CD24 is a promising immunotherapeutic target for enhancing efficacy of third-generation EGFR-TKIs on EGFR-mutated lung cancer.

IF 24.9 1区医学 Q1 ONCOLOGY

Cancer Communications Pub Date : 2025-10-13 DOI:10.1002/cac2.70068

Jiaqi Liang, Guoshu Bi, Xiaolong Huang, Zhijie Xu, Yiwei Huang, Yunyi Bian, Guangyao Shan, Wei Guo, Yuanliang Yan, Qihai Sui, Xiaodong Yang, Zhencong Chen, Tao Lu, Huan Zhang, Qun Wang, Wei Jiang, Cheng Zhan

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引用次数: 0

Abstract

Background: Third-generation epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) show initial efficacy in EGFR-mutated lung cancer, but residual disease persists. This study aimed to investigate cluster of differentiation 24 (CD24) as a translational immunotherapeutic target for enhancing third-generation EGFR-TKI efficacy.

Methods: We conducted RNA-sequencing (RNA-seq) on drug-responsive, drug-tolerant persister, and drug-resistant cells to identify therapeutic targets to pair with EGFR-TKIs. For validation, we integrated single-cell RNA-seq data from 29 lung cancer specimens and used single-nucleus RNA-seq and immunohistochemistry on clinical residual tumor samples following TKI therapy (TKI-residual). With CRISPR/Cas9, we studied the effect of CD24 on proliferation and phagocytic clearance during EGFR-TKI treatment. We tested CD24 knockout or ATG-031 (a first-in-class CD24 antibody) with EGFR-TKIs in vitro, xenografts, and spontaneous lung cancer models. To explore mechanisms, we used DNA affinity precipitation, chromatin immunoprecipitation sequencing, and luciferase assays to identify transcription factors regulating CD24. Co-immunoprecipitation combined with mass spectrometry and phosphoproteomics were used to study YIN-YANG-1 (YY1) S247 phosphorylation's expression and function, while kinase inhibitors assessed upstream phosphorylation of YY1 S247 and its regulation of CD24.

Results: CD24 expression rose in drug-responsive, -resistant, and -tolerant lung cancer cells and post-EGFR-TKI treatment clinical specimens. This elevation promoted cell proliferation and shielded tumor cells from macrophage-mediated phagocytosis. Genetic depletion of CD24 or treatment with ATG-031 significantly enhanced phagocytosis and tumor eradication in vitro, in xenografts, and in mice harboring EGFRL858R·T790M-driven spontaneous lung tumors. Furthermore, we revealed that YY1 S247 phosphorylation was responsible for the upregulation of CD24 upon EGFR-TKI treatment, facilitating YY1 dimerization and the formation of promoter-enhancer loops that regulate CD24 expression.

Conclusions: CD24 is a promising target in EGFR-mutated lung cancers, potentially enhancing efficacy of third-generation EGFR-TKIs.

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CD24是提高第三代EGFR-TKIs治疗egfr突变肺癌疗效的有希望的免疫治疗靶点。

背景：第三代表皮生长因子受体（EGFR）酪氨酸激酶抑制剂（TKIs）在EGFR突变的肺癌中显示出初步疗效，但残留疾病仍然存在。本研究旨在探讨CD24作为提高第三代EGFR-TKI疗效的转化性免疫治疗靶点。方法：我们对药物反应性、耐药持久性和耐药细胞进行rna测序（RNA-seq），以确定与EGFR-TKIs配对的治疗靶点。为了验证，我们整合了来自29例肺癌标本的单细胞RNA-seq数据，并对TKI治疗后的临床残留肿瘤样本（TKI-residual）进行了单核RNA-seq和免疫组织化学分析。利用CRISPR/Cas9，我们研究了在EGFR-TKI治疗期间CD24对细胞增殖和吞噬清除的影响。我们在体外、异种移植和自发性肺癌模型中对EGFR-TKIs进行了CD24敲除或ATG-031（一种一流的CD24抗体）测试。为了探索机制，我们使用DNA亲和沉淀、染色质免疫沉淀测序和荧光素酶测定来鉴定调节CD24的转录因子。采用免疫共沉淀法结合质谱法和磷酸化蛋白质组学研究了YIN-YANG-1 (YY1) S247磷酸化的表达和功能，激酶抑制剂评估了YY1 S247上游磷酸化及其对CD24的调控。结果：CD24在耐药、耐药、耐药肺癌细胞及egfr - tki治疗后临床标本中表达升高。这种升高促进了细胞增殖，并保护肿瘤细胞免受巨噬细胞介导的吞噬作用。CD24基因缺失或ATG-031治疗可显著增强体外、异种移植物和携带EGFRL858R·t790m驱动的自发性肺肿瘤的小鼠的吞噬和肿瘤根除。此外，我们发现YY1 S247磷酸化是EGFR-TKI处理时CD24上调的原因，促进YY1二聚化和形成调节CD24表达的启动子-增强子环。结论：CD24是egfr突变肺癌的一个有希望的靶点，可能增强第三代EGFR-TKIs的疗效。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cancer Communications Biochemistry, Genetics and Molecular Biology-Cancer Research

CiteScore

25.50

自引率

4.30%

发文量

153

审稿时长

4 weeks

期刊介绍： Cancer Communications is an open access, peer-reviewed online journal that encompasses basic, clinical, and translational cancer research. The journal welcomes submissions concerning clinical trials, epidemiology, molecular and cellular biology, and genetics.