Methylation of the JMJD2B epigenetic regulator differentially affects its ability to coactivate the ETV1 and JUN transcription factors

Tae-Dong Kim; Ruicai Gu; Ralf Janknecht

Methylation of the JMJD2B epigenetic regulator differentially affects its ability to coactivate the ETV1 and JUN transcription factors

Int J Biochem Mol Biol. 2023 Dec 15;14(6):101-115. eCollection 2023.

Authors

Tae-Dong Kim¹, Ruicai Gu¹, Ralf Janknecht^{1

2

3}

Affiliations

¹ Department of Cell Biology, University of Oklahoma Health Sciences Center Oklahoma, OK, USA.
² Stephenson Cancer Center, University of Oklahoma Health Sciences Center Oklahoma, OK, USA.
³ Department of Pathology, University of Oklahoma Health Sciences Center Oklahoma, OK, USA.

PMID: 38213775
PMCID: PMC10776875

Abstract

Objectives: Jumonji C domain-containing (JMJD) 2B (JMJD2B) is a transcriptional cofactor and histone demethylase that is involved in prostate cancer formation. However, how its function is regulated by posttranslational modification has remained elusive. Hence, we examined if JMJD2B would be regulated by lysine methylation.

Methods: Through in vitro methylation assays and Western blotting with methyl-lysine specific antibodies, we analyzed lysine methylation within JMJD2B. Identified methylated lysine residues were mutated to arginine residues and the respective impact on JMJD2B transcriptional activity measured with a reporter gene assay in human LNCaP prostate cancer cells.

Results: We discovered that JMJD2B is methylated on up to six different lysine residues. Further, we identified the suppressor of variegation 3-9/enhancer of zeste/trithorax (SET) domain-containing protein 7/9 (SET7/9) as the methyltransferase being responsible for this posttranslational modification. Mutating the methylation sites in JMJD2B to arginine residues led to diminished coactivation of the Ju-nana (JUN) transcription factor, which is a known oncogenic protein in prostate tumors. In contrast, methylation of JMJD2B had no impact on its ability to coactivate another transcription factor associated with prostate cancer, the DNA-binding protein E26 transformation-specific (ETS) variant 1 (ETV1). Consistent with a potential joint action of JMJD2B, SET7/9 and JUN in prostate cancer, the expression of JMJD2B in human prostate tumors was positively correlated with both SET7/9 and JUN levels.

Conclusions: The identified SET7/9-mediated methylation of JMJD2B appears to impact its cooperation with selected interacting transcription factors in prostate cancer cells. Given the implicated roles of JMJD2B beyond prostate tumorigenesis, SET7/9-mediated methylation of JMJD2B possibly also influences the development of other cancers, while its impairment might have relevance for obesity or a global developmental delay that can be elicited by reduced JMJD2B activity.

Keywords: Gene transcription; SET domain-containing 7 (SETD7); lysine demethylase 4B (KDM4B); posttranslational modification; prostate cancer.

Grants and funding

R03 CA223615/CA/NCI NIH HHS/United States