8 occurred in the NSCLC patient with the longest duration of stable disease. The most frequent treatment related adverse events (TRAEs) reported in ≥10% of patients were pruritis, anemia, fatigue, decreased appetite, and rash. Grade 3 TRAEs, rash and lymphocyte count decreased, were reported in 5 patients and a grade 4 TRAE of lipase increased (asymptomatic) was reported in 1 patient. Conclusions The combination of PF-8600 and uto had a tolerable safety profile and demonstrated clinical benefit, including in an NSCLC patient who had progressed on anti-PD1 therapy and achieved a durable partial response. Further combinations with one or both of these immune costimulatory receptor agonist antibodies might enhance their efficacy. Acknowledgements This study was funded by Pfizer Inc. Editorial support was provided by Chu Kong Liew, PhD, of Engage Scientific Solutions and was funded by Pfizer Inc. 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引用次数: 9

摘要

背景PF-04518600 (PF-8600)和utomilumab (uto)分别是针对肿瘤坏死因子超家族受体OX40和4-1BB的人源化激动剂IgG2单克隆抗体。在一项I期剂量递增研究(NCT02315066)中,该抗体组合在所有剂量水平下都是耐受的,并且在免疫检查点抑制剂耐药的黑色素瘤患者中诱导了应答。我们报告了一项剂量扩大队列研究的结果,该研究针对的是使用PF-8600 (OX40抗体)联合uto治疗的黑色素瘤和非小细胞肺癌(NSCLC)患者。检查了疗效、安全性以及基线和药效学生物标志物与疗效的关系。方法在这个扩展队列中,纳入了局部晚期/转移性黑色素瘤(n=10)和NSCLC (n=20)患者,这些患者先前接受过抗pd1 /PD-L1治疗和/或抗CTLA4治疗(仅限黑色素瘤)。患者接受OX40抗体30 mg IV,每2周联合u20 mg IV,每28d。采用recst1.1每8周进行一次肿瘤评估。通过免疫组织化学和RNA测序分析在基线和6wks收集的成对活检样本,以评估OX40抗体与uto联合的药效学效果。纵向采集全血样本,从中提取DNA并提交给T细胞受体β链的高通量测序。结果1例NSCLC患者获得了持续至少6个月的部分缓解;根据基线活检亚组的分析,该患者的肿瘤FOXP3表达最低。共有7例(70%)黑色素瘤患者和7例(35%)非小细胞肺癌患者获得了稳定疾病(SD)的最佳总体缓解。SD的中位持续时间为16.3周(黑色素瘤:16.0周;NSCLC: 24.1周),疾病控制率为50%。在有明确反应的患者中,配对活检分析显示,CD8的最大增加发生在疾病稳定持续时间最长的NSCLC患者中。≥10%的患者报告的最常见的治疗相关不良事件(TRAEs)是瘙痒、贫血、疲劳、食欲下降和皮疹。5例患者报告了3级TRAE,皮疹和淋巴细胞计数减少,1例患者报告了脂肪酶4级TRAE增加(无症状)。结论:PF-8600联合uto具有可耐受的安全性和临床益处,包括在抗pd1治疗进展并获得持久部分缓解的非小细胞肺癌患者中。进一步与一种或两种免疫共刺激受体激动剂抗体联合使用可能会提高其疗效。本研究由辉瑞公司资助。编辑支持由Engage Scientific Solutions的Chu Kong Liew博士提供,由辉瑞公司资助。临床试验。伦理批准本研究由各研究中心的机构审查委员会批准,并按照《赫尔辛基宣言》的伦理原则进行。
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P860 Results from a combination of OX40 (PF-04518600) and 4–1BB (utomilumab) agonistic antibodies in melanoma and non-small cell lung cancer in a phase 1 dose expansion cohort
Background PF-04518600 (PF-8600) and utomilumab (uto) are humanized agonist IgG2 monoclonal antibodies for the tumor necrosis factor superfamily receptors OX40 and 4-1BB, respectively. In a phase I dose escalation study (NCT02315066), this antibody combination was tolerable at all dose levels and induced responses in patients with melanoma resistant to immune checkpoint inhibitors. We report results from a dose expansion cohort of this study of patients with melanoma and non-small cell lung cancer (NSCLC) treated with PF-8600 (OX40 antibody) in combination with uto. Efficacy, safety, and the association of baseline and pharmacodynamic biomarkers with efficacy were examined. Methods In this expansion cohort, patients with locally advanced/metastatic melanoma (n=10) and NSCLC (n=20) who progressed on prior anti-PD1/PD-L1 treatment and/or anti CTLA4 treatment (melanoma only) were enrolled. Patients received OX40 antibody 30 mg IV every 2wks in combination with uto 20 mg IV every 28d. Tumor assessments were performed every 8wks using RECIST1.1. Paired biopsy samples collected at baseline and 6wks were analyzed by immunohistochemistry and RNA sequencing to evaluate the pharmacodynamic effects of the OX40 antibody in combination with uto. Whole blood samples were collected longitudinally, from which DNA was extracted and submitted for high-throughput sequencing of the T cell receptor β-chain. Results One patient with NSCLC achieved a confirmed and ongoing partial response lasting at least 6 months; Based on analyses of a subset of baseline biopsies, this patient’s tumor had the lowest FOXP3 expression. A total of 7 (70%) melanoma patients and 7 (35%) NSCLC patients achieved a best overall response of stable disease (SD). The median duration of SD was 16.3 weeks (melanoma: 16.0 weeks; NSCLC: 24.1 weeks), for a disease control rate of 50%. Among patients with a defined response, paired biopsy analyses showed that the greatest increase in CD8 occurred in the NSCLC patient with the longest duration of stable disease. The most frequent treatment related adverse events (TRAEs) reported in ≥10% of patients were pruritis, anemia, fatigue, decreased appetite, and rash. Grade 3 TRAEs, rash and lymphocyte count decreased, were reported in 5 patients and a grade 4 TRAE of lipase increased (asymptomatic) was reported in 1 patient. Conclusions The combination of PF-8600 and uto had a tolerable safety profile and demonstrated clinical benefit, including in an NSCLC patient who had progressed on anti-PD1 therapy and achieved a durable partial response. Further combinations with one or both of these immune costimulatory receptor agonist antibodies might enhance their efficacy. Acknowledgements This study was funded by Pfizer Inc. Editorial support was provided by Chu Kong Liew, PhD, of Engage Scientific Solutions and was funded by Pfizer Inc. Trial Registration ClinicalTrials. gov: NCT02315066 Ethics Approval The study was approved by the institutional review board at each study center and conducted in accordance with the ethical principles of the Declaration of Helsinki.
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