Wang Chun, Kang Hui, Yi Yun, Ding Yang, Wang Fan, Luo Jie, Ye Mingliang, Hong Yinghui, Xia Chao, Yan Junwei, Liu Lan, Liu Jing, Zhong Zibiao, Zhang Zhonglin, Zhao Qiu, Chang Ying
Department of Gastroenterology, Zhongnan Hospital of Wuhan University, Wuhan, 430071, China.
Hubei Clinical Center and Key Laboratory of Intestinal and Colorectal Diseases, Wuhan, 430071, China.
J Transl Med. 2023 Dec 18;21(1):919. doi: 10.1186/s12967-023-04799-9.
Mutations in TP53 gene is considered a main driver of hepatocellular carcinoma (HCC). While TP53 mutations are the leading cause of p53 dysfunction, their occurrence rates may drop to approximately 10% in cohorts without hepatitis B virus and aflatoxin exposure. This observation suggests that the deactivation of wild-type p53 (p53) may be a critical factor in the majority of HCC cases. However, the mechanism undermining p53 activity in the liver remains unclear.
Microarray analysis and luciferase assay were utilized to confirm target associations. Gain- and/or loss-of-function methods were employed to assess alterations in signaling pathways. Protein interactions were analyzed by molecular immunological methods and further visualized by confocal microscopy. Bioinformatic analysis was performed to analyze clinical significance. Tumor xenograft nude mice were used to validate the findings in vivo.
Our study highlights the oncogenic role of Rictor, a key component of the mammalian target of rapamycin complex 2 (mTORC2), in hepatocytes. Rictor exerts its oncogenic function by binding to p53 and subsequently blocking p53 activity based on p53 status, requiring the involvement of mTOR. Moreover, we observed a dynamic nucleocytoplasmic distribution pattern of Rictor, characterized by its translocation from the nucleus (in precancerous lesions) to the cytoplasm (in HCCs) during malignant transformation. Notably, Rictor is directly targeted by the liver-enriched microRNA miR-192, and the disruption of the miR-192-Rictor-p53-miR-192 signaling axis was consistently observed in both human and rat HCC models. Clinical analysis associated lower miR-192/higher Rictor with shorter overall survival and more advanced clinical stages (P < 0.05). In mice, xenograft tumors overexpressing miR-192 exhibited lower Rictor expression levels, leading to higher p53 activity, and these tumors displayed slower growth compared to untreated HCC cells.
Rictor dynamically shuttles between the nucleus and cytoplasm during HCC development. Its pivotal oncogenic role involves binding and inhibiting p53 activity within the nucleus in early hepatocarcinogenesis. Targeting Rictor presents a promising strategy for HCC based on p53 status.
TP53基因的突变被认为是肝细胞癌(HCC)的主要驱动因素。虽然TP53突变是p53功能障碍的主要原因,但在没有乙型肝炎病毒和黄曲霉毒素暴露的队列中,其发生率可能降至约10%。这一观察结果表明,野生型p53(p53)的失活可能是大多数HCC病例的关键因素。然而,肝脏中破坏p53活性的机制仍不清楚。
利用微阵列分析和荧光素酶测定来确认靶点关联。采用功能获得和/或功能丧失方法来评估信号通路的改变。通过分子免疫学方法分析蛋白质相互作用,并通过共聚焦显微镜进一步可视化。进行生物信息学分析以分析临床意义。使用肿瘤异种移植裸鼠在体内验证研究结果。
我们的研究强调了雷帕霉素复合物2(mTORC2)的哺乳动物靶点的关键成分Rictor在肝细胞中的致癌作用。Rictor通过与p53结合发挥其致癌功能,随后根据p53状态阻断p53活性,这需要mTOR的参与。此外,我们观察到Rictor的动态核质分布模式,其特征是在恶性转化过程中从细胞核(在癌前病变中)转移到细胞质(在HCC中)。值得注意的是,Rictor是肝脏富集的微小RNA miR-192的直接靶点,并且在人类和大鼠HCC模型中均一致观察到miR-192-Rictor-p53-miR-192信号轴的破坏。临床分析表明,较低的miR-192/较高的Rictor与较短的总生存期和更晚期的临床分期相关(P<0.05)。在小鼠中,过表达miR-192的异种移植肿瘤表现出较低的Rictor表达水平,导致较高的p53活性,并且这些肿瘤与未处理的HCC细胞相比生长较慢。
Rictor在HCC发生发展过程中在细胞核和细胞质之间动态穿梭。其关键的致癌作用涉及在早期肝癌发生过程中在细胞核内结合并抑制p53活性。基于p53状态靶向Rictor为HCC提供了一种有前景的策略。
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