In Silico and In Vitro Evaluation of the Antifungal Activity of a New Chromone Derivative against Candida spp.

Author:

Araújo Gleycyelly Rodrigues1,Costa Palloma Christine Queiroga Gomes da2,Nogueira Paula Lima2,Alves Danielle da Nóbrega2,Ferreira Alana Rodrigues34,da Silva Pablo R.2ORCID,de Andrade Jéssica Cabral34,de Sousa Natália F.34,Loureiro Paulo Bruno Araujo34ORCID,Sobral Marianna Vieira34ORCID,Sousa Damião P.34ORCID,Scotti Marcus Tullius34ORCID,de Castro Ricardo Dias234ORCID,Scotti Luciana345ORCID

Affiliation:

1. Department of Clinical and Social Dentistry, Federal University of Paraíba, Campus I, João Pessoa 58051-900, PB, Brazil

2. Postgraduate Program in Dentistry, Department of Clinic and Social Dentistry, Center of Health Sciences, Federal University of Paraíba, João Pessoa 58051-900, PB, Brazil

3. Postgraduate Program in Natural and Synthetic Bioactive Products, Federal University of Paraíba, João Pessoa 58051-900, PB, Brazil

4. Health Sciences Center, Federal University of Paraíba, Campus I, João Pessoa 58051-900, PB, Brazil

5. Institute of Drugs and Medicines Research, Federal University of Paraíba, Via Ipê Amarelo, S/N, João Pessoa 58051-900, PB, Brazil

Abstract

Candida species are frequently implicated in the development of both superficial and invasive fungal infections, which can impact vital organs. In the quest for novel strategies to combat fungal infections, there has been growing interest in exploring synthetic and semi-synthetic products, particularly chromone derivatives, renowned for their antimicrobial properties. In the analysis of the antifungal activity of the compound (E)-benzylidene-chroman-4-one against Candida, in silico and laboratory tests were performed to predict possible mechanisms of action pathways, and in vitro tests were performed to determine antifungal activity (MIC and MFC), to verify potential modes of action on the fungal cell membrane and wall, and to assess cytotoxicity in human keratinocytes. The tested compound exhibited predicted affinity for all fungal targets, with the highest predicted affinity observed for thymidylate synthase (−102.589 kJ/mol). MIC and CFM values ranged from 264.52 μM (62.5 μg/mL) to 4232.44 μM (1000 μg/mL). The antifungal effect likely occurs due to the action of the compound on the plasma membrane. Therefore, (E)-benzylidene-chroman-4-one showed fungicidal-like activity against Candida spp., possibly targeting the plasma membrane.

Publisher

MDPI AG

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