Myofibroblast-derived extracellular vesicles facilitate cancer stemness of hepatocellular carcinoma via transferring ITGA5 to tumor cells

IF 27.7 1区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Cancer Pub Date : 2024-11-21 DOI:10.1186/s12943-024-02170-0

Yang Xiao, Ping Tao, Keke Zhang, Liuyan Chen, Jinyu Lv, Zhiwei Chen, Lu He, Hongling Jia, Jian Sun, Mingrong Cao, Jian Hong, Chen Qu

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引用次数: 0

Abstract

Myofibroblasts constitute a significant component of the tumor microenvironment (TME) and play a pivotal role in the progression of hepatocellular carcinoma (HCC). Integrin α5 (ITGA5) is a crucial regulator in myofibroblasts of malignant tumors. Therefore, the potential of ITGA5 as a novel target for the therapeutic strategy of HCC should be investigated. Digital scanning and analysis of the HCC tissue microarray were performed to locate the distribution of ITGA5 and conduct the prognosis analysis. CRISPR Cas9-mediated ITGA5 knockout was performed to establish the ITGA5-KO myofibroblast cell line. Extracellular vesicles (EVs) derived from LX2 were extracted for the treatment of HCC cells. Subsequently, the sphere-forming ability and the stemness markers expression of the treated HCC cells were examined. An orthotopic HCC mouse model with fibrotic injury was constructed to test the outcomes of ITGA5-targeting therapy and its efficacy in the programmed death-ligand 1 (PD-L1) treatment. Co-immunoprecipitation/mass spectrometry and transcriptome data were integrated to delve into the mechanism. The tissue microarray results revealed that ITGA5 was highly enriched in the stromal myofibroblasts of HCC tissues and contributed to enhanced tumor progression and poor prognosis. Notably, ITGA5 transmission via extracellular vesicles (EVs) from myofibroblasts to HCC cells induced the acquisition of cancer stem cell-like properties. Mechanistically, ITGA5 directly bind to YES1, facilitating the activation of YES1 and its downstream pathways, thereby enhancing the stemness of HCC cells. Furthermore, the blockade of ITGA5 impeded tumor progression driven by ITGA5+ myofibroblasts and enhanced the efficacy of treatment with PD-L1 in a mouse model of HCC. Our findings elucidated a novel mechanism by which the EV-mediated transfer of ITGA5 from myofibroblasts to tumor cells augmented HCC stemness. ITGA5-targeting therapy helped prevent the progression of HCC and improved the efficacy of PD-L1 treatment.

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来源于肌成纤维细胞的细胞外囊泡通过向肿瘤细胞转移 ITGA5 促进肝细胞癌的癌症干细胞化

肌成纤维细胞是肿瘤微环境（TME）的重要组成部分，在肝细胞癌（HCC）的发展过程中起着关键作用。整合素α5（ITGA5）是恶性肿瘤肌成纤维细胞的重要调节因子。因此，应研究 ITGA5 作为 HCC 治疗策略新靶点的潜力。研究人员对HCC组织芯片进行了数字扫描和分析，以确定ITGA5的分布并进行预后分析。通过CRISPR Cas9介导的ITGA5基因敲除，建立了ITGA5-KO肌成纤维细胞系。提取来自LX2的胞外小泡（EVs）处理HCC细胞。随后，研究人员检测了处理后的 HCC 细胞的成球能力和干性标志物的表达。为了检测ITGA5靶向治疗的结果及其在程序性死亡配体1（PD-L1）治疗中的疗效，研究人员构建了带有纤维化损伤的HCC小鼠模型。研究人员整合了免疫沉淀/质谱和转录组数据，以深入研究其机制。组织芯片研究结果显示，ITGA5高度富集于HCC组织的基质肌成纤维细胞中，并导致肿瘤恶化和预后不良。值得注意的是，ITGA5通过胞外囊泡（EVs）从肌成纤维细胞传递到HCC细胞，诱导了肿瘤干细胞样特性的获得。从机制上讲，ITGA5直接与YES1结合，促进了YES1及其下游通路的激活，从而增强了HCC细胞的干性。此外，在小鼠HCC模型中，阻断ITGA5可阻碍由ITGA5+肌成纤维细胞驱动的肿瘤进展，并增强PD-L1治疗的疗效。我们的研究结果阐明了一种新的机制，即由EV介导的ITGA5从肌成纤维细胞转移到肿瘤细胞可增强HCC干性。ITGA5靶向疗法有助于防止HCC的恶化，并提高了PD-L1治疗的疗效。

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

Molecular Cancer 医学-生化与分子生物学

CiteScore

54.90

自引率

2.70%

发文量

224

审稿时长

2 months

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