Discovery of Novel Pyridazine-Based Cyclooxygenase-2 Inhibitors with a Promising Gastric Safety Profile

Khan, Abida; Diwan, Anupama; Thabet, Hamdy Khamees; Imran, Mohd; Bakht, Md. Afroz

doi:10.3390/molecules25092002

Cited by 19 publications

(35 citation statements)

References 44 publications

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“…The results show that Shiyifang Vinum and four monomer compounds have a significant inhibitory effect on COX-2, and the IC 50 of quercetin, luteolin, kaempferol, apigenin, and Shiyifang Vinum was 1.198 μ g/ml, 3.102 μ g/ml, 8.774 μ g/ml, 35.518 μ g/ml, and 106.95 μ g/ml, respectively. The IC 50 of celecoxib, a selective COX-2 inhibitor, was 20 nM, which was consistent with the results reported in the kit (IC 50 was approximately 10–100 nM) and the test results (17.79 nM) are reported in the literature [ 19 ].…”

Section: Resultssupporting

confidence: 89%

“…The more stable the conformational stability of the compound and protein binding, the lower the energy and the greater the possibility of interaction [ 17 ]. In some studies, the binding energy of ≤ −5.0 kJ/mol was used as the screening standard [ 18 , 19 ]. In this study, 14 core active compounds with a moderate value greater than the average value in the compound target pathway network of Shiyifang Vinum were docked with 11 target proteins.…”

Section: Resultsmentioning

confidence: 99%

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Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology

Tian

Wei

Yao

et al. 2021

Evidence-Based Complementary and Alternative Medicine

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Objective. The possible core active compounds and potential mechanism of action of Shiyifang Vinum were explored through network pharmacology and in vitro enzyme activity verification experiments. Methods. We screened the core active components and the action targets of Shiyifang Vinum through the TCMSP database and literature mining and drew a Venn map of the intersection with anti-inflammatory and analgesic-related gene targets. Go and KEGG analyses were enriched with the David database. The compound target pathway network was constructed using Cytoscape 3.6.1. The binding strength of core active compounds and target proteins was verified through molecular docking, and the direct effects of Shiyifang Vinum and four monomer compounds on COX-2 enzyme activity were detected through an in vitro enzyme activity test. Results. 14 active compounds and 11 targets were screened out from Shiyifang Vinum through TCMSP database and literature mining; 252 GO entries were obtained by GO analysis, and 114 signal pathways were screened by KEGG analysis. The results of the molecular docking showed that the core compounds and target proteins had strong binding activity. In vitro validation experiments showed that both the Shiyifang Vinum and the four monomer compounds could inhibit the activity of COX-2. Conclusion. This study preliminarily explored the potential active compounds and target proteins of the anti-inflammatory and analgesic effects of Shiyifang Vinum, which could provide a scientific basis for further study on the anti-inflammatory and analgesic mechanism and material basis of this recipe.

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Section: Resultssupporting

confidence: 89%

Section: Resultsmentioning

confidence: 99%

Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology

Tian

Wei

Yao

et al. 2021

Evidence-Based Complementary and Alternative Medicine

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“…in vitro analysis of test compounds by performing enzyme immunoassay indicated selective COX‐2 inhibition potential superior to the standard drug celecoxib. Reportedly, the gastric safety of the test compounds arises from the noninhibition of COX‐1 isoenzyme (Khan, Diwan, Thabet, Imran, & Bakht, 2020). The above investigations clearly claimed a robust candidature of thiazolidinone nucleus in rational designing of physiologically benevolent anti‐inflammatory lead molecules focused on the selective inhibition of COX‐2 isoenzyme.…”

Section: Selective Cox‐2 Inhibitors Based On Azole Nucleusmentioning

confidence: 99%

“Azole” as privileged heterocycle for targeting the inducible cyclooxygenase enzyme

Prasher

Sharma

2020

Drug Development Research

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An over‐expression of COX‐2 isoenzyme belonging to the Cyclooxygenase Enzyme Family triggers the overproduction of pro‐inflammatory prostaglandins that instigate the development of chronic inflammation and related disorders. Hence, the rationally designed drugs for mitigating over‐activity of COX‐2 isoenzyme play a regulatory role toward the alleviation of the progression of these disorders. However, a selective COX‐2 inhibition chemotherapy prompts several side effects that necessitate the identification of novel molecular scaffolds for deliberating state‐of‐the‐art drug designing strategies. The heterocyclic “azole” scaffold, being polar and hydrophilic, possesses remarkable physicochemical advantages for designing physiologically active molecules capable of interacting with a wide range of biological components, including enzymes, peptides, and metabolites. The substituted derivatives of azole nuclei enable a comprehensive SAR analysis for the appraisal of bioactive profile of the deliberated molecules for obtaining the rationally designed compounds with prominent activities. The comprehensive SAR analysis readily prompted the identification of Y‐shaped molecules and the eminence of bulkier group for COX‐2 selective inhibition. This review presents an epigrammatic collation of the pharmacophore‐profile of the chemotherapeutics based on azole motif for a selective targeting of the COX‐2 isoenzyme.

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“…Thiazole ring is one of the most common heterocycles in biologically active molecules. Thiazole derivatives showed a various biological activities including anticancer, 1 anti-influenza, 2 antiviral, 3 anti-HIV, 4 anti-inflammatory, 5 antidiabetic, 6 antiplatelet, 7 antihypertensive, 8 anti-hyperlipidemic, 9 antileishmanial, 10 and antioxidant. 11 Nowadays the pharmacy is full of thiazole-derived antibiotics.…”

Section: Introductionmentioning

confidence: 99%

Synthetic Approaches toward Certain Structurally Related Antimicrobial Thiazole Derivatives (2010-2020)

Abuo‐Rahma¹,

Hassan²,

Hassan³

et al. 2021

HETEROCYCLES

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In the present literature review, we comprehensively discuss different methods of synthesis of published antimicrobial thiazole derivatives in the last decade mainly those which showed antibacterial, antimycobacterial and/or antifungal activity. Owing to the great diversity of thiazole-derived antimicrobial agents, we organized most of them chemically in stipulated classes. In each class, we mentioned common methods of thiazole ring closure and indicated antimicrobial activity of the most active derivatives in clear and simple way. CONTENTS1.

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Discovery of Novel Pyridazine-Based Cyclooxygenase-2 Inhibitors with a Promising Gastric Safety Profile

Cited by 19 publications

References 44 publications

Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology

Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology

“Azole” as privileged heterocycle for targeting the inducible cyclooxygenase enzyme

Synthetic Approaches toward Certain Structurally Related Antimicrobial Thiazole Derivatives (2010-2020)

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