Cytostatic effects of structurally different ginsenosides on yeast cells with altered sterol biosynthesis and transport

三萜 甾醇 麦角甾醇 皂甙 生物化学 糖苷 人参皂甙 环蒿醇 人参 酵母 化学 酿酒酵母 生物 立体化学 胆固醇 医学 替代医学 病理
作者
С. С. Соколов,Pavel E. Volynsky,O. T. Zangieva,Fedor F. Severin,Elena S. Glagoleva,Dmitry A. Knorre
出处
期刊:Biochimica Et Biophysica Acta - Biomembranes [Elsevier]
卷期号:1864 (10): 183993-183993 被引量:5
标识
DOI:10.1016/j.bbamem.2022.183993
摘要

Triterpene glycosides are a diverse group of plant secondary metabolites, consisting of a sterol-like aglycon and one or several sugar groups. A number of triterpene glycosides show membranolytic activity, and, therefore, are considered to be promising antimicrobial drugs. However, the interrelation between their structure, biological activities, and target membrane lipid composition remains elusive. Here we studied the antifungal effects of four Panax triterpene glycosides (ginsenosides) with sugar moieties at the C-3 (ginsenosides Rg3, Rh2), C-20 (compound K), and both (ginsenoside F2) positions in Saccharomyces cerevisiae mutants with altered sterol plasma membrane composition. We observed reduced cytostatic activity of the Rg3 and compound K in the UPC2-1 strain with high membrane sterol content. Moreover, LAM gene deletion reduced yeast resistance to Rg3 and digitonin, another saponin with glycosylated aglycon in the C-3 position. LAM genes encode plasma membrane-anchored StARkin superfamily-member sterol transporters. We also showed that the deletion of the ERG6 gene that inhibits ergosterol biosynthesis at the stage of zymosterol increased the cytostatic effects of Rg3 and Rh2, but not the other two tested ginsenosides. At the same time, in silico simulation revealed that the substitution of ergosterol with zymosterol in the membrane changes the spatial orientation of Rg3 and Rh2 in the membranes. These results imply that the plasma membrane sterol composition defines its interaction with triterpene glycoside depending on their glycoside group position. Our results also suggest that the biological role of membrane-anchored StARkin family protein is to protect eukaryotic cells from triterpenes glycosylated at the C-3 position.
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