Mutant p53 induces a hypoxia transcriptional program in gastric and esophageal adenocarcinoma
Nilay Sethi, … , William G. Kaelin Jr., Adam J. Bass
Nilay Sethi, … , William G. Kaelin Jr., Adam J. Bass
Published August 8, 2019
Citation Information: JCI Insight. 2019;4(15):e128439. https://doi.org/10.1172/jci.insight.128439.
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Research Article Oncology

Mutant p53 induces a hypoxia transcriptional program in gastric and esophageal adenocarcinoma

Abstract

Despite the propensity for gastric and esophageal adenocarcinomas to select for recurrent missense mutations in TP53, the precise functional consequence of these mutations remains unclear. Here we report that endogenous mRNA and protein levels of mutant p53 were elevated in cell lines and patients with gastric and esophageal cancer. Functional studies showed that mutant p53 was sufficient, but not necessary, for enhancing primary tumor growth in vivo. Unbiased genome-wide transcriptome analysis revealed that hypoxia signaling was induced by mutant p53 in 2 gastric cancer cell lines. Using real-time in vivo imaging, we confirmed that hypoxia reporter activity was elevated during the initiation of mutant p53 gastric cancer xenografts. Further investigation revealed that, like mutant p53, the HIF1/ARNT hypoxia pathway was not required for the primary tumor functions of advanced mutant p53 gastric cancer. These findings indicate that recurrent p53 mutations in gastroesophageal adenocarcinoma are unlikely to serve as effective therapeutic targets in advanced cancer. However, in elucidating the contribution of missense mutant p53 and hypoxia signaling, the results suggest hypotheses regarding how these recurrent genomic events may contribute to gastric and esophageal adenocarcinoma formation.

Authors

Nilay Sethi, Osamu Kikuchi, James McFarland, Yanxi Zhang, Max Chung, Nicholas Kafker, Mirazul Islam, Benjamin Lampson, Abhishek Chakraborty, William G. Kaelin Jr., Adam J. Bass

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Figure 5

Mutant p53 activates downstream mediators of hypoxia in gastric dysplasia and cancer.

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Mutant p53 activates downstream mediators of hypoxia in gastric dysplasi...
(A) HIF-responsive promoter (HRE) firefly luciferase reporter activity in HEK293T cells transiently transfected with the indicated mutant p53 constructs; 1 mM DMOG treatment was used as a positive control. Data were normalized to cotransfected constitutively active Renilla luciferase activity. (B) Immunoblot showing protein expression levels of NDRG1, HIF1α, and p53 in HGC27 cells expressing the indicated mutant p53. (C) Gene expression levels of TP53, VEGFA, and BCL2 in control or p53-R175H–overexpression HGC27 cells. Results are shown as mean ± SD. P values were calculated by Student’s t test (D) Protein expression of HIF1α and p53 in conditional Trp53LSL-R270H/+ dysplastic gastric organoids derived from MNU-exposed mice with and without AdenoCre virus in the presence or absence of 1 mM DMOG by immunoblot analysis. (E) Histopathology of dysplastic gastric lesions in Mist-p53+/– and Mist-p53R270H/+ mice after 1 year of DCA/MNU treatment. H&E staining (left panel); and HIF1α IHC (right panels). Scale bars: 250 μm.