Department of Oncology, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei, P. R. China.
Cancer Commun (Lond). 2023 Apr;43(4):435-454. doi: 10.1002/cac2.12412. Epub 2023 Feb 28.
Immune checkpoint inhibitors (ICIs) targeting programmed cell death protein 1 (PD-1) and programmed death-ligand 1 (PD-L1) have shown a moderate response in colorectal cancer (CRC) with deficient mismatch repair (dMMR) functions and poor response in patients with proficient MMR (pMMR). pMMR tumors are generally immunogenically "cold", emphasizing combination strategies to turn the "cold" tumor "hot" to enhance the efficacy of ICIs. ATR inhibitors (ATRi) have been proven to cooperate with radiation to promote antitumor immunity, but it is unclear whether ATRi could facilitate the efficacy of IR and ICI combinations in CRCs. This study aimed to investigate the efficacy of combining ATRi, irradiation (IR), and anti-PD-L1 antibodies in CRC mouse models with different microsatellite statuses.
The efficacy of combining ATRi, IR, and anti-PD-L1 antibodies was evaluated in CRC tumors. The tumor microenvironment and transcriptome signatures were investigated under different treatment regimens. The mechanisms were explored via cell viability assay, flow cytometry, immunofluorescence, immunoblotting, co-immunoprecipitation, and real-time quantitative PCR in multiple murine and human CRC cell lines.
Combining ATRi berzosertib and IR enhanced CD8 T cell infiltration and enhanced the efficacy of anti-PD-L1 therapy in mouse CRC models with different microsatellite statuses. The mechanistic study demonstrated that IR + ATRi could activate both the canonical cGAS-STING-pTBK1/pIRF3 axis by increasing cytosolic double-stranded DNA levels and the non-canonical STING signaling by attenuating SHP1-mediated inhibition of the TRAF6-STING-p65 axis, via promoting SUMOylation of SHP1 at lysine 127. By boosting the STING signaling, IR + ATRi induced type I interferon-related gene expression and strong innate immune activation and reinvigorated the cold tumor microenvironment, thus facilitating immunotherapy.
The combination of ATRi and IR could facilitate anti-PD-L1 therapy by promoting STING signaling in CRC models with different microsatellite statuses. The new combination strategy raised by our study is worth investigating in the management of CRC.
针对程序性细胞死亡蛋白 1(PD-1)和程序性死亡配体 1(PD-L1)的免疫检查点抑制剂(ICIs)在错配修复缺陷(dMMR)功能的结直肠癌(CRC)中显示出中等反应,而在具有良好错配修复(pMMR)功能的患者中反应较差。pMMR 肿瘤通常具有免疫原性“冷”,强调联合策略将“冷”肿瘤“热”化,以提高 ICI 的疗效。ATR 抑制剂(ATRi)已被证明可与辐射合作促进抗肿瘤免疫,但尚不清楚 ATRi 是否能促进 CRC 中 IR 和 ICI 联合的疗效。本研究旨在探讨 ATRi、辐射(IR)和抗 PD-L1 抗体联合应用于具有不同微卫星状态的 CRC 小鼠模型中的疗效。
评估了 ATRi、IR 和抗 PD-L1 抗体联合应用于 CRC 肿瘤的疗效。在不同治疗方案下研究了肿瘤微环境和转录组特征。通过细胞活力测定、流式细胞术、免疫荧光、免疫印迹、共免疫沉淀和实时定量 PCR 在多种鼠和人 CRC 细胞系中探索了机制。
ATR 抑制剂 berzosertib 与 IR 联合应用增强了 CD8 T 细胞浸润,并增强了具有不同微卫星状态的小鼠 CRC 模型中抗 PD-L1 治疗的疗效。机制研究表明,IR+ATRi 可通过增加细胞溶质双链 DNA 水平激活经典的 cGAS-STING-pTBK1/pIRF3 轴,同时通过削弱 SHP1 介导的 TRAF6-STING-p65 轴抑制来激活非经典的 STING 信号,通过促进 SHP1 赖氨酸 127 的 SUMO 化。通过增强 STING 信号,IR+ATRi 诱导 I 型干扰素相关基因表达和强烈的固有免疫激活,并重新激活冷肿瘤微环境,从而促进免疫治疗。
ATR 抑制剂和 IR 的联合应用可通过促进 CRC 模型中 STING 信号来促进抗 PD-L1 治疗。本研究提出的新联合策略值得在 CRC 的管理中进行研究。
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