Exploration of signature-related FAM genes and correlation between FAM50A expression and the pathogenesis and prognosis of hepatocellular carcinoma.

IF 1.7 4区医学 Q4 ONCOLOGY

Translational cancer research Pub Date : 2025-08-31 Epub Date: 2025-08-25 DOI:10.21037/tcr-2025-171

Shaohan Wu, Sijun Chen, Xiaofang Sun, Xujian Chen

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引用次数: 0

Abstract

Background: Hepatocellular carcinoma (HCC) ranks among the deadliest malignancies worldwide, with limited therapeutic options and poor prognosis for advanced-stage patients. The family with sequence similarity (FAM) genes are expected to be potential regulators in tumorigenesis, but their roles in HCC remain poorly understood. This study aimed to systematically investigate the expression profiles and functional roles of FAM genes in HCC.

Methods: We leveraged multiple databases, including The Cancer Genome Atlas (TCGA), Genotype-Tissue Expression (GTEx), International Cancer Genome Consortium (ICGC), Gene Expression Omnibus (GEO), Human Protein Atlas (HPA), and Clinical Proteomic Tumor Analysis Consortium (CPTAC), to assess the expression patterns, prognostic implications, DNA methylation, genomic alterations, and associated tumor immune microenvironments of FAM genes. Differentially expressed genes were pinpointed using the DESeq2 package. Least absolute shrinkage and selection operator (LASSO) Cox regression and a nomogram model were employed to identify prognostic FAM genes and estimate the survival outcomes for HCC patients. We performed tissue microarrays and immunohistochemistry on samples from 48 HCC patients to evaluate FAM50A expression. FAM50A was also knocked down in HCC cell lines to investigate its biological functions.

Results: Five overexpressed and signature-related FAM genes (FAM50A, FAM83D, FAM104B, FAM220A, and FAM222B) were identified and validated at both mRNA and protein levels. Elevated FAM50A expression was linked to advanced tumor stage, higher grade, and unfavorable prognosis. The constructed prognostic nomogram accurately predicted 1- and 3-year survival outcomes based on tumor stage, status, and FAM50A expression levels. Pathways enriched in FAM50A co-expressed genes included RNA processing, oxidative phosphorylation, and cell cycle regulation. Additionally, FAM50A expression was associated with immune cell infiltration and immune checkpoint activity. Knockdown of FAM50A led to the suppression of HCC cell proliferation, migration, and invasion.

Conclusions: This study identifies five FAM genes with prognostic relevance in HCC, among which FAM50A emerges as a potential independent prognostic biomarker and therapeutic target.

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探讨特征相关FAM基因及FAM50A表达与肝细胞癌发病及预后的关系。

背景：肝细胞癌（HCC）是世界范围内最致命的恶性肿瘤之一，晚期患者的治疗选择有限，预后差。具有序列相似性（FAM）基因的家族有望成为肿瘤发生的潜在调节因子，但它们在HCC中的作用仍然知之甚少。本研究旨在系统探讨FAM基因在HCC中的表达谱及其功能作用。方法：我们利用多个数据库，包括癌症基因组图谱（TCGA）、基因型-组织表达（GTEx）、国际癌症基因组联盟（ICGC）、基因表达综合（GEO）、人类蛋白质图谱（HPA）和临床蛋白质组学肿瘤分析联盟（CPTAC），来评估FAM基因的表达模式、预后意义、DNA甲基化、基因组改变和相关的肿瘤免疫微环境。使用DESeq2包确定差异表达基因。采用最小绝对收缩和选择算子（LASSO） Cox回归和nomogram模型来鉴定预后FAM基因并估计HCC患者的生存结果。我们对48例HCC患者的样本进行了组织微阵列和免疫组化，以评估FAM50A的表达。FAM50A在HCC细胞系中也被敲除以研究其生物学功能。结果：在mRNA和蛋白水平上鉴定并验证了5个过表达和签名相关的FAM基因（FAM50A、FAM83D、FAM104B、FAM220A和FAM222B）。FAM50A表达升高与肿瘤分期晚期、分级高、预后不良有关。构建的预后nomogram基于肿瘤分期、状态和FAM50A表达水平准确预测1年和3年的生存结果。FAM50A共表达基因富集的途径包括RNA加工、氧化磷酸化和细胞周期调控。此外，FAM50A的表达与免疫细胞浸润和免疫检查点活性有关。FAM50A基因敲低可抑制HCC细胞的增殖、迁移和侵袭。结论：本研究确定了5个与HCC预后相关的FAM基因，其中FAM50A成为潜在的独立预后生物标志物和治疗靶点。

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

Translational cancer research ONCOLOGY-

CiteScore

2.10

自引率

0.00%

发文量

252

期刊介绍： Translational Cancer Research (Transl Cancer Res TCR; Print ISSN: 2218-676X; Online ISSN 2219-6803; http://tcr.amegroups.com/) is an Open Access, peer-reviewed journal, indexed in Science Citation Index Expanded (SCIE). TCR publishes laboratory studies of novel therapeutic interventions as well as clinical trials which evaluate new treatment paradigms for cancer; results of novel research investigations which bridge the laboratory and clinical settings including risk assessment, cellular and molecular characterization, prevention, detection, diagnosis and treatment of human cancers with the overall goal of improving the clinical care of cancer patients. The focus of TCR is original, peer-reviewed, science-based research that successfully advances clinical medicine toward the goal of improving patients'' quality of life. The editors and an international advisory group of scientists and clinician-scientists as well as other experts will hold TCR articles to the high-quality standards. We accept Original Articles as well as Review Articles, Editorials and Brief Articles.