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  1. Pubblicazioni

Functional role of SGK3 in PI3K/Pten driven liver tumor development

Articolo
Data di Pubblicazione:
2019
Citazione:
Functional role of SGK3 in PI3K/Pten driven liver tumor development / Cao, H.; Xu, Z.; Wang, J.; Cigliano, A.; Pilo, M. G.; Ribback, S.; Zhang, S.; Qiao, Y.; Che, L.; Pascale, R. M.; Calvisi, D. F.; Chen, X.. - In: BMC CANCER. - ISSN 1471-2407. - 19:1(2019). [10.1186/s12885-019-5551-2]
Abstract:
Background: Hepatocellular carcinoma (HCC) is a leading cause of cancer related deaths worldwide. The PI3K cascade is one of the major signaling pathways underlying HCC development and progression. Activating mutations of PI3K catalytic subunit alpha (PIK3CA) and/or loss of Pten often occur in human HCCs. Serum and glucocorticoid kinase 3 (SGK3) belongs to the SGK family of AGK kinases and functions in parallel to AKT downstream of PI3K. Previous studies have shown that SGK3 may be the major kinase responsible for the oncogenic potential of PIK3CA helical domain mutants, such as PIK3CA(E545K), but not kinase domain mutants, such as PIK3CA(H1047R). Methods: We investigated the functional contribution of SGK3 in mediating activated PIK3CA mutant or loss of Pten induced HCC development using Sgk3 knockout mice. Results: We found that ablation of Sgk3 does not affect PIK3CA(H1047R) or PIK3CA(E545K) induced lipogenesis in the liver. Using PIK3CA(H1047R)/c-Met, PIK3CA(E545K)/c-Met, and sgPten/c-Met murine HCC models, we also demonstrated that deletion of Sgk3 moderately delays PIK3CA(E545K)/c-Met driven HCC, while not affecting PIK3CA(H1047R)/c-Met or sgPten/c-Met HCC formation in mice. Similarly, in human HCC cell lines, silencing of SGK3 reduced PIK3CA(E545K) -but not PIK3CA(H1047R)- induced accelerated tumor cell proliferation. Conclusion: Altogether, our data suggest that SGK3 plays a role in transducing helical domain mutant PIK3CA signaling during liver tumor development.
Tipologia CRIS:
1.1 Articolo in rivista
Keywords:
c-Met; Liver cancer; mTOR; PIK3CA mutants; Pten; SGK3
Elenco autori:
Cao, H.; Xu, Z.; Wang, J.; Cigliano, A.; Pilo, M. G.; Ribback, S.; Zhang, S.; Qiao, Y.; Che, L.; Pascale, R. M.; Calvisi, D. F.; Chen, X.
Autori di Ateneo:
CALVISI Diego Francesco
PASCALE Rosa Maria
Link alla scheda completa:
https://iris.uniss.it/handle/11388/240475
Pubblicato in:
BMC CANCER
Journal
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