The isoprenyl chain length of coenzyme Q mediates the nutritional resistance of fungi to amoeba predation

Nauman Saeed; Vito Valiante; Johann E Kufs; Falk Hillmann

doi:10.1128/mbio.00342-24

The isoprenyl chain length of coenzyme Q mediates the nutritional resistance of fungi to amoeba predation

mBio. 2024 May 15:e0034224. doi: 10.1128/mbio.00342-24. Online ahead of print.

Authors

Nauman Saeed^{1

2

3}, Vito Valiante⁴, Johann E Kufs⁵, Falk Hillmann³

Affiliations

¹ Evolution of Microbial Interactions, Leibniz Institute for Natural Product Research and Infection Biology (HKI), Jena, Germany.
² Institute of Microbiology, Faculty of Biological Sciences, Friedrich Schiller University Jena, Jena, Germany.
³ Biochemistry/Biotechnology, Faculty of Engineering, Wismar University of Applied Sciences Technology, Business and Design, Wismar, Germany.
⁴ Biobricks of Microbial Natural Product Syntheses, Leibniz Institute for Natural Product Research and Infection Biology (HKI), Jena, Germany.
⁵ Genome Engineering and Editing, Faculty of Technology, Bielefeld University, Bielefeld, Germany.

PMID: 38747615
DOI: 10.1128/mbio.00342-24

Abstract

Amoebae are environmental predators feeding on bacteria, fungi, and other eukaryotic microbes. Predatory interactions alter microbial communities and impose selective pressure toward phagocytic resistance or escape which may, in turn, foster virulence attributes. The ubiquitous fungivorous amoeba Protostelium aurantium has a wide prey spectrum in the fungal kingdom but discriminates against members of the Saccharomyces clade, such as Saccharomyces cerevisiae and Candida glabrata. Here, we show that this prey discrimination among fungi is solely based on the presence of ubiquinone as an essential cofactor for the predator. While the amoeba readily fed on fungi with CoQ presenting longer isoprenyl side chain variants CoQ8-10, such as those from the Candida clade, it failed to proliferate on those with shorter CoQ variants, specifically from the Saccharomyces clade (CoQ6). Supplementing non-edible yeast with CoQ9 or CoQ10 rescued the growth of P. aurantium, highlighting the importance of a long isoprenyl side chain. Heterologous biosynthesis of CoQ9 in S. cerevisiae by introducing genes responsible for CoQ9 production from the evolutionary more basic Yarrowia lipolytica complemented the function of the native CoQ6. The results suggest that the use of CoQ6 among members of the Saccharomyces clade might have originated as a predatory escape strategy in fungal lineages and could be retained in organisms that were able to thrive by fermentation.

Importance: Ubiquinones (CoQ) are universal electron carriers in the respiratory chain of all aerobic bacteria and eukaryotes. Usually 8-10 isoprenyl units ensure their localization within the lipid bilayer. Members of the Saccharomyces clade among fungi are unique in using only 6. The reason for this is unclear. Here we provide evidence that the use of CoQ6 efficiently protects these fungi from predation by the ubiquitous fungivorous amoeba Protostelium aurantium which lacks its own biosynthetic pathway for this vitamin. The amoebae were starving on a diet of CoQ6 yeasts which could be complemented by either the addition of longer CoQs or the genetic engineering of a CoQ9 biosynthetic pathway.

Keywords: Candida; Saccharomyces; amoeba; coenzyme Q; predation; ubiquinone; yeast.