Hog1 acts in a Mec1-independent manner to counteract oxidative stress following telomerase inactivation

Author:

Zeinoun Bechara,Teixeira Maria TeresaORCID,Barascu Aurélia

Abstract

AbstractReplicative senescence is triggered when telomeres reach critically short length and activate permanent DNA damage checkpoint-dependent cell cycle arrest. Mitochondrial dysfunction and increase in oxidative stress are both features of replicative senescence in mammalian cells. Here, we show that reactive oxygen species (ROS) levels increase in the telomerase-negative cells ofSaccharomyces cerevisiaeduring replicative senescence, and that this coincides with the activation of Hog1, a mammalian p38 mitogen-activated protein kinase (MAPK) ortholog. Hog1 activation is dependent on Pbs2, the MAPK kinase (MAPKK) in its canonical pathway, and counteracts increased ROS levels during replicative senescence. While Hog1 deletion accelerates replicative senescence, we found this could stem from decreased telomere length and reduced cell viability prior to telomerase inactivation. ROS levels also increase upon telomerase inactivation when Mec1, the yeast ortholog of ATR, is mutated, suggesting that oxidative stress is not simply a consequence of DNA damage checkpoint activation in budding yeast. We speculate that oxidative stress is a conserved hallmark of telomerase-negative eukaryote cells, and that its sources and consequences can be dissected inS. cerevisiae.

Publisher

Cold Spring Harbor Laboratory

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