eIF2α phosphorylation bypasses premature senescence caused by oxidative stress and pro-oxidant antitumor therapies

Kamindla Rajesh; Andreas I. Papadakis; Urszula Kazimierczak; Philippos Peidis; Shuo Wang; Gerardo Ferbeyre; Randal J. Kaufman; Antonis E. Koromilas

doi:doi:10.18632/aging.100620

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Research Paper Volume 5, Issue 12 pp 884—901

eIF2α phosphorylation bypasses premature senescence caused by oxidative stress and pro-oxidant antitumor therapies

Figure 2. Impaired eIF2α phosphorylation is associated with increased DNA Damage and G/M arrest. (A) eIF2αS/S and eIF2αA/A MEFs from passage 3 were stained for γ-H2AX and analyzed by fluorescence microscopy. DAPI staining was used to visualize nuclei. Histograms show the average number of γ-H2AX foci per cell (n=100). (B) eIF2αS/S and eIF2αA/A MEFs from passage 3 were subjected to cell cycle analysis by FACS. Histograms indicate the percentages of cells in G₀/G₁, S and G₂/M from three independent experiments. (C) Protein extracts (50 μg) from eIF2αS/S and eIF2αA/A MEFs from passage 3 were immunoblotted for the indicated proteins.