Fructose-Induced Carbonyl/Oxidative Stress inS. cerevisiae: Involvement of TOR

Author:

Valishkevych Bohdana V.1,Vasylkovska Ruslana A.1,Lozinska Liudmyla M.12,Semchyshyn Halyna M.1

Affiliation:

1. Department of Biochemistry and Biotechnology, Vasyl Stefanyk Precarpathian National University, 57 Shevchenko Street, Ivano-Frankivsk 76018, Ukraine

2. Department of Biology, Lund University, Sölvegatan 35, 223 62 Lund, Sweden

Abstract

The TOR (target of rapamycin) signaling pathway first described in the budding yeastSaccharomyces cerevisiaeis highly conserved in eukaryotes effector of cell growth, longevity, and stress response. TOR activation by nitrogen sources, in particular amino acids, is well studied; however its interplay with carbohydrates and carbonyl stress is poorly investigated. Fructose is a more potent glycoxidation agent capable of producing greater amounts of reactive carbonyl (RCS) and oxygen species (ROS) than glucose. The increased RCS/ROS production, as a result of glycoxidationin vivo, is supposed to be involved in carbonyl/oxidative stress, metabolic disorders, and lifespan shortening of eukaryotes. In this work we aim to expand our understanding of how TOR is involved in carbonyl/oxidative stress caused by reducing monosaccharides. It was found that in fructose-grown compared with glucose-grown cells the level of carbonyl/oxidative stress markers was higher. The defects in the TOR pathway inhibited metabolic rate and suppressed generation of glycoxidation products in fructose-grown yeast.

Publisher

Hindawi Limited

Subject

Biochemistry

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