What question did this study set out to answer?

To explore how AKT1-mediated phosphorylation of the glucocorticoid receptor contributes to resistance in prostate cancer therapy.

April 5, 2026

Abstract 332: AKT1 mediated post translational modification of the glucocorticoid receptor drives resistance to prostate cancer therapy.

Key Points

To explore how AKT1-mediated phosphorylation of the glucocorticoid receptor contributes to resistance in prostate cancer therapy.
Utilized GR-phospho proteomics data to analyze GR phosphorylation under enzalutamide resistance.
Identified AKT1 as the isoform responsible for phosphorylating GR at serine-134 via predictions from PhosphoNET.ca.
Conducted functional studies to assess the impact of AKT1 inhibition on GR activity and sensitivity to AR-targeted therapy.
Increased phosphorylation of GR at serine-134 was observed in enzalutamide-resistant prostate cancer cells.
Inhibiting AKT1 reduced GR phosphorylation at S134, restoring sensitivity to AR-directed therapy.
Suppression of pGR-s134 activity made cancer cells more vulnerable to enzalutamide and effective GR modulators.

Abstract

Abstract Increasing evidence shows that resistance to androgen-deprivation therapy (ADT) and next-generation androgen receptor (AR) antagonists in advanced prostate cancers develops partly through compensatory activation of alternative nuclear hormone receptors. Notably, induction of the glucocorticoid receptor (GR) has been demonstrated in both preclinical and clinical studies to confer resistance to AR-targeted therapies. Although total GR is crucial for tissue homeostasis and normal inflammatory responses, our preliminary GR-phospho proteomics data reveal that, under enzalutamide resistance, GR undergoes increased phosphorylation, especially at serine-134 (p-GR(s134)), suggesting a post-translational mechanism driving a pro-oncogenic GR activation in therapy-resistant tumors. We have previously shown that inhibiting AKT signaling, GR expression, and its pro-oncogenic activity restores sensitivity to AR-directed therapy. Predictions from PhosphoNET.ca and functional studies identify AKT1 as the AKT isoform responsible for phosphorylating GR at S134. Importantly, both functional and pharmacologic inhibition of AKT1 reduced GR phosphorylation at s134 without affecting total GR protein levels. While GR can be activated by ligands such as dexamethasone, our data suggest that, in PCa cells that adopt GR compensatory signaling for survival, GR activation is mediated by AKT1 phosphorylation. Overall, our data show that suppression of pGR-s134 activity renders these cancer cells re-vulnerable to AR-targeted drugs such as enzalutamide and enhances their response to GR modulators. Citation Format: Surendra Gulla, Tej Sharma, Ephraim Gardner, Abbas Jawadala, Sasikumar Ponnusamy, Tobi Ogunbowale, Maddie Aust, Jonathan E. Bard, Remi Adelaiye-Ogala. AKT1 mediated post translational modification of the glucocorticoid receptor drives resistance to prostate cancer therapy abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 332.

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Abstract 332: AKT1 mediated post translational modification of the glucocorticoid receptor drives resistance to prostate cancer therapy.

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