AI Article Synopsis
- Sorafenib and lenvatinib are drugs used to treat liver cancer (HCC), but this study examines how hepatitis B virus (HBV) infection impacts their effectiveness in liver cancer cells (HepG2).
- In HBV-infected HepG2 cells, there were notable changes in cell cycle gene expressions, leading to increased cell proliferation and resistance to both drugs, despite them decreasing cell viability in uninfected cells.
- The study found that while both drugs can lower certain signaling proteins in the cells, HBV infection specifically makes HepG2 cells less responsive, showing different resistance mechanisms for each drug.
Article Abstract
: Sorafenib and lenvatinib are tyrosine kinase inhibitors used in hepatocellular carcinoma (HCC) treatment. This study investigates how hepatitis B virus (HBV) infection affects their efficacy in HepG2 hepatoma cells. : HepG2 and HBV-infected HepG2/2215 cells were treated with varying concentrations of both drugs. The cell viability, cell cycle gene expression, cycle progression, and phosphorylation levels of ERK and AKT were analyzed. Results: The HBV-infected cells showed significant alterations in their cell cycle gene expressions, with an 80-fold increase in CCND2 expression and a higher proportion of cells in the G2/M phase, indicating enhanced proliferation. While both drugs decreased HepG2 cell viability in a concentration-dependent manner, HBV infection conferred resistance, as evidenced by the increased viable cells in the HepG2/2215 cultures. Sorafenib and lenvatinib decreased key cyclin and cyclin-dependent kinase expressions in uninfected cells, with less effect on the HBV-infected cells. Both drugs lowered the pERK and pAKT levels in the HepG2 cells. In the HBV-infected cells, sorafenib reduced the pERK and pAKT levels to a lesser extent. However, treatment with lenvatinib elevated the levels of pERK and pAKT. : In conclusion, HBV infection increases resistance to both sorafenib and lenvatinib in hepatoma cells by influencing the cell cycle regulatory genes and critical signaling pathways. However, the resistance mechanisms likely differ between the two medications.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11592932 | PMC |
| http://dx.doi.org/10.3390/cancers16223763 | DOI Listing |
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