Dual EZH2 and EHMT2 histone methyltransferase inhibition increases biological efficacy in breast cancer cells.

Curry, Edward; Green, Ian; Chapman-Rothe, Nadine; Shamsaei, Elham; Kandil, Sarah; Cherblanc, Fanny L; Payne, Luke; Bell, Emma; Ganesh, Thota; Srimongkolpithak, Nitipol; Caron, Joachim; Li, Fengling; Uren, Anthony G; Snyder, James P; Vedadi, Masoud; Fuchter, Matthew J; Brown, Robert

Curry, Edward; Green, Ian; Chapman-Rothe, Nadine; Shamsaei, Elham; Kandil, Sarah; Cherblanc, Fanny L; Payne, Luke; Bell, Emma; Ganesh, Thota; Srimongkolpithak, Nitipol; Caron, Joachim; Li, Fengling; Uren, Anthony G; Snyder, James P; Vedadi, Masoud; Fuchter, Matthew J; Brown, Robert.

Affiliation

Curry E; Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Green I; Division of Cancer, Department of Surgery and Cancer, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Chapman-Rothe N; Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Shamsaei E; Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Kandil S; Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Cherblanc FL; Department of Chemistry, Imperial College London, South Kensington Campus, London, SW7 2AZ UK.
Payne L; Division of Cancer, Department of Surgery and Cancer, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Bell E; Division of Cancer, Department of Surgery and Cancer, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK.
Ganesh T; Department of Pharmacology, Emory University, Atlanta, GA 30322 USA.
Srimongkolpithak N; Department of Chemistry, Imperial College London, South Kensington Campus, London, SW7 2AZ UK.
Caron J; Department of Chemistry, Imperial College London, South Kensington Campus, London, SW7 2AZ UK.
Li F; Structural Genomics Consortium, University of Toronto, Toronto, ON M5G 1L7 Canada.
Uren AG; MRC Clinical Sciences Centre, Hammersmith Hospital Campus, London, W12 0NN UK.
Snyder JP; Department of Chemistry, Emory University, Atlanta, GA 30322 USA.
Vedadi M; Structural Genomics Consortium, University of Toronto, Toronto, ON M5G 1L7 Canada.
Fuchter MJ; Department of Chemistry, Imperial College London, South Kensington Campus, London, SW7 2AZ UK.
Brown R; Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College London, Hammersmith Hospital Campus, London, W12 ONN UK ; Section of Molecular Pathology, Institute of Cancer Research, Sutton, SM2 5NG UK.

Clin Epigenetics ; 7: 84, 2015.

Article in En | MEDLINE | ID: mdl-26300989

ABSTRACT

ABSTRACT

BACKGROUND:

Many cancers show aberrant silencing of gene expression and overexpression of histone methyltransferases. The histone methyltransferases (HKMT) EZH2 and EHMT2 maintain the repressive chromatin histone methylation marks H3K27me and H3K9me, respectively, which are associated with transcriptional silencing. Although selective HKMT inhibitors reduce levels of individual repressive marks, removal of H3K27me3 by specific EZH2 inhibitors, for instance, may not be sufficient for inducing the expression of genes with multiple repressive marks.

RESULTS:

We report that gene expression and inhibition of triple negative breast cancer cell growth (MDA-MB-231) are markedly increased when targeting both EZH2 and EHMT2, either by siRNA knockdown or pharmacological inhibition, rather than either enzyme independently. Indeed, expression of certain genes is only induced upon dual inhibition. We sought to identify compounds which showed evidence of dual EZH2 and EHMT2 inhibition. Using a cell-based assay, based on the substrate competitive EHMT2 inhibitor BIX01294, we have identified proof-of-concept compounds that induce re-expression of a subset of genes consistent with dual HKMT inhibition. Chromatin immunoprecipitation verified a decrease in silencing marks and an increase in permissive marks at the promoter and transcription start site of re-expressed genes, while Western analysis showed reduction in global levels of H3K27me3 and H3K9me3. The compounds inhibit growth in a panel of breast cancer and lymphoma cell lines with low to sub-micromolar IC50s. Biochemically, the compounds are substrate competitive inhibitors against both EZH2 and EHMT1/2.

CONCLUSIONS:

We have demonstrated that dual inhibition of EZH2 and EHMT2 is more effective at eliciting biological responses of gene transcription and cancer cell growth inhibition compared to inhibition of single HKMTs, and we report the first dual EZH2-EHMT1/2 substrate competitive inhibitors that are functional in cells.

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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: Clin Epigenetics Year: 2015 Document type: Article

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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: Clin Epigenetics Year: 2015 Document type: Article