Guillaume Sicard, Dorian Protzenko, Sarah Giacometti, Fabrice Barlési, Joseph Ciccolini, Raphaelle Fanciullino
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Finally, an efficacy study was conducted comparing the antiproliferative performance of various schedules of anti-VEGF, Pemetrexed-Cisplatin doublet, plus anti-PD-1 (i.e., immunomonitoring-guided scheduling, concurrent dosing or a random sequence), as well as single agent anti-PD1. <b>Results:</b> Immunomonitoring showed marked differences between treatments, organs, and time points. However, harnessing tumor immunity (i.e., promoting CD8 T cells or increasing the T CD8/Treg ratio) started on D7 and peaked on D14 with the anti-VEGF followed by cytotoxics combination. Therefore, a 14-day delay between anti-VEGF/cytotoxic and anti-PD1 administration was considered the best sequence to test. Efficacy studies then confirmed that this sequence achieved higher antiproliferative efficacy compared to other treatment modalities (i.e., -71% in tumor volume compared to control). <b>Conclusions:</b> Anti-VEGF and cytotoxic agents show time-dependent immunomodulatory effects, suggesting that sequencing is a critical feature when combining these agents with immune checkpoint inhibitors. 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引用次数: 0
摘要
背景:许多肿瘤对免疫检查点抑制剂难治,但将其与细胞毒性药物联合使用有望提高敏感性。了解细胞毒素如何以及何时最有效地重新刺激肿瘤免疫有助于克服对免疫检查点抑制剂的耐药性。研究方法在移植了免疫难治性LL/2肺癌模型的C57BL/6小鼠中进行体内研究。在包括顺铂、培美曲塞和抗血管内皮生长因子(单独或联合)在内的多种治疗后,对肿瘤、脾脏和血液进行了长达 21 天的纵向免疫监测研究,以确定添加免疫检查点抑制剂的最佳时间窗。最后,还进行了一项疗效研究,比较了抗血管内皮生长因子、培美曲塞-顺铂双药加抗PD-1(即免疫监测指导下的排期、同时给药或随机排期)以及单药抗PD-1的抗增殖性能。结果显示免疫监测显示不同治疗、器官和时间点之间存在明显差异。然而,利用肿瘤免疫(即促进 CD8 T 细胞或增加 T CD8/Treg 比率)始于第 7 天,在抗血管内皮生长因子和细胞毒联合治疗的第 14 天达到高峰。因此,抗血管内皮生长因子/细胞毒素和抗 PD1 的给药间隔 14 天被认为是最佳的试验顺序。随后进行的疗效研究证实,与其他治疗方式相比,这种顺序能取得更高的抗增殖疗效(即与对照组相比,肿瘤体积减少 71%)。结论抗血管内皮生长因子和细胞毒性药物显示出时间依赖性免疫调节效应,这表明在将这些药物与免疫检查点抑制剂联合使用时,排序是一个关键特征。一项疗效研究证实,与同时给药相比,序贯疗法能进一步增强肺癌模型的抗增殖效果,并能部分逆转对细胞毒性药物和抗 PD1 的耐药性。
Overcoming immuno-resistance by rescheduling anti-VEGF/cytotoxics/anti-PD-1 combination in lung cancer model.
Background: Many tumors are refractory to immune checkpoint inhibitors, but their combination with cytotoxics is expected to improve sensitivity. Understanding how and when cytotoxics best re-stimulate tumor immunity could help overcome resistance to immune checkpoint inhibitors. Methods:In vivo studies were performed in C57BL/6 mice grafted with immune-refractory LL/2 lung cancer model. A longitudinal immunomonitoring study on tumor, spleen, and blood after multiple treatments including Cisplatin, Pemetrexed, and anti-VEGF, either alone or in combination, was performed, spanning a period of up to 21 days, to determine the optimal time window during which immune checkpoint inhibitors should be added. Finally, an efficacy study was conducted comparing the antiproliferative performance of various schedules of anti-VEGF, Pemetrexed-Cisplatin doublet, plus anti-PD-1 (i.e., immunomonitoring-guided scheduling, concurrent dosing or a random sequence), as well as single agent anti-PD1. Results: Immunomonitoring showed marked differences between treatments, organs, and time points. However, harnessing tumor immunity (i.e., promoting CD8 T cells or increasing the T CD8/Treg ratio) started on D7 and peaked on D14 with the anti-VEGF followed by cytotoxics combination. Therefore, a 14-day delay between anti-VEGF/cytotoxic and anti-PD1 administration was considered the best sequence to test. Efficacy studies then confirmed that this sequence achieved higher antiproliferative efficacy compared to other treatment modalities (i.e., -71% in tumor volume compared to control). Conclusions: Anti-VEGF and cytotoxic agents show time-dependent immunomodulatory effects, suggesting that sequencing is a critical feature when combining these agents with immune checkpoint inhibitors. An efficacy study confirmed that sequencing treatments further enhance antiproliferative effects in lung cancer models compared to concurrent dosing and partly reverse the resistance to cytotoxics and anti-PD1.
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