基因敲除
染色体易位
肿瘤微环境
细胞质
细胞生物学
核糖核酸
糖酵解
癌症研究
化学
亚细胞定位
肝细胞癌
细胞
生物
肿瘤细胞
基因
生物化学
新陈代谢
作者
Han-Yuan Liu,Xiao Li,Chenwei Zhang,Xiaopei Hao,Yongfang Cao,Yuliang Wang,Hao Zhuang,Na Yu,Tian Huang,Chuan Liu,Hengsong Cao,Zhengqing Lu,Jinhua Song,Li Liu,Hanjin Wang,Zhouxiao Li,Weiwei Tang
标识
DOI:10.1002/advs.202402115
摘要
Despite substantial breakthroughs in the treatment of hepatocellular carcinoma (HCC) in recent years, many patients are diagnosed in the middle or late stages, denying them the option for surgical excision. Therefore, it is of great importance to find effective therapeutic targets of HCC. In this study, it is found that Gap junction protein beta-2 (GJB2) is highly enriched in malignant cells based on single-cell RNA sequencing and higher expression of GJB2 indicates a worse prognosis. The localization of GJB2 in HCC cancer cells is changed compared with normal liver tissue. In cancer cells, GJB2 tends to be located in the cytoplasm and nucleus, while in normal tissues, GJB2 is mainly located on the cell membrane. GJB2 is related to glycolysis, promoting NF-κB pathway via inducing the ubiquitination degradation of IκBa, and activating HIF-1α/GLUT-1/PD-L1 pathway. In addition, GJB2 knockdown reshapes tumor immune microenvironment and Salvianolic acid B inhibits the activity of GJB2. In conclusion, GJB2 promotes HCC progression by activating glycolysis through cytoplasmic translocation and generating a suppressive tumor microenvironment. Salvianolic acid B inhibits the expression of GJB2 and enhances the sensitivity of anti-PD1 therapy, which may provide insights into the development of novel combination therapeutic strategies for HCC.
科研通智能强力驱动
Strongly Powered by AbleSci AI