Document Type
Article
Publication Date
2-4-2019
Abstract
Lysine methylation of histones and non-histone substrates by the SET domain containing protein lysine methyltransferase (KMT) G9a/EHMT2 governs transcription contributing to apoptosis, aberrant cell growth, and pluripotency. The positioning of chromosomes within the nuclear three-dimensional space involves interactions between nuclear lamina (NL) and the lamina-associated domains (LAD). Contact of individual LADs with the NL are dependent upon H3K9me2 introduced by G9a. The mechanisms governing the recruitment of G9a to distinct subcellular sites, into chromatin or to LAD, is not known. The cyclin D1 gene product encodes the regulatory subunit of the holoenzyme that phosphorylates pRB and NRF1 thereby governing cell-cycle progression and mitochondrial metabolism. Herein, we show that cyclin D1 enhanced H3K9 dimethylation though direct association with G9a. Endogenous cyclin D1 was required for the recruitment of G9a to target genes in chromatin, for G9a-induced H3K9me2 of histones, and for NL-LAD interaction. The finding that cyclin D1 is required for recruitment of G9a to target genes in chromatin and for H3K9 dimethylation, identifies a novel mechanism coordinating protein methylation.
Recommended Citation
Li, Zhiping; Jiao, Xuanmao; Di Sante, Gabriele; Ertel, Adam; Casimiro, Mathew C.; Wang, Min; Katiyar, Sanjay; Ju, Xiaoming; Klopfenstein, D. V.; Tozeren, Aydin; Dampier, William; Chepelev, Iouri; Jeltsch, Albert; and Pestell, Richard G., "Cyclin D1 integrates G9a-mediated histone methylation." (2019). Department of Cancer Biology Faculty Papers. Paper 148.
https://jdc.jefferson.edu/cbfp/148
Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 License.
PubMed ID
30718920
Language
English
Included in
Biological Phenomena, Cell Phenomena, and Immunity Commons, Medical Genetics Commons, Medical Microbiology Commons
Comments
This article has been peer reviewed. It is the author’s final published version in Oncogene, February 2019.
The published version is available at https://doi.org/10.1038/s41388-019-0723-8. Copyright © Li et al.