Abstract
Azole-based antifungal agents constitute one of the important classes of antifungal drugs. Hence, in the present work, 12 new benzimidazole-thiazole derivatives 3a–3l were synthesized to evaluate their anticandidal activity against C. albicans, C. glabrata, C. krusei, and C. parapsilopsis. The structures of the newly synthesized compounds 3a–3l were confirmed by IR, 1H-NMR, 13C-NMR, and ESI-MS spectroscopic methods. ADME parameters of synthesized compounds 3a–3l were predicted by an in-slico study and it was determined that all synthesized compounds may have a good pharmacokinetic profile. In the anticandidal activity studies, compounds 3c and 3d were found to be the most active compounds against all Candida species. In addition, cytoxicity studies showed that these compounds are nontoxic with a IC50 value higher than 500 µg/mL. The effect of compounds 3c and 3d on the ergosterol level of C. albicans was determined by an LC-MS-MS method. It was observed that both compounds cause a decrease in the ergosterol level. A molecular docking study including binding modes of 3c to lanosterol 14α-demethylase (CYP51), a key enzyme in ergosterol biosynthesis, was performed to elucidate the mechanism of the antifungal action. The docking studies revealed that there is a strong interaction between CYP51 and the most active compound 3c.
Highlights
Fungal infections represent a serious and presently unresolved health problem, in developed countries
Melting points of the compounds were measured by using an automatic melting point determination instrument (MP90, Mettler-Toledo, Columbus, OH, USA) and were presented as uncorrected
Chemical purities of the compounds were checked by classical TLC applications performed on silica gel 60 F254 (Merck KGaA)
Summary
Fungal infections represent a serious and presently unresolved health problem, in developed countries. Fungal infections represent 17% of all intensive care unit infections in Europe and the statistics for the United States are similar. Especially of systemic infections, is accompanied by moderate success rates and by high costs. Emerging resistance to commercially offered antifungals has been reported. Common non-life threatening by aggressive superficial infections such as recurrent vulvovaginal candidiasis, cause important restrictions to patients, resulting in reduced quality of life [1]. Invasive fungal infections and dermatomycoses are the other type of fungal infections, caused by fungal organisms in people with increased vulnerability such as burn patients, neonates, organ transplant patients, and cancer patients receiving chemotherapy
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