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首页> 外文期刊>Molecular cancer therapeutics >PD-1/PD-L1 Immune Checkpoint Inhibition with Radiation in Bladder Cancer: In Situ and Abscopal Effects
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PD-1/PD-L1 Immune Checkpoint Inhibition with Radiation in Bladder Cancer: In Situ and Abscopal Effects

机译:PD-1 / PD-L1免疫检查点抑制在膀胱癌中辐射:原位和俯视效应

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The combination of radiation with immune checkpoint inhibitors was reported in some cancers to have synergic effects both locally and distally. Our aim was to assess this combined therapy on both radiated and nonradiated bladder tumors and to characterize the immune landscape within the tumor microenvironment. Murine bladder cancer cells (MB49) were injected subcutaneously in both flanks of C57BL/6 mice. Mice were randomly assigned to the following treatments: placebo, anti-PD-L1 (four intraperitoneal injections over 2 weeks), radiation to right flank (10 Gy in two fractions), or radiation+anti-PD-L1. Tumor digestion, flow cytometry, and qPCR were performed. Log-rank analysis was used for statistical significance. Radiation+anti-PD-L1 group demonstrated statistically significant slower tumor growth rate both in the radiated and non-irradiated tumors (P < 0.001). Survival curves demonstrated superior survival in the combination group compared with each treatment alone (P = 0.02). Flow cytometry showed increased infiltration of immunosuppressive cells as well as CTL in the radiation and combination groups (P = 0.04). Ratio of immunosuppressive cells to CTL shifted in favor of cytotoxic activity in the combination arm (P < 0.001). The qPCR analysis revealed down-regulation of immunosuppressive genes (CCL22, IL22, and IL13), as well as upregulation of markers of CTL activation (CXCL9, GZMA, and GZMB) within both the radiated and distant tumors within the combination group. Combining radiation with immune checkpoint inhibitor provided better response in the radiated tumors and also the distant tumors along with a shift within the tumor microenvironment favoring cytotoxic activity. These findings demonstrate a possible abscopal effect in urothelial carcinoma with combination therapy.
机译:在一些癌症中报道了具有免疫检查点抑制剂的辐射的组合,以在局部和远端具有协同作用。我们的目的是评估辐射和非丙醇肿瘤的这种组合治疗,并表征肿瘤微环境中的免疫景观。在C57BL / 6小鼠的两侧皮下注射鼠膀胱癌细胞(MB49)。将小鼠随机分配给以下处理:安慰剂,抗PD-L1(2周内四个腹腔注射),辐射到右侧(两个级分中10Gy),或辐射+抗PD-L1。进行肿瘤消化,流式细胞术和QPCR。对数秩分析用于统计显着性。辐射+抗PD-L1组在辐射和非照射肿瘤中表现出统计学上显着的肿瘤生长速率(P <0.001)。生存曲线与单独的每种处理相比,组合组的卓越存活率(p = 0.02)。流式细胞术显示辐射和组合组中免疫抑制细胞以及CTL的渗透增加(P = 0.04)。免疫抑制细胞与CTL的比例转移有利于组合臂中的细胞毒性活性(P <0.001)。 QPCR分析揭示了免疫抑制基因(CCL22,IL22和IL13)的下调,以及在组合组内的辐射和远处肿瘤中的CTL活化(CXCL9,GZMA和GZMB)的标志物上调。将辐射与免疫检查点抑制剂组合在辐射肿瘤中提供更好的响应以及远处肿瘤以及有利于细胞毒性活性的肿瘤微环境的转变。这些研究结果表明了尿路上皮癌的可能俯视效应,组合治疗。

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