Mechanistic Insights into the Selective Dual BET and PLK1 Inhibitory Activity of a Novel Benzamide Compound in Castration-Resistant Prostrate Cancer

Oluwole B Akawa; Temitayo I Subair; Kehinde F Omolabi; Felix O Okunlola; Mahmoud E S Soliman

doi:10.1002/cbdv.202100519

Mechanistic Insights into the Selective Dual BET and PLK1 Inhibitory Activity of a Novel Benzamide Compound in Castration-Resistant Prostrate Cancer

Chem Biodivers. 2021 Dec;18(12):e2100519. doi: 10.1002/cbdv.202100519. Epub 2021 Nov 16.

Authors

Oluwole B Akawa^{1

2}, Temitayo I Subair¹, Kehinde F Omolabi¹, Felix O Okunlola¹, Mahmoud E S Soliman¹

Affiliations

¹ Molecular Bio-computation and Drug Design Laboratory, School of Health Sciences, University of KwaZulu-Natal, Westville Campus, Durban, 4001, South Africa.
² Department of Pharmacology and Therapeutics, College of Medicine and Health Sciences, Afe Babalola University, Ado Ekiti, 360001, Nigeria.

PMID: 34729902
DOI: 10.1002/cbdv.202100519

Abstract

Though multifactorial, BET and PLK1 proteins have been found to be key players in the oncogenic process leading to castration-resistant prostate cancer through regulation of AR and MYC-mediated transcription. Hence, dual inhibition of these proteins appears to be an auspicious approach for CRPC therapy. WNY0824 has been reported to exhibit nanomolar range inhibition as well as significant anti-proliferative activity on AR-positive CRPC cells in vitro. However, structural, and mechanistic events associated with its dual inhibitory and anti-proliferative mechanisms remain unclear. Utilizing integrative computer-assisted atomistic techniques, analyses revealed that the dual-inhibitory activity of WNY0824 against BRD4 and PLK1 proteins is mediated by conserved residues present in the binding cavities of both proteins which are shown to elicit various strong intermolecular interactions and thus favour binding affinity. Also, binding orientation of the ligand at the protein binding cavities allowed for important hydrophobic interactions which resulted in high binding free energy of -42.50 kcal/mol and -51.64 kcal/mol towards BRD4 and PLK1, respectively. While van der Waals interactions are very important to ligand binding in BRD4-WNY complex, electrostatic interactions are pertinent to PLK1-WNY complex. Intriguingly, WNY0824 triggered conformational alterations in both proteins through increased structural instability, decreased structural compactness and mitigation in exposure of residues to solvent surface area. Consequently, critical interactions peculiar to the oncogenic activities of BRD4 and PLK1 were inhibited, a phenomenon that results in an antagonism of CRPC progression. The mechanistic insights presented in this report would further assist in the structure-based design of improved inhibitors useful in CRPC therapy.

Keywords: androgen; bromodomain and extra-terminal domain (BET); castration resistant prostate cancer (CRPC); molecular dynamic simulation; polo-like kinase 1; prostate cancer; testosterone.

MeSH terms

Antineoplastic Agents / chemistry
Antineoplastic Agents / pharmacology*
Benzamides / chemistry
Benzamides / pharmacology*
Cell Cycle Proteins / antagonists & inhibitors*
Cell Cycle Proteins / metabolism
Humans
Male
Models, Molecular
Molecular Structure
Polo-Like Kinase 1
Prostatic Neoplasms / drug therapy*
Prostatic Neoplasms / metabolism
Protein Kinase Inhibitors / chemistry
Protein Kinase Inhibitors / pharmacology*
Protein Serine-Threonine Kinases / antagonists & inhibitors*
Protein Serine-Threonine Kinases / metabolism
Proteins / antagonists & inhibitors*
Proteins / metabolism
Proto-Oncogene Proteins / antagonists & inhibitors*
Proto-Oncogene Proteins / metabolism

Substances

Antineoplastic Agents
Benzamides
Cell Cycle Proteins
Protein Kinase Inhibitors
Proteins
Proto-Oncogene Proteins
bromodomain and extra-terminal domain protein, human
benzamide
Protein Serine-Threonine Kinases

Abstract

MeSH terms

Substances

Grants and funding