Abstract 19P
Background
Hepatocellular carcinoma (HCC) ranks as the 6th most commonly diagnosed cancer worldwide and is the 3rd leading cause of cancer-related deaths. More than 50% of patients with HCC exhibit abnormal activation of the RAS-RAF-MEK-ERK signaling pathway in their tumors. Kinase Suppressor of Ras 1 (KSR1) is a pivotal scaffold protein for the RAS-RAF-MEK-ERK signaling pathway and facilitates the assembly and activation of key signaling components within the pathway. Here, we investigated the oncogenic role of KSR1 in hepatic tumorigenesis and therapeutic effects of targeting KSR1 on HCC induced by activated RAS-RAF-MEK-ERK signaling.
Methods
Transgenic mouse model for HCC was created via hydrodynamic tail veil injection (HTVI). Livers were harvested and examined for the presence of tumors through gross examination. Tumor tissues were then formalin-fixed and further processed for immunohistochemical analysis. To suppress the activity of KSR1 in HCC induced in the murine model, we employed two approaches: the expression of short hairpin RNA downregulating KSR1 (shKSR1) in the tumor, and the administration of mice with APS-2-79, a pharmacological inhibitor of KSR.
Results
Tumors were observed in livers expressing both KSR1 and shRNA down-regulating P53 (shP53), while the expression of KSR1 or shP53 alone failed to induce tumors. Expression of KSR1 led to elevated levels of MEK and ERK phosphorylation, suggesting that KSR1 promotes tumorigenesis in the liver by activating the RAS-RAF-MEK-ERK signaling pathway. Inhibition of KSR1 in tumors induced by activated RAS (HRASG12V) led to a significant reduction in tumorigenesis in the mouse models. Additionally, the administration of APS-2-79 to mice harboring RAF-induced HCC led to an increase in overall survival.
Conclusions
Our findings indicate that targeting KSR1 is a promising strategy for the treatment of HCC driven by activated RAS-RAF-MEK-ERK signaling.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
National Research Foundation of Korea.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
32P - Patient derived circulating tumor cell clusters for personalized chemotherapy
Presenter: Prashant Kumar
Session: Poster session 07
Resources:
Abstract
33P - Anti-tumor effect of Debio 0432, a potent and selective USP1 inhibitor, in combination with PARP inhibitors
Presenter: Noémie Luong
Session: Poster session 07
34P - A novel gene family underlying cancer cell resilience
Presenter: David Amici
Session: Poster session 07
35P - The selective WEE1 inhibitor azenosertib shows synergistic anti-tumor effects in combination with topoisomerase I inhibitor-based antibody drug conjugates
Presenter: Jianhui Ma
Session: Poster session 07
36P - Branched-chain amino acids metabolism reprogramming in trastuzumab primary resistant HER2 positive breast cancer
Presenter: Yijia Hua
Session: Poster session 07
37P - A consensus gene set facilitates enrichment analysis of cancer hallmarks
Presenter: Otília Menyhart
Session: Poster session 07
38P - Feasibility of expanding tumor-infiltrating lymphocytes from cryopreserved tumor specimens after long-term storage
Presenter: Daria Kuznetsova
Session: Poster session 07
39P - Search for rare copy number variants associated with hereditary breast cancer in Finnish case-control cohorts
Presenter: Timo Kumpula
Session: Poster session 07
40P - STOPIN: A new approach to solve the hematological toxicity of antibody-drug conjugates (ADC) with soft topoisomerase inhibitor
Presenter: Xinghai Wang
Session: Poster session 07
41P - Cancer therapy-related cardiac dysfunction (CTRCD) after radiation therapy for breast cancer: Results of the French BACCARAT study
Presenter: Manoj Kumar Francois HONARYAR
Session: Poster session 07
Resources:
Abstract