摘要:用pepinemab(一流的信号素4D单抗)重编程TME中的骨髓细胞,增强联合免疫治疗

E. Evans, H. Bussler, C. Mallow, C. Reilly, Sebold Torno, Maria Scrivens, Alan P. Howell, Leslie Balch, J. Leonard, T. Fisher, C. Allen, Paúl E. Clavijo, Gregory Lesiniski, Christina Wu, S. Hu-Lieskovan, A. Ribas, Emily G Greengard, Ernest S. Smith, M. Zauderer
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Antitumor activity and immune response was characterized by immunohistochemistry, flow cytometry, functional assays, and cytokine, chemokine and gene expression analysis. Pepinemab (VX15/2503) is currently being evaluated as single agent or in combination with other immunotherapies in four clinical trials: (i) a phase 1b/2a combination trial of pepinemab with avelumab in NSCLC (CLASSICAL-Lung) (NCT03268057); (ii) a phase 1 combination trial of pepinemab with nivolumab or ipilimumab in melanoma patients who have progressed on any anti-PD-1/PD-L1 (NCT03373188); (iii) a neoadjuvant integrated biomarker trial in patients with metastatic colorectal and pancreatic cancers treated with pepinemab in combination with nivolumab or ipilimumab (NCT03373188); and (iv) a phase 1/2 trial of pepinemab in children with solid tumors and children and young adults with osteosarcoma (NCT03320330). Results: SEMA4D exerts multifaceted effects within the tumor microenvironment by creating a barrier at the tumor-stroma margin to restrict immune cell infiltration and promoting immunosuppressive activity of myeloid-derived cells. Blocking antibody to SEMA4D directly enhanced M1/M2 ratio and both reduced expression of chemokines that recruit MDSC and the ability of MDSC to suppress T-cell proliferation. Antibody blockade reduced the function of immunosuppressive myeloid and regulatory T-cells in the TME while simultaneously restoring the ability of dendritic cells and cytotoxic T-cells to migrate into the tumor in several syngeneic tumor models. Importantly, anti-SEMA4D MAb enhanced the activity of co-administered immunotherapies in murine colon, head and neck (HNSCC), and melanoma models. For example, anti-SEMA4D plus anti-CTLA-4 resulted in 100% survival and 90% complete tumor rejection (CR) (p Citation Format: Elizabeth E. Evans, Holm Bussler, Crystal Mallow, Christine Reilly, Sebold Torno, Maria Scrivens, Alan Howell, Leslie Balch, John E. Leonard, Terrence L. Fisher, Clint Allen, Paul Clavijo, Gregory Lesiniski, Christina Wu, Siwen Hu-Lieskovan, Antoni Ribas, Emily Greengard, Ernest S. Smith, Maurice Zauderer. Reprogramming myeloid cells in TME with pepinemab, first-in-class semaphorin 4D MAb, enhances combination immunotherapy [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. 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引用次数: 0

