Synthesis of Functionalized 2′,5‐Oxo‐spiro[furan‐2,3′‐indoline]‐3‐carboxylate Derivatives as Antiproliferative Agents: ADMET Studies, and Molecular Docking against P2Y12 Inhibitors

Author:

Asif Mohd1ORCID,Saquib Mohammad2,Rahman Khan Abdul1,Aqil Farrukh3,salem Almalki Amani4,Ali Alasmary Fatmah4,Singh Jaya5,Nasibullah Malik1ORCID

Affiliation:

1. Department of Chemistry Integral University Lucknow 226026, U.P. India

2. Department of Chemistry University of Allahabad Prayagraj (Allahabad) 211002 India

3. UofL Health-Brown Cancer Center and Department of Medicine University of Louisville Louisville KY40202 USA

4. Chemistry Department College of Science King Saud University Riyadh 11451 Saudi Arabia

5. Department of Chemistry LRPG College Sahibabad Ghaziabad 201005 India

Abstract

AbstractHerein, we present a one‐pot, three‐component synthesis of spirooxindole‐oxofuran carboxylate derivatives (4 ad) through the Huisgen reaction. The newly synthesized spirocyclic compounds were tested for in vitroantiproliferative efficacy against 60 human cancer cell lines at the National Cancer Institute (NCI) in the United States. The screening results indicated that two spirooxindole compounds, 4 b and4 c, possessed the strongest anti‐cancer efficacy in terms of percentage growth inhibition (% GI), with values of 34.17 and 38.19 at 10−5 M concentration against the CNS cancer panel‘s SNB‐75 cell line, respectively. Furthermore, molecular docking investigations demonstrated the binding affinity for the P2Y12 receptor. The compound 4 c which exhibited strong antiproliferative activity with high binding energies might therefore, serve as a potential lead molecule for the development of more effective anti‐cancer agents.

Publisher

Wiley

Subject

General Chemistry

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