Beijing National Laboratory for Molecular Sciences, College of Chemistry and Molecular Engineering, Peking University, Beijing, 100871, China.
Changping Laboratory, Beijing, 102206, China.
Mol Cancer. 2024 Sep 6;23(1):190. doi: 10.1186/s12943-024-02100-0.
Epigenetic alterations, such as those in chromatin structure and DNA methylation, have been extensively studied in a number of tumor types. But oral cancer, particularly oral adenocarcinoma, has received far less attention. Here, we combined laser-capture microdissection and muti-omics mini-bulk sequencing to systematically characterize the epigenetic landscape of oral cancer, including chromatin architecture, DNA methylation, H3K27me3 modification, and gene expression. In carcinogenesis, tumor cells exhibit reorganized chromatin spatial structures, including compromised compartment structures and altered gene-gene interaction networks. Notably, some structural alterations are observed in phenotypically non-malignant paracancerous but not in normal cells. We developed transformer models to identify the cancer propensity of individual genome loci, thereby determining the carcinogenic status of each sample. Insights into cancer epigenetic landscapes provide evidence that chromatin reorganization is an important hallmark of oral cancer progression, which is also linked with genomic alterations and DNA methylation reprogramming. In particular, regions of frequent copy number alternations in cancer cells are associated with strong spatial insulation in both cancer and normal samples. Aberrant methylation reprogramming in oral squamous cell carcinomas is closely related to chromatin structure and H3K27me3 signals, which are further influenced by intrinsic sequence properties. Our findings indicate that structural changes are both significant and conserved in two distinct types of oral cancer, closely linked to transcriptomic alterations and cancer development. Notably, the structural changes remain markedly evident in oral adenocarcinoma despite the considerably lower incidence of genomic copy number alterations and lesser extent of methylation alterations compared to squamous cell carcinoma. We expect that the comprehensive analysis of epigenetic reprogramming of different types and subtypes of primary oral tumors can provide additional guidance to the design of novel detection and therapy for oral cancer.
表观遗传改变,如染色质结构和 DNA 甲基化的改变,已在许多肿瘤类型中得到广泛研究。但口腔癌,特别是口腔腺癌,受到的关注要少得多。在这里,我们结合激光捕获显微切割和多组学 mini-bulk 测序,系统地表征了口腔癌的表观遗传景观,包括染色质结构、DNA 甲基化、H3K27me3 修饰和基因表达。在肿瘤发生过程中,肿瘤细胞表现出重新组织的染色质空间结构,包括受损的隔室结构和改变的基因-基因相互作用网络。值得注意的是,一些结构改变仅发生在表型非恶性的癌旁组织中,而不在正常细胞中观察到。我们开发了转换器模型来识别单个基因组位点的癌症倾向,从而确定每个样本的致癌状态。对癌症表观遗传景观的深入了解提供了证据,表明染色质重排是口腔癌进展的一个重要标志,它与基因组改变和 DNA 甲基化重编程有关。特别是,癌细胞中频繁的拷贝数改变区域与癌症和正常样本中强烈的空间隔离有关。口腔鳞状细胞癌中异常的甲基化重编程与染色质结构和 H3K27me3 信号密切相关,而这些信号进一步受到内在序列特性的影响。我们的研究结果表明,结构变化在两种不同类型的口腔癌中都是显著和保守的,与转录组改变和癌症发展密切相关。值得注意的是,尽管与鳞状细胞癌相比,口腔腺癌的基因组拷贝数改变和甲基化改变的程度较低,但结构改变仍然明显。我们期望对不同类型和亚型的原发性口腔肿瘤的表观遗传重编程进行全面分析,为口腔癌的新型检测和治疗方法的设计提供额外的指导。
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