Hypoxia-induced p53 modulates both apoptosis and radiosensitivity via AKT
Katarzyna B. Leszczynska, … , Francesca M. Buffa, Ester M. Hammond
Katarzyna B. Leszczynska, … , Francesca M. Buffa, Ester M. Hammond
Published May 11, 2015
Citation Information: J Clin Invest. 2015;125(6):2385-2398. https://doi.org/10.1172/JCI80402.
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Research Article Oncology

Hypoxia-induced p53 modulates both apoptosis and radiosensitivity via AKT

Abstract

Restoration of hypoxia-induced apoptosis in tumors harboring p53 mutations has been proposed as a potential therapeutic strategy; however, the transcriptional targets that mediate hypoxia-induced p53-dependent apoptosis remain elusive. Here, we demonstrated that hypoxia-induced p53-dependent apoptosis is reliant on the DNA-binding and transactivation domains of p53 but not on the acetylation sites K120 and K164, which, in contrast, are essential for DNA damage–induced, p53-dependent apoptosis. Evaluation of hypoxia-induced transcripts in multiple cell lines identified a group of genes that are hypoxia-inducible proapoptotic targets of p53, including inositol polyphosphate-5-phosphatase (INPP5D), pleckstrin domain–containing A3 (PHLDA3), sulfatase 2 (SULF2), B cell translocation gene 2 (BTG2), cytoplasmic FMR1-interacting protein 2 (CYFIP2), and KN motif and ankyrin repeat domains 3 (KANK3). These targets were also regulated by p53 in human cancers, including breast, brain, colorectal, kidney, bladder, and melanoma cancers. Downregulation of these hypoxia-inducible targets associated with poor prognosis, suggesting that hypoxia-induced apoptosis contributes to p53-mediated tumor suppression and treatment response. Induction of p53 targets, PHLDA3, and a specific INPP5D transcript mediated apoptosis in response to hypoxia through AKT inhibition. Moreover, pharmacological inhibition of AKT led to apoptosis in the hypoxic regions of p53-deficient tumors and consequently increased radiosensitivity. Together, these results identify mediators of hypoxia-induced p53-dependent apoptosis and suggest AKT inhibition may improve radiotherapy response in p53-deficient tumors.

Authors

Katarzyna B. Leszczynska, Iosifina P. Foskolou, Aswin G. Abraham, Selvakumar Anbalagan, Céline Tellier, Syed Haider, Paul N. Span, Eric E. O’Neill, Francesca M. Buffa, Ester M. Hammond

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Figure 1

Hypoxia-induced p53-dependent apoptosis is associated with the expression of specific genes.

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Hypoxia-induced p53-dependent apoptosis is associated with the expressio...
(A and B) Apoptosis in H1299 cells expressing either WT p53 (p53) or the mutants (K120R, K164R, K120/164R, R175H) from the 5xHRE promoter and exposed to 24 hours of hypoxia (Hyp) or normoxia (Norm) detected by PARP cleavage or morphologically, respectively. For Western blotting, the lanes were run on the same gel but were noncontiguous. The bar graph shows mean ± SEM (combined n = 3, 2-way ANOVA test [****P < 0.0001]). (C) Microarray gene expression analysis in H1299 cells transfected with either 5xHRE-p53 or 5xHRE-p53R175H and exposed to 16 hours of hypoxia. Heat map showing the top candidate genes induced by hypoxia in a p53-dependent manner. Well-characterized proapoptotic p53 targets are shown in the bottom 6 rows. Fold change ratios of gene expression for 5xHRE-p53/5xHRE-p53R175H samples are shown in red for upregulated and blue for downregulated genes. Columns numbered 1 to 3 represent technical replicates of hypoxic samples. (D) qPCR testing of the hypoxic regulation of p53 target genes identified as being essential to its tumor-suppressive role by Brady et al. (22) in H1299 cells transfected with 5xHRE-p53 and exposed to 24 hours of hypoxia. The bar graph shows mean ± SEM (combined n = 3, 2-way ANOVA test [P < 0.0001] followed by 2-tailed Student’s t test [***P < 0.001; ****P < 0.0001].