液体活检方法检测HCC，并通过血浆cfDNA甲基组分析确定GJA4作为HBV-HCC的潜在生物标志物。

IF 4.8 2区医学 Q1 GENETICS & HEREDITY

Clinical Epigenetics Pub Date : 2025-06-11 DOI:10.1186/s13148-025-01909-w

Jialing Sun, Xinfeng Sun, Weihuang He, Bingding Huang, Wenxing Feng, Zhiyi Han, Ruyun Ruan, Yuanke Pan, Jinxin Zhu, Jing Li, Xin Zhong, Mengqing Ma, Rui Hu, Minling Lv, Qi Huang, Wei Zhang, Mingji Feng, Jinyu Yi, Pin Cui, Xiaozhou Zhou

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引用次数: 0

摘要

背景：早期发现肝细胞癌（HCC）可大大提高患者的生存率。血浆cfDNA甲基化已被证明有潜力成为一种诊断HCC的非侵入性方法。然而，鉴定出的HCC血浆cfDNA甲基化位点对早期HCC诊断的敏感性较低。因此，我们的目标是开发一种基于游离DNA （cfDNA）甲基化的高灵敏度标记面板来检测HCC。方法：该研究纳入374名参与者，包括102名健康个体，51名HBV患者，50名肝硬化患者和171名HCC患者（56名根据BCLC分期为0期或A期）。两种cfDNA甲基化测序方法（全基因组亚硫酸酯测序（WGBS）和靶向亚硫酸酯测序（TBS））与机器学习建模一起用于检测四组参与者之间基于差异甲基化区域（DMR）的hbv相关HCC。结果：TBS分析区分各阶段HCC患者和健康人的总灵敏度为96.67%，特异性为93.7%，而甲胎蛋白（AFP）的敏感性为18% ~ 60%，区分早期HCC患者和健康人的敏感性为90.0%，特异性为93.75%。在HCC和非癌组之间发现了许多显著的DMRs，为HCC检测提供了候选生物标志物。其中一种位于GJA4启动子区域的DMRs被发现在hbv相关的HCC癌变的整个过程中始终存在。使用TCGA的数据，比较160名健康人与369名HCC患者的GJA4表达谱进一步支持了这一观点。结论：本研究通过血浆cfDNA甲基组分析为HCC的检测、分期和早期检测提供了生物标志物。此外，GJA4启动子甲基化的动态改变可能为研究hbv相关HCC的癌变和预后提供分子线索。

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A liquid biopsy approach detects HCC and identifies GJA4 as a potential biomarker for HBV-HCC via plasma cfDNA methylome profiling.

Background: Early detection of hepatocellular carcinoma (HCC) can greatly improve the survival rate of patients. Plasma cfDNA methylation has been shown to have the potential to be a non-invasive method for diagnosing HCC. However, the identified HCC plasma cfDNA methylation sites were less sensitive to early HCC diagnosis. Therefore, we aimed to develop a highly sensitive marker panel based on cell-free DNA (cfDNA) methylation for the detection of HCC.

Methods: The study included 374 participants, including 102 healthy individuals, 51 HBV patients, 50 cirrhosis patients, and 171 HCC patients (56 at stage 0 or A according to BCLC staging). Two cfDNA methylation sequencing assays (whole genome bisulfite sequencing (WGBS) and targeted bisulfite sequencing (TBS)) were used along with machine learning modeling to detect HBV-related HCC based on differentially methylated regions (DMR) among the four participant groups.

Results: TBS analysis achieved an overall sensitivity of 96.67% at a specificity of 93.7% than alpha-fetoprotein (AFP) of 18%-60%, to discriminate all stages of HCC patients from healthy people, and sensitivity of 90.0% at a specificity of 93.75% to discriminate early-stage HCC patients from healthy people. A number of significant DMRs between HCC and non-cancer groups were identified, providing candidate biomarkers for HCC detection. Among these DMRs, one that locates in the promoter region of GJA4, was found to be consistently present in the whole process of HBV-related HCC carcinogenesis. Using data from TCGA, comparison of expression profile of GJA4 between 160 healthy people and 369 HCC patients further supported this scenario.

Conclusions: This study provides biomarkers for detecting, staging and early detection of HCC using plasma cfDNA methylome profiling. Additionally, the dynamic alteration of GJA4 promoter methylation may serve as a molecular clue for studying HBV-related HCC carcinogenesis and prognosis.

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来源期刊

Clinical Epigenetics ONCOLOGY-

自引率

5.30%

发文量

150

期刊介绍： Clinical Epigenetics, the official journal of the Clinical Epigenetics Society, is an open access, peer-reviewed journal that encompasses all aspects of epigenetic principles and mechanisms in relation to human disease, diagnosis and therapy. Clinical trials and research in disease model organisms are particularly welcome.