Abstract:The effects of ursodeoxycholic acid (UDCA, 450 mg daily) in patients with histologically proven chronic active hepatitis (CAH) have been evaluated in a randomized, double-blind, placebo-controlled study. Twenty-six patients with serum alanine aminotransferase (ALT) values at least twice the normal upper limit in two of three pre-treatment tests received UDCA or a placebo for twelve weeks. In all UDCA-treated patients, serum aspartate amino-transferase (AST), ALT, gamma-glutamyl transpeptidase (GGT) and alkalin… Show more
“…However, the efficacy of UDCA for attenuating hepatobiliary damages seemed beyond doubt, and several studies have demonstrated the efficacy of UDCA in this respect. 24,25 There was no statistically significant difference in the ratio of reduction in ALP levels between the group that received prior treatment with UDCA and that which did not ( Table 2). The main mechanism by which UDCA lowers serum biliary enzyme levels is thought to be the replacement of toxic bile salts with nontoxic hydrophobic ones, which differs from the mechanism of bezafibrate, as mentioned earlier.…”
Bezafibrate significantly reduced the level of biliary enzymes in various chronic liver diseases and may be useful for the treatment of certain liver disease subsets.
“…However, the efficacy of UDCA for attenuating hepatobiliary damages seemed beyond doubt, and several studies have demonstrated the efficacy of UDCA in this respect. 24,25 There was no statistically significant difference in the ratio of reduction in ALP levels between the group that received prior treatment with UDCA and that which did not ( Table 2). The main mechanism by which UDCA lowers serum biliary enzyme levels is thought to be the replacement of toxic bile salts with nontoxic hydrophobic ones, which differs from the mechanism of bezafibrate, as mentioned earlier.…”
Bezafibrate significantly reduced the level of biliary enzymes in various chronic liver diseases and may be useful for the treatment of certain liver disease subsets.
“…[7][8][9] In primary biliary cirrhosis, an improved survival rate and liver morphology have been shown. 8,10 In CF, UDCA has been shown to improve LFT and to ameliorate the hepatic wash-out of isotope at hepatobiliary scintigraphy.…”
“…It reduces the effect of hydrophobic bile acids on the hepatocytes through its choleritic and antiâapoptotic effects (12). In addition, it decreases hepatitis C virusârelated hepatic injury by modifying the expression of HLAâClass I and reinforces the natural antiviral mechanisms such as natural killer cells, 2âł, 5âł oligo adenylate synthetase activity thus degrading viral mRNA (13, 14). UDCA was shown to achieve normalization of serum transaminases twice as much as amantadine hydrochloride or silymarin (15).…”
Twenty-four weeks N-IFN-BT achieved a fourfold-higher ETBR and a tenfold-higher SBR compared with silymarin therapy, which reflects an improvement of necroinflammatory activity as proven by repeat histopathology.
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