Yap methylation-induced FGL1 expression suppresses anti-tumor immunity and promotes tumor progression in KRAS-driven lung adenocarcinoma

IF 20.1 1区 医学 Q1 ONCOLOGY Cancer Communications Pub Date : 2024-09-28 DOI:10.1002/cac2.12609
Ji Jiang, Pengfei Ye, Ningning Sun, Weihua Zhu, Mei Yang, Manman Yu, Jingjing Yu, Hui Zhang, Zijie Gao, Ningjie Zhang, Shijie Guo, Yuru Ji, Siqi Li, Cuncun Zhang, Sainan Miao, Mengqi Chai, Wenmin Liu, Yue An, Jian Hong, Wei Wei, Shihao Zhang, Huan Qiu
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Abstract

Background

Despite significant strides in lung cancer immunotherapy, the response rates for Kirsten rat sarcoma viral oncogene homolog (KRAS)-driven lung adenocarcinoma (LUAD) patients remain limited. Fibrinogen-like protein 1 (FGL1) is a newly identified immune checkpoint target, and the study of related resistance mechanisms is crucial for improving the treatment outcomes of LUAD patients. This study aimed to elucidate the potential mechanism by which FGL1 regulates the tumor microenvironment in KRAS-mutated cancer.

Methods

The expression levels of FGL1 and SET1 histone methyltransferase (SET1A) in lung cancer were assessed using public databases and clinical samples. Lentiviruses were constructed for transduction to overexpress or silence FGL1 in lung cancer cells and mouse models. The effects of FGL1 and Yes-associated protein (Yap) on the immunoreactivity of cytotoxic T cells in tumor tissues were evaluated using immunofluorescence staining and flow cytometry. Chromatin immunoprecipitation and dual luciferase reporter assays were used to study the SET1A-directed transcriptional program.

Results

Upregulation of FGL1 expression in KRAS-mutated cancer was inversely correlated with the infiltration of CD8+ T cells. Mechanistically, KRAS activated extracellular signal-regulated kinase 1/2 (ERK1/2), which subsequently phosphorylated SET1A and increased its stability and nuclear localization. SET1A-mediated methylation of Yap led to Yap sequestration in the nucleus, thereby promoting Yap-induced transcription of FGL1 and immune evasion in KRAS-driven LUAD. Notably, dual blockade of programmed cell death-1 (PD-1) and FGL1 further increased the therapeutic efficacy of anti-PD-1 immunotherapy in LUAD patients.

Conclusion

FGL1 could be used as a diagnostic biomarker of KRAS-mutated lung cancer, and targeting the Yap-FGL1 axis could increase the efficacy of anti-PD-1 immunotherapy.

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Yap甲基化诱导的FGL1表达抑制了KRAS驱动的肺腺癌中的抗肿瘤免疫并促进了肿瘤进展。
背景:尽管肺癌免疫疗法取得了长足进步,但克氏鼠肉瘤病毒癌基因同源物(KRAS)驱动的肺腺癌(LUAD)患者的应答率仍然有限。纤维蛋白原样蛋白1(FGL1)是新发现的免疫检查点靶点,研究相关的耐药机制对于改善LUAD患者的治疗效果至关重要。本研究旨在阐明FGL1调控KRAS突变癌症肿瘤微环境的潜在机制:方法:利用公共数据库和临床样本评估了FGL1和SET1组蛋白甲基转移酶(SET1A)在肺癌中的表达水平。构建了慢病毒,用于在肺癌细胞和小鼠模型中转导过表达或沉默FGL1。利用免疫荧光染色和流式细胞术评估了FGL1和Yes相关蛋白(Yap)对肿瘤组织中细胞毒性T细胞免疫活性的影响。染色质免疫沉淀和双荧光素酶报告实验用于研究 SET1A 引导的转录程序:结果:KRAS突变癌症中FGL1表达的上调与CD8+ T细胞的浸润成反比。从机理上讲,KRAS激活了细胞外信号调节激酶1/2(ERK1/2),ERK1/2随后磷酸化了SET1A,增加了其稳定性和核定位。SET1A 介导的 Yap 甲基化导致 Yap 封存在细胞核中,从而促进 Yap 诱导的 FGL1 转录和 KRAS 驱动的 LUAD 的免疫逃避。值得注意的是,程序性细胞死亡-1(PD-1)和FGL1的双重阻断进一步提高了抗PD-1免疫疗法对LUAD患者的疗效:结论:FGL1可作为KRAS突变肺癌的诊断生物标记物,靶向Yap-FGL1轴可提高抗PD-1免疫疗法的疗效。
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
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.
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