| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2041000 | Cell Reports | 2012 | 11 Pages |
SummarySenescence is a cellular response preventing tumorigenesis. The Ras oncogene is frequently activated or mutated in human cancers, but Ras activation is insufficient to transform primary cells. In a search for cooperating oncogenes, we identify the lysine demethylase JMJD2A/KDM4A. We show that JMJD2A functions as a negative regulator of Ras-induced senescence and collaborates with oncogenic Ras to promote cellular transformation by negatively regulating the p53 pathway. We find CHD5, a known tumor suppressor regulating p53 activity, as a target of JMJD2A. The expression of JMJD2A inhibits Ras-mediated CHD5 induction leading to a reduced activity of the p53 pathway. In addition, we show that JMJD2A is overexpressed in mouse and human lung cancers. Depletion of JMJD2A in the human lung cancer cell line A549 bearing an activated K-Ras allele triggers senescence. We propose that JMJD2A is an oncogene that represents a target for Ras-expressing tumors.
Graphical AbstractFigure optionsDownload full-size imageDownload as PowerPoint slideHighlights► JMJD2A contributes to the bypass of Ras-induced senescence ► Genome-wide search for gene promoters regulated by JMJD2A identifies CHD5 ► JMJD2A cooperates with Ras to transform primary cells ► JMJD2A depletion in human lung cancer cells leads to massive senescence
