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多组学分析揭示了免疫原性细胞死亡衍生的SCN5A在肝细胞癌中的诊断和治疗价值。

Multi-omics Analysis Revealed the Diagnostic and Therapeutic Value of Immunogenic Cell Death-derived SCN5A in Hepatocellular Carcinoma.

作者信息

Liang Zicheng, Tan Wei, Fang Xiayi, Zhang Zhen, Tan Xiaoning, Zeng Puhua

机构信息

Graduate School, Hunan University of Chinese Medicine, Changsha, 410208, China.

Cancer Research Institute, Hunan Academy of Chinese Medicine, Changsha, 410006, China.

出版信息

Mol Biotechnol. 2025 Apr 24. doi: 10.1007/s12033-025-01444-2.

Abstract

This study explores the diagnostic and therapeutic potential of SCN5A, an immunogenic cell death (ICD)-related gene, in hepatocellular carcinoma (HCC). Integrated analysis of four databases identified 62 ICD-associated genes (ICDGs), with SCN5A emerging as a key player linked to HCC prognosis and immune microenvironment modulation. Single-cell RNA sequencing revealed correlations between ICD activity and tumor immune dynamics. Bulk RNA sequencing categorized HCC into distinct molecular subtypes with varied immunological features. Machine learning-based prognostic models highlighted SCN5A's clinical relevance, supported by phenome-wide association studies connecting SCN5A to liver malignancies. Experimental validation showed elevated SCN5A expression in HepG2 cells, where siRNA-mediated knockdown significantly impaired proliferation (CCK8 and colony formation assays), invasion (Transwell), migration (wound healing), and apoptotic index (TUNEL assays and Bax, Bcl-2 expression). Molecular docking identified propafenone as a high-affinity SCN5A binder, which suppressed SCN5A expression and mirrored knockdown effects by inhibiting HCC cell growth and metastasis while promoting apoptosis. These findings position SCN5A as a novel ICD-linked biomarker and therapeutic target in HCC, with propafenone repurposing showing promising anti-tumor efficacy through SCN5A modulation. This work bridges computational biology with experimental oncology to advance ICD-targeted HCC treatment strategies.

摘要

本研究探讨了免疫原性细胞死亡(ICD)相关基因SCN5A在肝细胞癌(HCC)中的诊断和治疗潜力。对四个数据库的综合分析确定了62个ICD相关基因(ICDG),其中SCN5A成为与HCC预后和免疫微环境调节相关的关键因素。单细胞RNA测序揭示了ICD活性与肿瘤免疫动力学之间的相关性。批量RNA测序将HCC分为具有不同免疫特征的不同分子亚型。基于机器学习的预后模型突出了SCN5A的临床相关性,全表型关联研究将SCN5A与肝脏恶性肿瘤联系起来,为其提供了支持。实验验证显示HepG2细胞中SCN5A表达升高,其中siRNA介导的敲低显著损害增殖(CCK8和集落形成试验)、侵袭(Transwell)、迁移(伤口愈合)和凋亡指数(TUNEL试验以及Bax、Bcl-2表达)。分子对接确定普罗帕酮为高亲和力SCN5A结合剂,其通过抑制HCC细胞生长和转移同时促进凋亡来抑制SCN5A表达并反映敲低效应。这些发现将SCN5A定位为HCC中一种新型的ICD相关生物标志物和治疗靶点,普罗帕酮的重新利用通过调节SCN5A显示出有前景的抗肿瘤疗效。这项工作将计算生物学与实验肿瘤学相结合,以推进针对ICD的HCC治疗策略。

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