4.6 Article

Antimicrobial Profile of Actinomycin D Analogs Secreted by Egyptian Desert Streptomyces sp. DH7

Journal

ANTIBIOTICS-BASEL
Volume 10, Issue 10, Pages -

Publisher

MDPI
DOI: 10.3390/antibiotics10101264

Keywords

desert actinobacteria; MRSA; actinomycin D; Sinai desert; Egypt

Funding

  1. Egyptian Science and Technology Develop ment Fund (STDF) [5251]

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The research explored desert Actinobacteria from the Sinai Peninsula, showing high inhibitory effects against multidrug-resistant Staphylococcus aureus strains. Compounds with potential antibacterial activities were isolated and purified, including actinomycin D analogues previously not reported from natural sources. This study highlights the potential of Sinai desert ecosystems as rich sources of antibiotic-producing Actinobacteria.
Egyptian deserts are an underexplored ecological niche, especially the Sinai Peninsula. In our recent study, we explored this extreme environment and shed light on the bioactive capabilities of desert Actinobacteria isolated from Sinai. Fifty desert Actinobacteria were isolated from the Sinai desert using mineral salt media, basal media, and starch casein media. The filtrate of Streptomyces sp. DH 7 displayed a high inhibitory effect against multidrug-resistant Staphylococcus aureus (MRSA) strains. The 16S rDNA sequencing confirmed that isolate DH7 belongs to the genus Streptomyces. The NJ phylogenetic tree showed relatedness to the Streptomyces flavofuscus strain NRRL B-2594 and Streptomyces pratensis strain ch24. The minimum inhibitory concentrations against MRSA were 16 and 32 mu g/mu L. Chemical investigation of the ethyl acetate extract of Streptomyces sp. DH7 led to the isolation and purification of natural products 1-4. Structure elucidation of the purified compounds was performed using detailed spectroscopic analysis including 1 and 2D NMR, and ESI-MS spectrometry. To the best of our knowledge, this is the first report for the isolation of compounds 1-4 from a natural source, while synthetic analogs were previously reported in the literature. Compounds 3-4 were identified as actinomycin D analogues and this is the first report for the production of actinomycin D analogs from the Sinai desert with an inhibitory effect against MRSA. We indorse further study for this analog that can develop enhanced antimicrobial activities. We confirm that the desert ecosystems in Egypt are rich sources of antibiotic-producing Actinobacteria.

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