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Journal of Enzyme Inhibition and Medicinal Chemistry Volume 38, 2023 - Issue 1
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Research Paper

Simultaneous administration of EZH2 and BET inhibitors inhibits proliferation and clonogenic ability of metastatic prostate cancer cells

Aide Negria Department of Medicine and Surgery, University of Parma, Parma, Italy
,
Marina Marozzia Department of Medicine and Surgery, University of Parma, Parma, Italy
,
Daniela Trisciuogliob Institute of Molecular Biology and Pathology (IMBP), National Research Council (CNR) c/o Department of Biology and Biotechnology “Charles Darwin,” Sapienza University of Rome, Rome, Italy
,
Dante Rotilic Department of Chemistry and Technology of Drugs, Sapienza University of Rome, Rome, ItalyORCID Iconhttps://orcid.org/0000-0002-8428-8763
ORCID Icon,
Antonello Maic Department of Chemistry and Technology of Drugs, Sapienza University of Rome, Rome, ItalyORCID Iconhttps://orcid.org/0000-0001-9176-2382
ORCID Icon &
Federica Rizzia Department of Medicine and Surgery, University of Parma, Parma, Italy;d National Institute of Biostructure and Biosystems (INBB), Rome, ItalyCorrespondence[email protected]
Article: 2163242 | Received 11 Nov 2022, Accepted 20 Dec 2022, Published online: 11 Jan 2023
 
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Abstract

Androgen deprivation therapy (ADT) is a common treatment for recurrent prostate cancer (PC). However, after a certain period of responsiveness, ADT resistance occurs virtually in all patients and the disease progresses to lethal metastatic castration-resistant prostate cancer (mCRPC). Aberrant expression and function of the epigenetic modifiers EZH2 and BET over activates c-myc, an oncogenic transcription factor critically contributing to mCRPC. In the present work, we tested, for the first time, the combination of an EZH2 inhibitor with a BET inhibitor in metastatic PC cells. The combination outperformed single drugs in inhibiting cell viability, cell proliferation and clonogenic ability, and concomitantly reduced both c-myc and NF-kB expression. Although these promising results will warrant further in vivo validation, they represent the first step to establishing the rationale that the proposed combination might be suitable for mCRPC treatment, by exploiting molecular targets different from androgen receptor.

Disclosure statement

The authors report no conflicts of interest.

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