March 3, 2026Open Access

SUMOylation of UBE2C facilitates hepatocellular carcinoma proliferation and invasion via the MAPK pathway

Puntos clave

UBE2C expression and stability are enhanced through MYBL2 and SUMOylation, leading to increased hepatocellular carcinoma proliferation and invasion.
MAPK pathway activation is a key mechanism through which UBE2C promotes tumor progression, representing a critical axis for therapeutic targeting.
This study identifies a previously unknown oncogenic axis, indicating that targeting MYBL2/UBE2C could provide a new therapeutic approach for hepatocellular carcinoma.
The findings highlight the importance of the oncogenic interactions in HCC, calling for further exploration of their therapeutic implications.

Resumen

We reveal a novel oncogenic axis in which MYBL2 and SUMOylation cooperatively increase UBE2C expression and stability, promoting HCC progression via MAPK pathway activation. Targeting the MYBL2/UBE2C/MAPK axis represents a potential therapeutic strategy for treating HCC.

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