Cercospora sp. as a source of anti-aging polyketides targeting 26S proteasome and scale-up production in submerged bioreactor
[Display omitted] •Cercospora sp. was identified as a source of proteasome activators.•Three Polyketides were isolated, identified and tested in vitro for their effect on proteasome.•Fulvic acid showed an activation effect on 26S proteasome.•Production of fulvic acid in submerged bioreactor was opti...
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Veröffentlicht in: | Journal of biotechnology 2019-08, Vol.301, p.88-96 |
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Sprache: | eng |
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•Cercospora sp. was identified as a source of proteasome activators.•Three Polyketides were isolated, identified and tested in vitro for their effect on proteasome.•Fulvic acid showed an activation effect on 26S proteasome.•Production of fulvic acid in submerged bioreactor was optimized at 162.3 mg of fulvic acid/L.
From a large screening of microbial extracts for the discovery of proteasome modulating natural products, the fungal strain Cercospora sp. (CF-223709) was selected as the most promising for further investigation. Different liquid cultures of the strain were initially screened for their anti-oxidant activity (DPPH, ABTS) and for their cytotoxicity against the A2058, HepG2 and CCD25sk cell lines. A detailed chemical analysis and evaluation of the capacity to activate 26S-proteasome was followed for the most active extract. Three main polyketides were isolated and characterized by extensive analysis of NMR and HRMS spectra data as penialidine F (1), fulvic acid (2), and SB238569 (3). Fulvic acid showed the most significant anti-oxidant activity. Its IC50 value (8.16 μM) against the ABTS radical resulted 3-fold lower than the standard trolox. Fulvic acid also demonstrated a significant effect on proteasome by enhancing the chymotrypsin- and caspase-like activities of the 26S proteasome of human fibroblasts by 71.43% and 37.5% at 1 μM, respectively. Furthermore by scaling up the culture in a 30 L submerged bioreactor, Cercospora sp. produced up to 162.6 ± 1.3 mg of fulvic acid/L. Our findings suggest that CF-223709 can be a promising source of proteasome activating natural compounds. |
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ISSN: | 0168-1656 1873-4863 |
DOI: | 10.1016/j.jbiotec.2019.05.015 |