Synergistic antifungal activity and potential mechanism of action of a glycolipid-like compound produced by Streptomyces blastmyceticus S108 against Candida clinical isolates

A Ayed; R Essid; H Mankai; A Echmar; N Fares; M Hammami; N Sewald; F Limam; O Tabbene

doi:10.1093/jambio/lxad246

Synergistic antifungal activity and potential mechanism of action of a glycolipid-like compound produced by Streptomyces blastmyceticus S108 against Candida clinical isolates

J Appl Microbiol. 2023 Nov 1;134(11):lxad246. doi: 10.1093/jambio/lxad246.

Authors

A Ayed¹, R Essid¹, H Mankai¹, A Echmar¹, N Fares¹, M Hammami², N Sewald³, F Limam¹, O Tabbene¹

Affiliations

¹ Laboratory of Bioactive Substances, Center of Biotechnology of Borj Cedria, BP 901, Hammam-Lif 2050, Tunisia.
² Laboratory of Aromatic and Medicinal Plants, Center of Biotechnology of Borj Cedria, Hammam-Lif 2050, Tunisia.
³ Organic and Bioorganic Chemistry, Faculty of Chemistry, Bielefeld University, 33615 Bielefeld, Germany.

PMID: 37884451
DOI: 10.1093/jambio/lxad246

Abstract

Aim: The present study aimed to investigate a novel antifungal compound produced by Streptomyces blastmyceticus S108 strain. Its effectiveness against clinical isolates of Candida species and its synergistic effect with conventional antifungal drugs were assessed, and its molecular mechanism of action was further studied against Candida albicans.

Methods and results: A newly isolated strain from Tunisian soil, S. blastmyceticus S108, showed significant antifungal activity against Candida species by well diffusion method. The butanolic extract of S108 strain supernatant exhibited the best anti-Candida activity with a minimal inhibitory concentration (MIC) value of 250 μg ml-1, determined by the microdilution method. The bio-guided purification steps of the butanolic extract were performed by chromatographic techniques. Among the fractions obtained, F13 demonstrated the highest level of activity, displaying a MIC of 31.25 μg ml-1. Gas chromatography-mass spectrometry and electrospray ionization mass spectrometry analyses of this fraction (F13) revealed the glycolipidic nature of the active molecule with a molecular weight of 685.6 m/z. This antifungal metabolite remained stable to physicochemical changes and did not show hemolytic activity even at 4MIC corresponding to 125 µg ml-1 toward human erythrocytes. Besides, the glycolipid compound was combined with 5-flucytosine and showed a high synergistic effect with a fractional inhibitory concentration index value 0.14 against C. albicans ATCC 10231. This combination resulted in a decrease of MIC values of 5-flucytosine and the glycolipid-like compound by 8- and 64-fold, respectively. The examination of gene expression in treated C. albicans cells by quantitative polymerase chain reaction (qPCR) revealed that the active compound tested alone or in combination with 5-flucytosine blocks the ergosterol biosynthesis pathway by downregulating the expression of ERG1, ERG3, ERG5, ERG11, and ERG25 genes.

Conclusion and impact of the study: The new glycolipid-like compound, produced by Streptomyces S108 isolate, could be a promising drug for medical use against pathogenic Candida isolates.

Keywords: Candida albicans; Streptomyces blastmyceticus S108; antifungal activity; ergosterol biosynthesis pathway; glycolipid; synergistic effect.

MeSH terms

Antifungal Agents* / chemistry
Candida
Candida albicans
Flucytosine / pharmacology
Humans
Microbial Sensitivity Tests
Plant Extracts / pharmacology
Streptomyces* / genetics

Substances

Antifungal Agents
Flucytosine
Plant Extracts

Supplementary concepts

Streptomyces blastmyceticus

Grants and funding

Ministry of Higher Education and Scientific Research