The hVps34‐
            <scp>SGK</scp>
            3 pathway alleviates sustained PI3K/Akt inhibition by stimulating
            <scp>mTORC</scp>
            1 and tumour growth

Bago, Ružica; Sommer, Eeva; Castel, Pau; Crafter, Claire; Bailey, Fiona P.; Shpiro, Natalia; Baselga, José; Cross, Darren A.E.; Eyers, Patrick A.; Alessi, Dario R.

doi:10.15252/embj.201693929

Cited by 81 publications

(135 citation statements)

References 62 publications

(95 reference statements)

Supporting

Mentioning

124

Contrasting

Order By: Relevance

“…The almost undetectable expression of Sgk2 suggests that this isoform is unlikely to play a critical role in the control of thyroid cell proliferation. On the other hand, Sgk3 is unique among the SGK genes, since it has a N-terminal PX-domain targeting the protein to the endosomes, where it is activated in response to the class III PI3K Vps34 (23). Based on these notions, as well as on preliminary shRNA-based experiments showing very limited effects of Sgk3 depletion on cell proliferation (Suppl.…”

Section: Resultsmentioning

confidence: 99%

SGK1 Is a Critical Component of an AKT-Independent Pathway Essential for PI3K-Mediated Tumor Development and Maintenance

et al. 2017

View full text Add to dashboard Cite

Activation of the PI3K-AKT signaling cascade is a common critical event during malignant transformation. In this study, we used thyroid gland epithelial cells and a series of genetically engineered mouse strains as model systems to demonstrate that, while necessary, AKT activation is not sufficient for PI3K-driven transformation. Instead, transformation requires the activity of the PDK1-regulated AGC family of protein kinases. In particular, SGK1 was found to be essential for proliferation and survival of thyroid cancer cells harboring PI3K-activating mutations. Notably, co-targeting SGK1 and AKT resulted in significantly higher growth suppression than inhibiting either PI3K or AKT alone. Overall, these findings underscore the clinical relevance of AKT-independent pathways in tumors driven by genetic lesions targeting the PI3K cascade.

show abstract

Section: Resultsmentioning

confidence: 99%

SGK1 Is a Critical Component of an AKT-Independent Pathway Essential for PI3K-Mediated Tumor Development and Maintenance

et al. 2017

View full text Add to dashboard Cite

show abstract

“…Analysis of 18 biopsies from patients treated with alpelisib showed that samples with high SGK1 mRNA and phospho-N-Myc downstream regulated 1 (NDRG1; a substrate for and biomarker of SGK1 activation) levels correlated with intrinsic resistance to alpelisib, whereas most phospho-NDRG1-negative tumors were from patients who attained partial responses or stable disease. Similarly, SGK3 overexpression and/or activation has been repeatedly linked to PI3K/mTOR inhibitor resistance in breast cancer cells (Bago et al, 2016; Gasser et al, 2014). These reports offer a common mechanism for intrinsic or acquired resistance to PI3K or AKT inhibitors.…”

Section: Therapeutic Targeting Of the Pi3k Pathway In Cancermentioning

confidence: 99%

The PI3K Pathway in Human Disease

Fruman

Chiu

Hopkins

et al. 2017

Cell

1,886

1,658

View full text Add to dashboard Cite

Phosphoinositide 3-kinase (PI3K) activity is stimulated by diverse oncogenes and growth factor receptors, and elevated PI3K signaling is considered a hallmark of cancer. Many PI3K pathway-targeted therapies have been tested in oncology trials, resulting in regulatory approval of one isoform-selective inhibitor (idelalisib) for treatment of certain blood cancers, and a variety of other agents at different stages of development. In parallel to PI3K research by cancer biologists, investigations in other fields have uncovered exciting and often unpredicted roles for PI3K catalytic and regulatory subunits in normal cell function and in disease. Many of these functions impinge upon oncology by influencing the efficacy and toxicity of PI3K-targeted therapies. Here we provide a perspective on the roles of class I PI3Ks in the regulation of cellular metabolism and in immune system functions, two topics closely intertwined with cancer biology. We also discuss recent progress developing PI3K-targeted therapies for treatment of cancer and other diseases.

show abstract

“…SGK3 has been shown to play a pivotal role in Akt-independent signaling downstream of oncogenic PIK3CA mutations in some human cancers, including breast cancer (11). Most recently, Bago et al reported that SGK3 counteracts the inhibition of PI3K/Akt signaling and stimulates tumor growth (12). SGK3 is amplified and hyperactivated in breast cancer (13), and its expression is regulated by ERα and positively correlates with ERα levels in breast tumors (14,15).…”

mentioning

confidence: 99%

SGK3 sustains ERα signaling and drives acquired aromatase inhibitor resistance through maintaining endoplasmic reticulum homeostasis

Wang

Zhou

Phung

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Many estrogen receptor alpha (ERα)-positive breast cancers initially respond to aromatase inhibitors (AIs), but eventually acquire resistance. Here, we report that serum-and glucocorticoid-inducible kinase 3 (SGK3), a kinase transcriptionally regulated by ERα in breast cancer, sustains ERα signaling and drives acquired AI resistance. SGK3 is up-regulated and essential for endoplasmic reticulum (EnR) homeostasis through preserving sarcoplasmic/EnR calcium ATPase 2b (SERCA2b) function in AI-resistant cells. We have further found that EnR stress response down-regulates ERα expression through the protein kinase RNA-like EnR kinase (PERK) arm, and SGK3 retains ERα expression and signaling by preventing excessive EnR stress. Our study reveals regulation of ERα expression mediated by the EnR stress response and the feed-forward regulation between SGK3 and ERα in breast cancer. Given SGK3 inhibition reduces AI-resistant cell survival by eliciting excessive EnR stress and also depletes ERα expression/function, we propose SGK3 inhibition as a potential effective treatment of acquired AI-resistant breast cancer.SGK3 | aromatase inhibitor | endoplasmic reticulum stress | estrogen receptor | SERCA2

show abstract

The hVps34‐ SGK 3 pathway alleviates sustained PI3K/Akt inhibition by stimulating mTORC 1 and tumour growth

Cited by 81 publications

References 62 publications

SGK1 Is a Critical Component of an AKT-Independent Pathway Essential for PI3K-Mediated Tumor Development and Maintenance

SGK1 Is a Critical Component of an AKT-Independent Pathway Essential for PI3K-Mediated Tumor Development and Maintenance

The PI3K Pathway in Human Disease

SGK3 sustains ERα signaling and drives acquired aromatase inhibitor resistance through maintaining endoplasmic reticulum homeostasis

Contact Info

Product

Resources

About