Identification of Novel Cyclooxygenase-1 Selective Inhibitors of Thiadiazole-Based Scaffold as Potent Anti-Inflammatory Agents with Safety Gastric and Cytotoxic Profile

Michelyne Haroun; Maria Fesatidou; Anthi Petrou; Christophe Tratrat; Panagiotis Zagaliotis; Antonis Gavalas; Katharigatta N Venugopala; Hafedh Kochkar; Promise M Emeka; Nancy S Younis; Dalia Ahmed Elmaghraby; Mervt M Almostafa; Muhammad Shahzad Chohan; Ioannis S Vizirianakis; Aliki Papadimitriou-Tsantarliotou; Athina Geronikaki

doi:10.3390/molecules28083416

Identification of Novel Cyclooxygenase-1 Selective Inhibitors of Thiadiazole-Based Scaffold as Potent Anti-Inflammatory Agents with Safety Gastric and Cytotoxic Profile

Molecules. 2023 Apr 12;28(8):3416. doi: 10.3390/molecules28083416.

Authors

Michelyne Haroun¹, Maria Fesatidou², Anthi Petrou², Christophe Tratrat¹, Panagiotis Zagaliotis^{2

3}, Antonis Gavalas², Katharigatta N Venugopala^{1

4}, Hafedh Kochkar^{5

6}, Promise M Emeka¹, Nancy S Younis¹, Dalia Ahmed Elmaghraby⁷, Mervt M Almostafa⁸, Muhammad Shahzad Chohan⁹, Ioannis S Vizirianakis^{10

11}, Aliki Papadimitriou-Tsantarliotou¹⁰, Athina Geronikaki²

Affiliations

¹ Department of Pharmaceutical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
² School of Pharmacy, Aristotle, University of Thessaloniki, 54124 Thessaloniki, Greece.
³ Division of Infectious Diseases, Weill Cornell Medicine, New York, NY 10065, USA.
⁴ Department of Biotechnology and Food Technology, Faculty of Applied Sciences, Durban University of Technology, Durban 4001, South Africa.
⁵ Department of Chemistry, College of Science, Imam Abdulrahman Bin Faisal University, Dammam 31441, Saudi Arabia.
⁶ Basic & Applied Scientific Research Center, Imam Abdulrahman Bin Faisal University, Dammam 31441, Saudi Arabia.
⁷ Department of Pharmacy Practice, College of Clinical Pharmacy, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
⁸ Department of Chemistry, College of Science, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
⁹ Biomedical Sciences Department, College of Clinical Pharmacy, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
¹⁰ Laboratory of Pharmacology, School of Pharmacy, Aristotle University of Thessaloniki, 54124 Thessaloniki, Greece.
¹¹ Department of Health Sciences, School of Life and Health Sciences, University of Nicosia, 2417 Nicosia, Cyprus.

Abstract

Major obstacles faced by the use of nonsteroidal anti-inflammatory drugs (NSAID) are their gastrointestinal toxicity induced by non-selective inhibition of both cyclooxygenases (COX) 1 and 2 and their cardiotoxicity associated with a certain class of COX-2 selective inhibitors. Recent studies have demonstrated that selective COX-1 and COX-2 inhibition generates compounds with no gastric damage. The aim of the current study is to develop novel anti-inflammatory agents with a better gastric profile. In our previous paper, we investigated the anti-inflammatory activity of 4-methylthiazole-based thiazolidinones. Thus, based on these observations, herein we report the evaluation of anti-inflammatory activity, drug action, ulcerogenicity and cytotoxicity of a series of 5-adamantylthiadiazole-based thiazolidinone derivatives. The in vivo anti-inflammatory activity revealed that the compounds possessed moderate to excellent anti-inflammatory activity. Four compounds 3, 4, 10 and 11 showed highest potency (62.0, 66.7, 55.8 and 60.0%, respectively), which was higher than the control drug indomethacin (47.0%). To determine their possible mode of action, the enzymatic assay was conducted against COX-1, COX-2 and LOX. The biological results demonstrated that these compounds are effective COX-1 inhibitors. Thus, the IC₅₀ values of the three most active compounds 3, 4 and 14 as COX-1 inhibitors were 1.08, 1.12 and 9.62 μΜ, respectively, compared to ibuprofen (12.7 μΜ) and naproxen (40.10 μΜ) used as control drugs. Moreover, the ulcerogenic effect of the best compounds 3, 4 and 14 were evaluated and revealed that no gastric damage was observed. Furthermore, compounds were found to be nontoxic. A molecular modeling study provided molecular insight to rationalize the COX selectivity. In summary, we discovered a novel class of selective COX-1 inhibitors that could be effectively used as potential anti-inflammatory agents.

Keywords: anti-inflammatory; cyclooxygenase; cytotoxicity; enzyme inhibition; lipoxygenase; molecular modeling; thiadiazole; ulcerogenic effect.

MeSH terms

Anti-Inflammatory Agents / therapeutic use
Anti-Inflammatory Agents, Non-Steroidal / therapeutic use
Antineoplastic Agents* / pharmacology
Cyclooxygenase 1 / metabolism
Cyclooxygenase 2 / metabolism
Cyclooxygenase 2 Inhibitors / pharmacology
Cyclooxygenase 2 Inhibitors / therapeutic use
Edema / drug therapy
Humans
Molecular Docking Simulation
Structure-Activity Relationship
Thiadiazoles* / therapeutic use

Substances

Cyclooxygenase 1
Cyclooxygenase 2
Thiadiazoles
Anti-Inflammatory Agents
Anti-Inflammatory Agents, Non-Steroidal
Cyclooxygenase 2 Inhibitors
Antineoplastic Agents
4-thiazolidinone

Grants and funding

This research was funded by the Deputyship for Research & Innovation, Ministry of Education in Saudi Arabia (project number INST176).