New bioactive metabolites from the elicited marine sponge-derived bacterium Actinokineospora spheciospongiae sp. nov.

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作者
Ahmed Tawfike
Eman Zekry Attia
Samar Yehia Desoukey
Dina Hajjar
Arwa A. Makki
Peter J. Schupp
RuAngelie Edrada-Ebel
Usama Ramadan Abdelmohsen
机构
[1] Rothamsted Research,Computational and Analytical Science Department
[2] Helwan University,Department of Pharmacognosy, Faculty of Pharmacy
[3] Minia University,Department of Pharmacognosy, Faculty of Pharmacy
[4] University of Jeddah,Department of Biochemistry, Faculty of Science, Center for Science and Medical Research
[5] Carl-von-Ossietzky University Oldenburg,undefined
[6] Institute for Chemistry and Biology of the Marine Environment,undefined
来源
AMB Express | / 9卷
关键词
Sponges; Actinomycetes; Fridamycin; Elicitation; Antitrypanosomal;
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摘要
Several approaches have been dedicated to activate the cryptic gene clusters in the genomes of actinomycetes for the targeted discovery of new fascinating biomedical lead structures. In the current study, N-acetylglucosamine was used to maximize the chemical diversity of sponge-derived actinomycete Actinokineospora spheciospongiae sp. nov. HR–ESI–MS was employed for dereplication study and orthogonal partial least square-discriminant analysis was applied to evaluate the HR–ESI–MS data of the different fractions. As a result, two new fridamycins H (1) and I (2), along with three known compounds actinosporin C (3), D (4), and G (5) were isolated from the solid culture of sponge-associated actinomycete Actinokineospora spheciospongiae sp. nov., elicited with N-acetylglucosamine. Characterization of the isolated compounds was pursued using mass spectrometry and NMR spectral data. Fridamycin H (1) exhibited significant growth inhibitory activity towards Trypanosoma brucei strain TC221. These results highlight the potential of elicitation in sponge-associated actinomycetes as an effective strategy for the discovery of new anti-infective natural products.
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