| Literature DB >> 31655859 |
Andrea Magrì1,2,3, Maria Carmela Di Rosa1,3, Ivan Orlandi4, Francesca Guarino1,3, Simona Reina1,2,3, Maria Guarnaccia5, Giovanna Morello5, Antonio Spampinato5, Sebastiano Cavallaro5, Angela Messina2,3, Marina Vai6, Vito De Pinto7,8.
Abstract
The Voltage-Dependent Anion-selective Channel (VDAC) is the pore-forming protein of mitochondrial outer membrane, allowing metabolites and ions exchanges. In Saccharomyces cerevisiae, inactivation of POR1, encoding VDAC1, produces defective growth in the presence of non-fermentable carbon source. Here, we characterized the whole-genome expression pattern of a VDAC1-null strain (Δpor1) by microarray analysis, discovering that the expression of mitochondrial genes was completely abolished, as consequence of the dramatic reduction of mtDNA. To overcome organelle dysfunction, Δpor1 cells do not activate the rescue signaling retrograde response, as ρ0 cells, and rather carry out complete metabolic rewiring. The TCA cycle works in a "branched" fashion, shunting intermediates towards mitochondrial pyruvate generation via malic enzyme, and the glycolysis-derived pyruvate is pushed towards cytosolic utilization by PDH bypass rather than the canonical mitochondrial uptake. Overall, Δpor1 cells enhance phospholipid biosynthesis, accumulate lipid droplets, increase vacuoles and cell size, overproduce and excrete inositol. Such unexpected re-arrangement of whole metabolism suggests a regulatory role of VDAC1 in cell bioenergetics.Entities:
Keywords: Fatty acids; Inositol; Mitochondrial DNA; PDH bypass; Porin; Retrograde signaling; Warburg effect
Year: 2019 PMID: 31655859 DOI: 10.1007/s00018-019-03342-8
Source DB: PubMed Journal: Cell Mol Life Sci ISSN: 1420-682X Impact factor: 9.261