非小细胞肺癌中的 EGFR 致癌突变通过上调 CD47 来损害巨噬细胞的吞噬作用并介导固有免疫逃避。
EGFR Oncogenic Mutations in NSCLC Impair Macrophage Phagocytosis and Mediate Innate Immune Evasion Through Up-Regulation of CD47.
机构信息
Department of Medical Oncology, State Key Laboratory of Oncology in South China, Guangdong Provincial Clinical Research Center for Cancer, Sun Yat-sen University Cancer Center, Guangzhou, People's Republic of China; Department of Thoracic Oncology, the Cancer Center of the Fifth Affiliated Hospital of Sun Yat-sen University, Zhuhai, Guangdong, People's Republic of China.
Department of Medical Oncology, State Key Laboratory of Oncology in South China, Guangdong Provincial Clinical Research Center for Cancer, Sun Yat-sen University Cancer Center, Guangzhou, People's Republic of China.
出版信息
J Thorac Oncol. 2024 Aug;19(8):1186-1200. doi: 10.1016/j.jtho.2024.03.019. Epub 2024 Mar 27.
INTRODUCTION
EGFR-mutated NSCLC is characterized by an immunosuppressive microenvironment that confers limited clinical effectiveness to anti-PD-1 or PD-L1 antibodies. Despite the discouraging outcomes of immunotherapy, novel immune checkpoints are constantly emerging, among which the specific vulnerability for therapeutic intervention in the context of EGFR-mutated NSCLC remains unresolved.
METHODS
Data sets of patient- and cell line-levels were used for screening and mutual validation of association between EGFR mutation and a panel of immune checkpoint-related genes. Regulatory mechanism was elucidated through in vitro manipulation of EGFR signaling pathway and evaluated by immunoblot analysis, quantitative polymerase chain reaction, flow cytometry, immunofluorescence staining, and chromatin immunoprecipitation. In vivo investigation of different therapeutic strategies were conducted using both immunocompetent and immunodeficient mouse models.
RESULTS
Among all screened immune checkpoints, CD47 emerged as the candidate most relevant to EGFR activation. Mechanistically, EGFR mutation constitutively activated downstream ERK and AKT pathways to respectively up-regulate the transcriptional factors c-Myc and NF-κB, both of which structurally bound to the promotor region of CD47 and actively transcribed this "don't eat me" signal. Impaired macrophage phagocytosis was observed on introduction of EGFR-sensitizing mutations in NSCLC cell line models, whereas CD47 blockade restored the phagocytic capacity and augmented tumor cell killing in both in vitro and in vivo models. Remarkably, the combination of anti-CD47 antibody with EGFR tyrosine kinase inhibitor revealed an additive antitumor activity compared with monotherapy of either antitumor agent in both immunocompetent and adaptive immunity-deficient mouse models.
CONCLUSIONS
EGFR-sensitizing mutation facilitates NSCLC's escape from innate immune attack through up-regulating CD47. Combination therapy incorporating CD47 blockade holds substantial promise for clinical translation in developing more effective therapeutic approaches against EGFR-mutant NSCLC.
简介
EGFR 突变型 NSCLC 的特征是免疫抑制微环境,这使得抗 PD-1 或 PD-L1 抗体的临床疗效有限。尽管免疫疗法的结果令人沮丧,但新的免疫检查点不断涌现,其中在 EGFR 突变型 NSCLC 背景下治疗干预的特定脆弱性仍未得到解决。
方法
使用患者和细胞系水平的数据集筛选和相互验证 EGFR 突变与一系列免疫检查点相关基因之间的关联。通过体外操纵 EGFR 信号通路阐明调控机制,并通过免疫印迹分析、定量聚合酶链反应、流式细胞术、免疫荧光染色和染色质免疫沉淀进行评估。使用免疫功能正常和免疫缺陷的小鼠模型进行不同治疗策略的体内研究。
结果
在所有筛选的免疫检查点中,CD47 是与 EGFR 激活最相关的候选物。从机制上讲,EGFR 突变持续激活下游 ERK 和 AKT 通路,分别上调转录因子 c-Myc 和 NF-κB,它们都与 CD47 的启动子区域结合,并积极转录这个“不要吃我”信号。在 NSCLC 细胞系模型中引入 EGFR 敏化突变时,观察到巨噬细胞吞噬作用受损,而 CD47 阻断恢复了体外和体内模型中的吞噬能力,并增强了肿瘤细胞杀伤作用。值得注意的是,与单药治疗相比,抗 CD47 抗体与 EGFR 酪氨酸激酶抑制剂联合使用在免疫功能正常和适应性免疫缺陷小鼠模型中均显示出相加的抗肿瘤活性。
结论
EGFR 敏化突变通过上调 CD47 促进 NSCLC 逃避先天免疫攻击。包含 CD47 阻断的联合治疗为开发针对 EGFR 突变型 NSCLC 的更有效的治疗方法提供了实质性的临床转化前景。
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