March 3, 2026Open Access

Coexistent PTEN and PIK3CA alterations hyperactivate mTORC1 signaling in endometrial cancers and cause their selective sensitivity to mTORC1 inhibition

Key Points

Endometrial cancers with PTEN and PIK3CA alterations exhibit hyperactivated mTORC1 signaling, indicating a unique treatment need.
Tumors with both mutations resist PI3K and AKT inhibitors but show sensitivity to mTORC1 inhibition, revealing a critical therapeutic target.
Assessment of coexistent PTEN and PIK3CA mutations demonstrates their role in cancer signaling pathways, emphasizing the importance of targeted treatments.
This analysis highlights the potential for mTORC1 inhibition as a targeted strategy in specific endometrial cancers, with implications for future therapies.

Abstract

We have found the mechanistic consequences of PTEN/PIK3CA co-alterations in endometrial tumors and that these mutations result in a profound hyperactivation of mTORC1 signaling. Single mutant tumors are sensitive to PI3K inhibition but those with both mutations are insensitive to PI3K or AKT inhibition but are exquisitely dependent on mTORC1 kinase. This provides strong preclinical rationale for targeting mTORC1, alone or combined with RAS inhibition (in RAS co-mutant tumors), as an effective therapeutic strategy.

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Coexistent PTEN and PIK3CA alterations hyperactivate mTORC1 signaling in endometrial cancers and cause their selective sensitivity to mTORC1 inhibition

Key Points

Abstract

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