Author:
Johnston Emily J.,Tallis Jess,Cunningham-Oakes Edward,Moses Tessa,Moore Simon J.,Hosking Sarah,Rosser Susan J.
Abstract
AbstractEscin is a mixture of over 30 glycosylated triterpenoid (saponin) structures, extracted from the dried fruit of horse chestnuts. Escin is currently used as an anti-inflammatory, and has potential applications in the treatment of arthritis and cancer. Engineered yeast would enable production of specific bioactive components of escin at industrial scale, however many saponins have been shown to be toxic to yeast. Here we report that a Saccharomyces cerevisiae strain specifically lacking the sterol C-5 desaturase gene ERG3, exhibits striking enhanced tolerance to escin treatment. Transcriptome analyses, as well as pre-mixing of escin with sterols, support the hypothesis that escin interacts directly with ergosterol, but not as strongly with the altered sterols present in erg3Δ. A diverse range of saponins are of commercial interest, and this research highlights the value of screening lipidome mutants to identify appropriate hosts for engineering the industrial production of saponins.
Funder
Industrial Biotechnology Innovation Centre
Biotechnology and Biological Sciences Research Council
BBSRC, EPSRC and Innovate UK
BBSRC and IBioIC
Publisher
Springer Science and Business Media LLC
Cited by
1 articles.
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