Distinct Mechanisms of Cytotoxicity in Novel Nitrogenous Heterocycles: Future Directions for a New Anti-Cancer Agent

Rasha Saad Suliman; Sahar Saleh Alghamdi; Rizwan Ali; Ishrat Rahman; Tariq Alqahtani; Ibrahim K Frah; Dimah A Aljatli; Sarah Huwaizi; Shatha Algheribe; Zeyad Alehaideb; Imadul Islam

doi:10.3390/molecules27082409

Distinct Mechanisms of Cytotoxicity in Novel Nitrogenous Heterocycles: Future Directions for a New Anti-Cancer Agent

Molecules. 2022 Apr 8;27(8):2409. doi: 10.3390/molecules27082409.

Authors

Rasha Saad Suliman^{1

2}, Sahar Saleh Alghamdi^{1

2}, Rizwan Ali^{1

2}, Ishrat Rahman³, Tariq Alqahtani^{1

2}, Ibrahim K Frah¹, Dimah A Aljatli¹, Sarah Huwaizi², Shatha Algheribe², Zeyad Alehaideb², Imadul Islam²

Affiliations

¹ College of Pharmacy, King Saud bin Abdulaziz University for Health Sciences, Riyadh 14611, Saudi Arabia.
² Medical Research Core Facility and Platforms, King Abdullah International Medical Research Center (KAIMRC), Ministry of National Guard Health Affairs, Riyadh 14811, Saudi Arabia.
³ Department of Basic Dental Sciences, College of Dentistry, Princess Nourah Bint Abdulrahman University, Riyadh 11671, Saudi Arabia.

Abstract

Electron-rich, nitrogenous heteroaromatic compounds interact more with biological/cellular components than their non-nitrogenous counterparts. The strong intermolecular interactions with proteins, enzymes, and receptors confer significant biological and therapeutic properties to the imidazole derivatives, giving rise to a well-known and extensively used range of therapeutic drugs used for infections, inflammation, and cancer, to name a few. The current study investigates the anti-cancer properties of fourteen previously synthesized nitrogenous heterocycles, derivatives of imidazole and oxazolone, on a panel of cancer cell lines and, in addition, predicts the molecular interactions, pharmacokinetic and safety profiles of these compounds.

Method: The MTT and CellTiter-Glo^® assays were used to screen the imidazole and oxazolone derivatives on six cancer cell lines: HL60, MDA-MB-321, KAIMRC1, KMIRC2, MCF-10A, and HCT8. Subsequently, in vitro tubulin staining and imaging were performed, and the level of apoptosis was measured using the Promega ApoTox-Glo^® triplex assay. Furthermore, several computational tools were utilized to investigate the pharmacokinetics and safety profile, including PASS Online, SEA Search, the QikProp tool, SwissADME, ProTox-II, and an in silico molecular docking study on tubulin to identify the critical molecular interactions.

Results: In vitro analysis identified compounds 8 and 9 to possess the most significant potent cytotoxic activity on the HL60 and MDA-MB-231 cell lines, supported by PASS Online anti-cancer predictions with pa scores of 0.413 and 0.434, respectively. In addition, compound 9 induced caspase 3/7 dependent-apoptosis and interfered with tubulin polymerization in the MDA-MB-231 cell line, consistent with in silico docking results, identifying binding similarity to the native ligand colchicine. All the derivatives, including compounds 8 and 9, had acceptable pharmacokinetics; however, the safety profile was suboptimal for all the tested derivates except compound 4.

Conclusion: The imidazole derivative compound 9 is a promising anti-cancer agent that switches on caspase-dependent apoptotic cell death and modulates microtubule function. Therefore, it could be a lead compound for further drug optimization and development.

Keywords: ADME; Imidazole; anti-cancer; oxazolone; target prediction; tubulin inhibitors.

MeSH terms

Antineoplastic Agents* / chemistry
Antineoplastic Agents* / pharmacology
Cell Line, Tumor
Cell Proliferation
Drug Screening Assays, Antitumor
Molecular Docking Simulation
Molecular Structure
Nitrogen / pharmacology
Oxazolone / pharmacology
Structure-Activity Relationship
Tubulin Modulators / pharmacology
Tubulin* / metabolism

Substances

Antineoplastic Agents
Tubulin
Tubulin Modulators
Oxazolone
Nitrogen

Grants and funding

SP20.441.R/King Abdullah International Medical Research Center