Copyright
©2005 Baishideng Publishing Group Inc.
World J Gastroenterol. Jan 7, 2005; 11(1): 7-16
Published online Jan 7, 2005. doi: 10.3748/wjg.v11.i1.7
Published online Jan 7, 2005. doi: 10.3748/wjg.v11.i1.7
Table 1 Diseases most commonly associated with PSC.
| Celiac disease |
| Rheumatoid arthritis |
| Thyroiditis |
| Sjogren’s syndrome |
| Lupus erythematosus |
| Lupic nephritis |
| Chronic pancreatitis |
| Retroperitoneal fibrosis |
| Systemic sclerosis |
| Peyronie’s disease |
| Autoimmune hemolytic anemia |
| Immune thrombocytopenic purpura |
| Membranous nephropathy |
| Histiocytosis X |
| Cystic fibrosis |
| Angioblastic lymphadenopathy |
| Intra-abdominal adenopathy |
| Vasculitis |
| Pseudotumor of the orbit |
| Gallbladder disease |
Table 2 Targets, mechanisms and effects of UDCA therapy.
| Target | Mechanisms | Effects | References |
| Cholesterol | Intestinal absorption ↓ | Biliary cholesterol decreased by 40-60% | [118] |
| Conversion to bile acids ↑ | Serum LDL and HDL cholesterol decreased | ||
| Bile acid pool | Ileal absorption of endogenous hydrophobic bile acids ↓ | Serum UDCA increased by 10-64% | |
| Total bile acids ↑ Hydrophobic bile acids ↓ | [74-77,119,120] | ||
| Unchanged hydrophilic bile acid pool | [121,122] | ||
| Bile flow | Exocytocis and canalicular transport ↑(due to ↑ cytoplasmatic free Ca2+) | ||
| Modulation of membrane transport proteins | Excretory rates and bile acids transit time ↑ | [123-125] | |
| Hypercholeresis | [80] | ||
| Gallbladder | Modulation of smooth muscle contractility (CCK receptor + cholinergic nerves) | Fasting gallbladder volume↑ | [126-128] |
| Postprandial gallbladder emptying ν | |||
| Gallbladder bile | Biliary total proteins ↓ | Crystallization-promoting activity ↓ | [129,130] |
| Concanavalin A-binding fraction ↓ | Inhibition of cholesterol crystallization | ||
| Immune system | Expression of MHC class I and II ↓ | Immunomodulatory effect T-cell hepatocellular damage ↓ | [82,83] |
| Cells | Hydrophobic bile acid induced cell damage↓ | Cytoprotection (e.g., liver damage ↓) | [85,86] |
| Apoptosis or necrosis ↓ | |||
| Neoplasms | Unknown (decreased fecal hydrophobic deoxycholate, lithocholate) | Chemo protection (neoplasm proliferation ↓) | [87,89,131] |
Table 3 Regimens and effects of UDCA for PSC therapy.
| Regimen | Assessment | Outcome | References | |
| Low doses (single administration) | 8-13 mg/(kg·d) | Liver biochemistry | Improved | [92] |
| Histology, symptoms, survival | Ineffective | |||
| 13-15 mg/(kg·d) | Liver biochemistry | Improved | [90] | |
| Histology, symptoms, survival | Ineffective | |||
| Low doses (multiple administration)1 | 10-12 mg/(kg·d) t.i.d. | Liver biochemistry | Improved | [93] |
| Histology, symptoms | No progression | |||
| 20 mg/(kg·d) | Liver biochemistry | Improved | [94] | |
| Histology | Improved | |||
| High doses | 25-30 mg/(kg·d) | ERCP | No progression | |
| Liver biochemistry | Improved | |||
| Mayo risk score and survival at 4 yr | Improved | [95] | ||
| Combination | UDCA 650 mg/d + azathioprine 1-1.5 mg/(kg·d)+ prednisolone 1-10 mg/(kg·d) | Liver biochemistry | Improved | |
| Histology | Improved | [96] | ||
| ERCP | Improved |
- Citation: Portincasa P, Vacca M, Moschetta A, Petruzzelli M, Palasciano G, van Erpecum KJ, van Berge-Henegouwen GP. Primary sclerosing cholangitis: Updates in diagnosis and therapy. World J Gastroenterol 2005; 11(1): 7-16
- URL: https://www.wjgnet.com/1007-9327/full/v11/i1/7.htm
- DOI: https://dx.doi.org/10.3748/wjg.v11.i1.7