Design, Synthesis and Evaluation of Antifungal Activity of Pyrazoleacetamide Derivatives

Author:

Kachi Onkar G.1ORCID,Pawar Hari R.1ORCID,Chabukswar Anuruddha R.2ORCID,Jagdale Swati2ORCID,Swamy Vishwanath3,Vinayak Kadam4,Hingane Dattatray5,Shinde Mahadev6,Pawar Nagesh7

Affiliation:

1. Department of Chemistry, MES Abasaheb Garware College, Karve Road, Pune, 411 004, India

2. Department Pharmaceutical Sciences, School of Health Sciences & Technology, Dr. Vishwanath Karad MIT World Peace University, Kothrud, Pune, 411038, MS, India

3. TCG Life Sciences, Hinjewadi, Pimpri, Pune, 411 057, India

4. Department of Chemistry, MGVS Arts Commerce & Science College, Surgana, Nashik, 422211, India

5. Department of Chemistry, Mahatma Phule College, Pimpri, Pune, 411017, India

6. Department of Chemistry, Arts, Science and Commerce College, Indapur, Maharashtra 413106, India

7. Department of Chemistry, B.K. Birla College, Kalyan. Kalyan West, Maharashtra, 421301, India

Abstract

Background: Fungal infections have posed a big challenge in the management of their treatment. Due to the resistance and toxicity of existing drug molecules in the light of pandemic infections, like COVID-19, there is an urgent need to find newer derivatives of active molecules, which can be effective in fungal infections. Objective: In the present study, we aimed to design pyrazole derivatives using molecular modeling studies against target 1EA1 and synthesize 10 molecules of pyrazole derivatives using a multi-step synthesis approach. Methods: Designed pyrazole derivatives were synthesized by conventional organic methods. The newly synthesized pyrazole molecules were characterized by using FT-IR, 1HNMR, 13CNMR, and LC-MS techniques. Molecular docking studies were also performed. The antifungal activity of newly synthesized compounds was assessed in vitro against Candida albicans and Aspergillus niger using the well plate method. Results: Two of the compounds, OK-7 and OK-8, have been found to show significant docking interaction with target protein 1EA1. These two compounds have also been found to show significant anti-fungal activity against Candida albicans and Aspergillus nigra when compared to the standard fluconazole. The Minimum Inhibitory Concentration (MIC) value of these two compounds has been found to be 50 μg/ml. Conclusion: Pyrazole derivatives with -CH3, CH3O-, and -CN groups have been found to be active against tested fungi and can be further explored for their potential as promising anti-fungal agents for applications in the field of medicinal chemistry.

Publisher

Bentham Science Publishers Ltd.

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