Application of Feature-Based Molecular Networking for Comparative Metabolomics and Targeted Isolation of Stereoisomers from Algicolous Fungi

Bicheng Fan; Laura Grauso; Fengjie Li; Silvia Scarpato; Alfonso Mangoni; Deniz Tasdemir

doi:10.3390/md20030210

Application of Feature-Based Molecular Networking for Comparative Metabolomics and Targeted Isolation of Stereoisomers from Algicolous Fungi

Mar Drugs. 2022 Mar 16;20(3):210. doi: 10.3390/md20030210.

Authors

Bicheng Fan¹, Laura Grauso², Fengjie Li¹, Silvia Scarpato³, Alfonso Mangoni³, Deniz Tasdemir^{1

4}

Affiliations

¹ GEOMAR Centre for Marine Biotechnology (GEOMAR-Biotech), Research Unit Marine Natural Product Chemistry, GEOMAR Helmholtz Centre for Ocean Research Kiel, Am Kiel-Kanal 44, 24106 Kiel, Germany.
² Dipartimento di Agraria, Università degli Studi di Napoli Federico II, 80055 Portici, Italy.
³ Dipartimento di Farmacia, Università degli Studi di Napoli Federico II, 80131 Napoli, Italy.
⁴ Faculty of Mathematics and Natural Sciences, Kiel University, Christian-Albrechts-Platz 4, 24118 Kiel, Germany.

Abstract

Seaweed endophytic (algicolous) fungi are talented producers of bioactive natural products. We have previously isolated two strains of the endophytic fungus, Pyrenochaetopsis sp. FVE-001 and FVE-087, from the thalli of the brown alga Fucus vesiculosus. Initial chemical studies yielded four new decalinoylspirotetramic acid derivatives with antimelanoma activity, namely pyrenosetins A-C (1-3) from Pyrenochaetopsis sp. strain FVE-001, and pyrenosetin D (4) from strain FVE-087. In this study, we applied a comparative metabolomics study employing HRMS/MS based feature-based molecular networking (FB MN) on both Pyrenochaetopsis strains. A higher chemical capacity in production of decalin derivatives was observed in Pyrenochaetopsis sp. FVE-087. Notably, several decalins showed different retention times despite the same MS data and MS/MS fragmentation pattern with the previously isolated pyrenosetins, indicating they may be their stereoisomers. FB MN-based targeted isolation studies coupled with antimelanoma activity testing on the strain FVE-087 afforded two new stereoisomers, pyrenosetins E (5) and F (6). Extensive NMR spectroscopy including DFT computational studies, HR-ESIMS, and Mosher's ester method were used in the structure elucidation of compounds 5 and 6. The 3'R,5'R stereochemistry determined for compound 6 was identical to that previously reported for pyrenosetin C (3), whose stereochemistry was revised as 3'S,5'R in this study. Pyrenosetin E (5) inhibited the growth of human malignant melanoma cells (A-375) with an IC₅₀ value of 40.9 μM, while 6 was inactive. This study points out significant variations in the chemical repertoire of two closely related fungal strains and the versatility of FB MN in identification and targeted isolation of stereoisomers. It also confirms that the little-known fungal genus Pyrenochaetopsis is a prolific source of complex decalinoylspirotetramic acid derivatives.

Keywords: Fucus vesiculosus; Pyrenochaetopsis sp.; anticancer; decalinoylspirotetramic acid; feature-based molecular networking; malignant melanoma; pyrenosetin; stereoisomers.

Publication types

Comparative Study

MeSH terms

Ascomycota / metabolism*
Cell Line
Cell Survival / drug effects
Complex Mixtures / chemistry*
Complex Mixtures / pharmacology
Endophytes / metabolism*
Fucus / microbiology*
Humans
Metabolomics
Seaweed / microbiology*
Stereoisomerism

Substances

Complex Mixtures