| Literature DB >> 31373686 |
Dimitrios Mathios1, Taeyoung Hwang2,3, Yuanxuan Xia1, Jillian Phallen4, Yuan Rui2,3, Alfred P See5, Russell Maxwell1,6, Zineb Belcaid1, Joshua Casaos1, Peter C Burger7, Kerrie L McDonald8, Gary L Gallia1, Leslie Cope4, Mihoko Kai6, Henry Brem1, Drew M Pardoll4,9,10, Patrick Ha11, Jordan J Green1,2,3,4, Victor E Velculescu4,10, Chetan Bettegowda1,4, Chul-Kee Park1,12, Michael Lim1.
Abstract
DNA methylation has long been recognized as a tumor-promoting factor when aberrantly regulated in the promoter region of genes. However, the effect of intragenic DNA methylation remains poorly understood on the clinical aspects of cancer. Here, we first evaluated the significance of intragenic DNA methylation for survival outcomes of cancer patients in a genome-wide manner. Glioblastoma patients with hypermethylated intragenic regions exhibited better survival than hypomethylated patients. Enrichment analyses of intragenic DNA methylation profiles with epigenetic signatures prioritized the intragenic DNA methylation of ZMIZ1 as a possible glioblastoma prognostic marker that is independent of MGMT methylation in IDH1 wild-type patients. This intragenic region harbored molecular signatures of alternative transcription across many cell types. Furthermore, we found that the intragenic region of ZMIZ1 can serve as a molecular marker in multiple cancers including astrocytomas, bladder cancer and renal cell carcinoma according to DNA methylation status. Finally, in vitro and in vivo experiments uncovered the role of ZMIZ1 as a driver of tumor cell migration. Altogether, our results identify ZMIZ1 as a prognostic marker in cancer and highlight the clinical significance of intragenic methylation in cancer.Entities:
Keywords: TCGA; ZMIZ1; glioblastoma; intragenic DNA methylation; prognostic cancer marker
Year: 2019 PMID: 31373686 DOI: 10.1002/ijc.32587
Source DB: PubMed Journal: Int J Cancer ISSN: 0020-7136 Impact factor: 7.396