肿瘤内注射toll样受体9 (TLR9)激动剂CMP-001联合派姆单抗治疗抗pd -1难治性黑色素瘤的持久疗效

M. Milhem, Y. Zakharia, D. Davar, E. Buchbinder, T. Medina, A. Daud, A. Ribas, J. Niu, G. Gibney, K. Margolin, A. Olszanski, Interjit Mehmi, Takami Sato, M. Shaheen, Aaron H. Morris, D. Mauro, Katie M. Campbell, R. Bao, G. Weiner, J. Luke, A. Krieg, J. Kirkwood
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CMP-001 is administered IT into accessible lesion(s) either with, or without on-site saline dilution (table 1), and response assessed by RECIST v1.1. Monotherapy patients who progress can be rolled over onto combination therapy and continue on study. Baseline and on-therapy serum is analyzed for cytokines, and immunohistochemistry and RNA-Seq are performed on available tumor biopsies. Abstract O85 Table 1 Advanced anti-PD-1 Refractory melanoma patient population by treatment allocation Results Adverse events (AEs) attributed to CMP-001 in combination with pembrolizumab or as monotherapy consisted predominately of transient low-Grade flu-like symptoms and injection site reactions: Grade 3+ related AEs were reported in 33% of patients treated with combination therapy and 22% of patients with monotherapy. The Objective Response Rate (ORR) with undiluted CMP-001 in combination with pembrolizumab was 24% (18/75; 95% confidence interval: 15%-35% (table 1); on-site dilution of CMP-001 was associated with a substantial decrease in ORR to 12% (7/61; 95% confidence interval: 5%-22% (table 1). Three additional patients had a delayed partial response after an initial period of disease progression. Anti-tumor response was comparable between injected and uninjected lesions. The median duration of response to combination therapy has not been reached. The ORR to CMP-001 monotherapy was 22% (5/23; 95% confidence interval: 7%-44% (table 1); time from last anti-PD-1 therapy before CMP-001 was 1.5 to >20 months in responders; 3 of the patients responding to CMP-001 monotherapy achieved PR at the first evaluation, but progressed by the second evaluation. 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引用次数: 18

摘要

肿瘤内注射CMP-001是一种包装在病毒样颗粒内的CpG-A TLR9激动剂,旨在激活肿瘤相关浆细胞样树突状细胞,诱导富含干扰素的肿瘤微环境和抗肿瘤CD8+ T细胞反应。方法CMP-001-001是一项正在进行的1b期临床试验,评估CMP-001联合派姆单抗(pembrolizumab)的安全性和有效性。N = 144)或单独(第2部分;N = 23),对既往抗pd -1治疗耐药的晚期黑色素瘤患者(表1)。CMP-001在有或没有现场生理盐水稀释的情况下被给予可达病变(s)(表1),并通过RECIST v1.1评估反应。单药治疗取得进展的患者可以转到联合治疗并继续研究。分析基线和治疗期间血清的细胞因子,并对可用的肿瘤活检进行免疫组织化学和RNA-Seq。表1晚期抗pd -1难治性黑色素瘤患者群体的治疗分配结果CMP-001联合派姆单抗或单药治疗的不良事件(ae)主要由短暂的低级别流感样症状和注射部位反应组成:33%的联合治疗患者和22%的单药治疗患者报告了3+级相关ae。未稀释CMP-001联合派姆单抗的客观缓解率(ORR)为24% (18/75;95%置信区间:15%-35%(表1);现场稀释CMP-001与ORR大幅下降至12%相关(7/61;95%置信区间:5%-22%(表1)。另外3例患者在疾病初期进展后出现部分延迟缓解。注射和未注射病变的抗肿瘤反应相当。联合治疗的中位反应持续时间尚未达到。CMP-001单药治疗的ORR为22% (5/23;95%置信区间:7%-44%(表1);从CMP-001之前的最后一次抗pd -1治疗时间为1.5至>20个月;3例对CMP-001单药治疗有反应的患者在第一次评估时达到PR,但在第二次评估时进展。在接受联合治疗的患者中进行的血清和肿瘤活检转化研究支持了TLR9激活的机制,并确定了血清CXCL10的诱导与应答之间可能存在关联。结论IT CMP-001单用和联合派姆单抗耐受性良好,可逆转抗pd -1治疗的耐药,并可在晚期黑色素瘤患者中产生深度和持久的临床反应。伦理审批CMP-001-001由WCG-WIRB集中审批,WIRB审批跟踪号为20152597。
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O85 Durable responses in anti-PD-1 refractory melanoma following intratumoral injection of a toll-like receptor 9 (TLR9) agonist, CMP-001, in combination with pembrolizumab
Background Intratumoral (IT) injection of CMP-001, a CpG-A TLR9 agonist packaged within a virus-like particle, is designed to activate tumor-associated plasmacytoid dendritic cells, inducing an interferon-rich tumor microenvironment and anti-tumor CD8+ T cell responses. Methods CMP-001-001 is an ongoing Phase 1b trial evaluating the safety and efficacy of CMP-001 in combination with pembrolizumab (Part 1; N = 144) or alone (Part 2; N = 23) in patients with advanced melanoma resistant to prior anti-PD-1 therapy (Tables 1). CMP-001 is administered IT into accessible lesion(s) either with, or without on-site saline dilution (table 1), and response assessed by RECIST v1.1. Monotherapy patients who progress can be rolled over onto combination therapy and continue on study. Baseline and on-therapy serum is analyzed for cytokines, and immunohistochemistry and RNA-Seq are performed on available tumor biopsies. Abstract O85 Table 1 Advanced anti-PD-1 Refractory melanoma patient population by treatment allocation Results Adverse events (AEs) attributed to CMP-001 in combination with pembrolizumab or as monotherapy consisted predominately of transient low-Grade flu-like symptoms and injection site reactions: Grade 3+ related AEs were reported in 33% of patients treated with combination therapy and 22% of patients with monotherapy. The Objective Response Rate (ORR) with undiluted CMP-001 in combination with pembrolizumab was 24% (18/75; 95% confidence interval: 15%-35% (table 1); on-site dilution of CMP-001 was associated with a substantial decrease in ORR to 12% (7/61; 95% confidence interval: 5%-22% (table 1). Three additional patients had a delayed partial response after an initial period of disease progression. Anti-tumor response was comparable between injected and uninjected lesions. The median duration of response to combination therapy has not been reached. The ORR to CMP-001 monotherapy was 22% (5/23; 95% confidence interval: 7%-44% (table 1); time from last anti-PD-1 therapy before CMP-001 was 1.5 to >20 months in responders; 3 of the patients responding to CMP-001 monotherapy achieved PR at the first evaluation, but progressed by the second evaluation. Serum and tumor biopsy translational studies in the patients receiving combination therapy supported the proposed mechanism of TLR9 activation and identified a possible association between induction of serum CXCL10 and response. Conclusions IT CMP-001 alone and in combination with pembrolizumab appears well tolerated, can reverse resistance to anti-PD-1 therapy, and can produce deep and durable clinical responses in patients with advanced melanoma. Ethics Approval CMP-001-001 was centrally approved by the WCG-WIRB, WIRB approval tracking number 20152597.
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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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