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HPV 相关头颈部鳞状细胞癌中信号转导通路的表观遗传调控。

Epigenetic modulation of signal transduction pathways in HPV-associated HNSCC.

机构信息

Department of Otolaryngology/Head and Neck Research, Henry Ford Hospital, Detroit, Michigan 48202, USA.

出版信息

Otolaryngol Head Neck Surg. 2013 Sep;149(3):409-16. doi: 10.1177/0194599813490895. Epub 2013 Jun 4.

Abstract

OBJECTIVE

Human papilloma virus (HPV) positive and HPV negative head and neck squamous cell cancer (HNSCC) are biologically distinct with a prognostic advantage for HPV positive patients compared to HPV negative cases. DNA promoter methylation is central to human diseases such as cancer, including HNSCC, with reported genome-wide hypomethylaton and promoter hypermethylation in HPV positive HNSCC tumors. The goal of this study was to identify differentially methylated genes in HPV positive versus HPV negative primary HNSCC genomes with clues to signaling networks.

STUDY DESIGN

Laboratory-based study.

SETTING

Primary care academic health care system.

SUBJECTS AND METHODS

DNA from 4 HPV positive and 4 HPV negative freshly frozen primary HNSCC were subject to comprehensive genome-wide methylation profiling. Differentially methylated gene lists were examined using the Signal Transduction Pathways (canonical) filter in the Genomatix Pathway System (GePS).

RESULTS

Twofold methylation differences were observed between HPV positive and HPV negative cases for 1168 genes. Pathway analysis applied to investigate the biological role of the 1168 differentially methylated genes revealed 8 signal transduction pathways forming a network of 66 genes, of which 62% are hypermethylated.

CONCLUSION

Our study reveals a predominant hypermethylation profile for genes in signal transduction pathways of HPV positive HNSCC tumor genomes. Because signaling events in the cell play a critical role in the execution of key biological functions, insights into how complex cellular signaling cascades and networks may be programmed in HNSCC are likely to be critical in the development of new biological agents designed to hit multiple targets.

摘要

目的

人乳头瘤病毒(HPV)阳性和 HPV 阴性头颈部鳞状细胞癌(HNSCC)在生物学上是不同的,与 HPV 阴性病例相比,HPV 阳性患者具有预后优势。DNA 启动子甲基化是人类疾病(包括 HNSCC)的核心,据报道 HPV 阳性 HNSCC 肿瘤中存在全基因组低甲基化和启动子过度甲基化。本研究的目的是确定 HPV 阳性与 HPV 阴性原发性 HNSCC 基因组中差异甲基化的基因,为信号网络提供线索。

研究设计

基于实验室的研究。

设置

初级保健学术医疗系统。

受试者和方法

对 4 例 HPV 阳性和 4 例 HPV 阴性新鲜冷冻的原发性 HNSCC 的 DNA 进行了全基因组广泛甲基化分析。使用 Genomatix 通路系统(GePS)中的信号转导途径(经典)过滤器检查差异甲基化基因列表。

结果

HPV 阳性和 HPV 阴性病例之间观察到 1168 个基因的两倍甲基化差异。对 1168 个差异甲基化基因进行通路分析,以研究其在生物学中的作用,结果发现 8 个信号转导通路形成了一个由 66 个基因组成的网络,其中 62%为过度甲基化。

结论

我们的研究揭示了 HPV 阳性 HNSCC 肿瘤基因组中信号转导途径基因的主要过度甲基化模式。由于细胞内的信号事件在执行关键生物学功能中起着至关重要的作用,因此深入了解复杂的细胞信号级联和网络如何在 HNSCC 中编程,很可能对开发旨在靶向多个靶点的新型生物制剂具有重要意义。

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