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Stratifin promotes the malignant progression of HCC via binding and hyperactivating AKT signaling

Rong Li, Xijing Yan, Wenhui Zhong, Jun Zheng, Xuejiao Li, Jinliang Liang, Zhongying Hu, Huanyi Liu, Guihua Chen, Yang Yang, Jianwei Zhang, Enze Qu, Wei Liu, Wei Liu

2024Cancer Letters13 citationsDOIOpen Access PDF

Abstract

Hepatocellular carcinoma (HCC) is a highly aggressive malignant tumor with limited treatment options and poor prognosis. In this study, we reveal the pivotal role of Stratifin (SFN), also recognized as 14-3-3σ, in driving HCC progression. Our investigation underscores a substantial upregulation of SFN within HCC tissues, manifesting a significant association with worse prognostic outcomes among HCC patients. In vitro and in vivo experiments reveal that SFN overexpression significantly amplifies proliferation, mitigates sorafenib-induced effects on HCC cells, and enhances tumorigenesis. While SFN silencing exerts converse effects on HCC progression. Additionally, we unveil a critical interaction between SFN and AKT, where SFN boosts AKT kinase activity by disrupting the binding of PHLPP2 and AKT, thereby intensifying the malignant progression of HCC cells. In conclusion, this study identifies the oncogenic role of SFN and elucidates the regulatory mechanism of the SFN/AKT axis in HCC, which may provide valuable insights into the mechanisms of HCC progression and potential targets for therapeutic intervention.

Topics & Concepts

Protein kinase BCancer researchHepatocellular carcinomaDownregulation and upregulationGene silencingTumor progressionSorafenibCarcinogenesisMedicineOncologySignal transductionInternal medicineBiologyCancerCell biologyBiochemistryGene14-3-3 protein interactionsUbiquitin and proteasome pathwaysCancer Mechanisms and Therapy
Stratifin promotes the malignant progression of HCC via binding and hyperactivating AKT signaling | Litcius