TABLE 1.
Validation of the combination of MYC, TP53R249S, and KRASG12D for transforming PHHs into HCC.
|
Hepatocytes a OC b |
PHH1 (AKB) | PHH2 (XSM) | PHH3 (ANG) | In total d |
|---|---|---|---|---|
| MTK | 6/10 c | 4/6 | 4/6 | 14/22 |
| MT | 1/6 | 1/3 | 0/3 | 2/12 |
| TK | 0/3 | 0/3 | 0/3 | 0/9 |
| MK | 0/3 | 0/3 | 0/3 | 0/9 |
| Mock | 0/3 | 0/3 | 0/3 | 0/9 |
Hepatocytes: PHHs from three donors, including PHH1 (AKB, female, 39 years old), PHH2 (XSM, female, 59 years old), and PHH3 (ANG, male, 3 months old), were purchased from Bioreclamation IVT (Baltimore, MD, USA) and were used in the experiment.
OC: A cocktail of lentivirus containing different combinations of oncogenic candidates (M for MYC, T for TP53R249S, and K for KRASG12D) were transduced into PHHs from different donors. Mock: lentivirus containing EGFP only.
6/10: The frequency of mice that developed iHCC in the group where PHHs from different donors (PHH1~PHH3) were transduced with indicated combination of oncogenic candidates. For example, 6 out of 10 mice, in which PHHs from the donor PHH1 were transduced with MTK and were transplanted, were observed bearing tumors.
In total: ***P < 0.001 for MTK‐ versus MT/Mock‐transduced PHH by one‐way ANOVA with Tukey's multiple comparison test; data are presented as the mean ± SD.