1. Stimulation of B7-H1 in Hepatocarcinoma Cells by Hepatitis B virus X Antigen.
- Author
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Wu, Shengxi, Yang, Chengying, Guo, Sheng, Fei, Lei, Luo, Na, Fu, Xiaolan, Chen, Yongwen, and Wu, Yuzhang
- Subjects
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HEPATITIS B virus , *TRANSCRIPTION factors , *T cells , *APOPTOSIS , *MESSENGER RNA , *FLOW cytometry , *MUTAGENESIS , *ANTIGENS - Abstract
The cross-talk between the hepatitis B virus X protein (HBx) and B7-H1 in hepatocarcinoma (HCC) is unclear. This study analyzed the potential relationships between HBx and B7-H1 in hepatocarcinogenesis. One of human HCC cell lines, HepG2 cells, was transfected to stably express HBx protein (HBx+-HepG2). The transcription of B7-H1 mRNA was increased significantly in these cells compared to cells transfected with control vector (HBx--HepG2), as confirmed by a comparative genome-wide microarray analysis (Capitalbio) and real time quantitative PCR (qPCR). Flow cytometry and western-blot further demonstrated that B7-H1 protein synthesis was enhanced in HBx+-HepG2 cells. Site-directed mutagenesis of promoter constructs revealed that the transcription factor (NF)-κB binding site between 128 and 137 bp upstream of B7-H1 gene transcriptional start site is primarily responsible for HBx-mediated B7-H1 expression. Co-culture experiments with HBx+-HepG2/T cells showed that the number of apoptotic T cells increased profoundly, and this effect could be partially prevented when a neutralizing mAb against B7-H1 was added to the culture, demonstrating that B7-H1 signaling can promote T cell apoptosis. Our results suggest that the expression of B7-H1 in hepatocarcimona cells can be initiated by HBx antigen, thus inducing T cell apoptosis and finally potentially facilitates the genesis of HCC. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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