AI Article Synopsis
- The study investigates the effects of losing tumor suppressors Pten and p53 in breast cancer, revealing that their combined loss leads to faster tumor formation and more aggressive claudin-low, triple-negative-like breast cancers (TNBC).
- Mammary-specific deletion of Pten resulted in different tumor characteristics based on the progenitor cells targeted, indicating a distinct impact on tumor behavior.
- Researchers found that eEF2K inhibitors are more effective than traditional treatments on TNBC cells lacking Pten and p53, suggesting a new therapeutic approach tailored for these patients with high AKT signaling.
Article Abstract
The tumor suppressors Pten and p53 are frequently lost in breast cancer, yet the consequences of their combined inactivation are poorly understood. Here, we show that mammary-specific deletion of Pten via WAP-Cre, which targets alveolar progenitors, induced tumors with shortened latency compared to those induced by MMTV-Cre, which targets basal/luminal progenitors. Combined Pten-p53 mutations accelerated formation of claudin-low, triple-negative-like breast cancer (TNBC) that exhibited hyper-activated AKT signaling and more mesenchymal features relative to Pten or p53 single-mutant tumors. Twenty-four genes that were significantly and differentially expressed between WAP-Cre:Pten/p53 and MMTV-Cre:Pten/p53 tumors predicted poor survival for claudin-low patients. Kinome screens identified eukaryotic elongation factor-2 kinase (eEF2K) inhibitors as more potent than PI3K/AKT/mTOR inhibitors on both mouse and human Pten/p53-deficient TNBC cells. Sensitivity to eEF2K inhibition correlated with AKT pathway activity. eEF2K monotherapy suppressed growth of Pten/p53-deficient TNBC xenografts in vivo and cooperated with doxorubicin to efficiently kill tumor cells in vitro. Our results identify a prognostic signature for claudin-low patients and provide a rationale for using eEF2K inhibitors for treatment of TNBC with elevated AKT signaling.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4287974 | PMC |
| http://dx.doi.org/10.15252/emmm.201404402 | DOI Listing |
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