Table 6.
Pharmacokinetic variabilities of NASH group compared with control group and judgment of related influencing factors.
| Drugs | PK changes (ig) |
PK changes (iv) |
Cyp450s changes |
AUCmetabolite/AUCparent drug |
Gut microbiota |
Main influencing factors | ||||
|---|---|---|---|---|---|---|---|---|---|---|
| Parent drug | Metabolite | Parent drug | Metabolite | Activity | Expression | ig | iv | Biotransformation | Host/gut microbiota | |
| Omeprazole | AUC↑, CLz/F↓ |
AUC↓, Cmax ↓, t1/2↓ | AUC(0-12h)↑ | − | Cyp2c29↓ | Cyp2c29↓ | ↓ | ↓ | Yes | gut microbiota |
| Phenacetin | AUC↑, Cmax ↑,CLz/F↓ | AUC↑, t1/2 ↓, CLz/F↓ | − | AUC(0-12h)↑ | Cyp1a2↓ | Cyp1a2↓ | − | − | Yes | gut microbiota |
| Midazolam | AUC↑, Cmax ↑,CLz/F↓ | AUC↑, Cmax ↑, Tmax ↑, t1/2↑, CLz/F↓ |
− | AUC↑, Cmax ↑,CLz/F↓ | Cyp3a11↓ | Cyp3a11↓ | − | − | Yes | gut microbiota |
| Chlorzoxazone | AUC↑, Cmax ↑,CLz/F↓ | − | − | − | Cyp2e1− | Cyp2e1↓ | − | − | Yes | gut microbiota |
| Tolbutamide | AUC↑, Cmax ↑, Tmax ↑ t1/2↑, CLz/F↓ |
AUC↑, Cmax ↑, Tmax ↑, t1/2↑ | AUC↑, t1/2↑,CLz/F↓ | AUC↑, Cmax ↑, Tmax ↑,CLz/F↓ | Cyp2c65↓ | Cyp2c65↓ | ↓ | ↓ | No | host |
| Metoprolol | − | − | − | − | Cyp2d22− | Cyp2d22− | − | − | No | Neither |
Note: The results in the table are from the NASH group vs. the control group in mice. −: not significant. ↑: significantly increased. ↓: significantly decreased. ig: intragastric administration. iv: intravenous administration. Based on the results of Cyp450 enzymes in vitro as the standard, combined with the results of Cyp450 enzymes in vivo, their relationships can be roughly divided into three categories: 1) if the results were consistent, the pharmacokinetic variabilities were mainly related to the host alteration; 2) if the results were inconsistent, the pharmacokinetic variabilities were mainly related to the gut microbiota; and 3) if the results did not change, the pharmacokinetics were less affected by both factors.