Features and properties of maralixibat
| Alternative names | Maralixibat chloride; Livmarli™; CAN 108; lopixibat; lopixibat chloride; LUM-001; SD-5613; SHP 625 |
| Classes | Amines; anti-inflammatories; antihyperlipidaemics; azabicyclo compounds; benzothiepins; dioxoles; hepatoprotectants; onium compounds; small molecules |
| Mechanism of action | Sodium-bile acid cotransporter inhibition |
| Route of administration | Oral |
| Pharmacodynamics | Inhibits the ileal bile acid transporter, resulting in decreased reabsorption of bile acids from the terminal ileum and reductions in serum bile acid levels; may reduce absorption of fat-soluble vitamins |
| Pharmacokinetics | Minimal absorption; approximately dose-proportional exposure; 91% bound to human plasma proteins in vitro; limited metabolism; mean half-life of 1.6 h; excretion is predominantly (73%) through the faecal route, mostly as unchanged maralixibat |
| Most common adverse events | Diarrhoea, abdominal pain, vomiting, fat-soluble vitamin deficiency, transaminases increased, gastrointestinal bleeding |
| ATC codes | |
| WHO ATC code | A05A-X04 (maralixibat chloride) |
| EphMRA ATC code | A5A (Bile Therapy and Cholagogues) |
| Chemical name | 1-{[4-({4-[(4R,5R)-3,3-dibutyl-7-(dimethylamino)-4-hydroxy-1,1-dioxo-2,3,4,5-tetrahydro-1H-1λ6-benzothiepin-5-yl]phenoxy}methyl)phenyl]methyl}-1,4-diazabicyclo[2.2.2]octan-1-ium chloride |