摘要

目的:在临床前动物模型中,抗信号蛋白4D (SEMA4D, CD100)阻断抗体联合多种免疫疗法可增强肿瘤生长抑制。免疫检查点联合pepinemab (VX15/2503),一种人源抗sema4d抗体,目前正在几个临床试验中进行评估。方法:在同基因临床前模型中扩展机制研究SEMA4D阻断剂作为单一药物和与各种免疫治疗药物联合使用对肿瘤微环境内免疫环境的影响。通过免疫组织化学、流式细胞术、功能分析、细胞因子、趋化因子和基因表达分析来表征抗肿瘤活性和免疫应答。Pepinemab (VX15/2503)目前正在四项临床试验中作为单药或与其他免疫疗法联合进行评估:(i)在NSCLC (classic - lung) (NCT03268057)中,Pepinemab与avelumab的1b/2a期联合试验;(ii)在任何抗pd -1/PD-L1治疗进展的黑色素瘤患者中,pepinemab与nivolumab或ipilimumab的一期联合试验(NCT03373188);(iii)在pepinemab联合nivolumab或ipilimumab治疗的转移性结直肠癌和胰腺癌患者中进行的新辅助综合生物标志物试验(NCT03373188);(iv) pepinemab在患有实体瘤的儿童和患有骨肉瘤的儿童和年轻人中的1/2期试验(NCT03320330)。结果:SEMA4D通过在肿瘤-基质边缘形成屏障,限制免疫细胞浸润,促进髓源性细胞的免疫抑制活性,在肿瘤微环境中发挥多方面的作用。SEMA4D阻断抗体直接提高M1/M2比值,同时降低募集MDSC趋化因子的表达和MDSC抑制t细胞增殖的能力。在几种同基因肿瘤模型中,抗体阻断降低了TME中免疫抑制性骨髓细胞和调节性t细胞的功能,同时恢复了树突状细胞和细胞毒性t细胞迁移到肿瘤中的能力。重要的是,anti-SEMA4D MAb增强了小鼠结肠、头颈部(HNSCC)和黑色素瘤模型中共给药免疫疗法的活性。例如,抗sema4d +抗ctla -4可获得100%的存活率和90%的肿瘤完全排斥(CR) (p引用格式:Elizabeth E. Evans, Holm Bussler, Crystal Mallow, Christine Reilly, Sebold Torno, Maria Scrivens, Alan Howell, Leslie Balch, John E. Leonard, Terrence L. Fisher, Clint Allen, Paul Clavijo, Gregory Lesiniski, Christina Wu, Siwen ho - lieskovan, Antoni Ribas, Emily greenard, Ernest S. Smith, Maurice Zauderer)。用pepinemab(一流的信号素4D单抗)重编程TME中的骨髓细胞,增强联合免疫治疗[摘要]。第四届CRI-CIMT-EATI-AACR国际癌症免疫治疗会议:将科学转化为生存;2018年9月30日至10月3日;纽约,纽约。费城(PA): AACR;癌症免疫学杂志2019;7(2增刊):摘要nr PR10。
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Abstract PR10: Reprogramming myeloid cells in TME with pepinemab, first-in-class semaphorin 4D MAb, enhances combination immunotherapy
Purpose: Tumor growth inhibition by anti-semaphorin 4D (SEMA4D, CD100) blocking antibody is enhanced when combined with various immunotherapies in preclinical animal models. Immune checkpoint combinations with pepinemab (VX15/2503), a humanized anti-SEMA4D antibody, are currently being evaluated in several clinical trials. Methods: Expanded mechanistic studies in syngeneic preclinical models investigated the effect of SEMA4D blockade on immune contexture within the tumor microenvironment, as a single agent and in combination with various immunotherapy agents. Antitumor activity and immune response was characterized by immunohistochemistry, flow cytometry, functional assays, and cytokine, chemokine and gene expression analysis. Pepinemab (VX15/2503) is currently being evaluated as single agent or in combination with other immunotherapies in four clinical trials: (i) a phase 1b/2a combination trial of pepinemab with avelumab in NSCLC (CLASSICAL-Lung) (NCT03268057); (ii) a phase 1 combination trial of pepinemab with nivolumab or ipilimumab in melanoma patients who have progressed on any anti-PD-1/PD-L1 (NCT03373188); (iii) a neoadjuvant integrated biomarker trial in patients with metastatic colorectal and pancreatic cancers treated with pepinemab in combination with nivolumab or ipilimumab (NCT03373188); and (iv) a phase 1/2 trial of pepinemab in children with solid tumors and children and young adults with osteosarcoma (NCT03320330). Results: SEMA4D exerts multifaceted effects within the tumor microenvironment by creating a barrier at the tumor-stroma margin to restrict immune cell infiltration and promoting immunosuppressive activity of myeloid-derived cells. Blocking antibody to SEMA4D directly enhanced M1/M2 ratio and both reduced expression of chemokines that recruit MDSC and the ability of MDSC to suppress T-cell proliferation. Antibody blockade reduced the function of immunosuppressive myeloid and regulatory T-cells in the TME while simultaneously restoring the ability of dendritic cells and cytotoxic T-cells to migrate into the tumor in several syngeneic tumor models. Importantly, anti-SEMA4D MAb enhanced the activity of co-administered immunotherapies in murine colon, head and neck (HNSCC), and melanoma models. For example, anti-SEMA4D plus anti-CTLA-4 resulted in 100% survival and 90% complete tumor rejection (CR) (p Citation Format: Elizabeth E. Evans, Holm Bussler, Crystal Mallow, Christine Reilly, Sebold Torno, Maria Scrivens, Alan Howell, Leslie Balch, John E. Leonard, Terrence L. Fisher, Clint Allen, Paul Clavijo, Gregory Lesiniski, Christina Wu, Siwen Hu-Lieskovan, Antoni Ribas, Emily Greengard, Ernest S. Smith, Maurice Zauderer. Reprogramming myeloid cells in TME with pepinemab, first-in-class semaphorin 4D MAb, enhances combination immunotherapy [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2019;7(2 Suppl):Abstract nr PR10.
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