Litcius/Paper detail

Cathepsin-facilitated invasion of BMI1-high hepatocellular carcinoma cells drives bile duct tumor thrombi formation

Lei‐Bo Xu, Yufei Qin, Liangping Su, Cheng Huang, Qiuping Xu, Rui Zhang, Xiang-de Shi, Ruipu Sun, Jiali Chen, Zhixiao Song, Xue Jiang, Lihuan Shang, Gang Xiao, Xiangzhan Kong, Chao Liu, Ping‐Pui Wong

2023Nature Communications20 citationsDOIOpen Access PDF

Abstract

Abstract Bile duct tumor thrombosis (BDTT) is a complication mostly observed in patients with advanced hepatocellular carcinoma (HCC), causing jaundice and associated with poor clinical outcome. However, its underlying molecular mechanism is unclear. Here, we develop spontaneous preclinical HCC animal models with BDTT to identify the role of BMI1 expressing tumor initiating cells (BMI1 high TICs) in inducing BDTT. BMI1 overexpression transforms liver progenitor cells into BMI1 high TICs, which possess strong tumorigenicity and increased trans-intrahepatic biliary epithelial migration ability by secreting lysosomal cathepsin B (CTSB). Orthotopic liver implantation of BMI1 high TICs into mice generates tumors and triggers CTSB mediated bile duct invasion to form tumor thrombus, while CTSB inhibitor treatment prohibits BDTT and extends mouse survival. Clinically, the elevated serum CTSB level determines BDTT incidence in HCC patients. Mechanistically, BMI1 epigenetically up-regulates CTSB secretion in TICs by repressing miR-218-1-3p expression. These findings identify a potential diagnostic and therapeutic target for HCC patients with BDTT.

Topics & Concepts

BMI1Hepatocellular carcinomaCathepsin BBile ductCancer researchMedicineCommon bile ductPathologyInternal medicineBiologyCancerEnzymeBiochemistryCholangiocarcinoma and Gallbladder Cancer StudiesMicroRNA in disease regulationCancer-related molecular mechanisms research