There is no approved therapy for NASH Weight reduction is typica

There is no approved therapy for NASH. Weight reduction is typically recommended, but the efficacy of weight reduction for the treatment of NASH AZD3965 supplier has not been carefully evaluated. We examined the relation of weight change and steatohepatitis by laboratory findings and unenhanced

CT. Methods: We enrolled the 85 patients that diagnosed for NASH clinically. NASH was established by the presence of hepatic ultrasonographic findings and elevated aminotrasnferase level (>40). Previous diagnosis of hepatic disease, serum creatinine level >1.5 mg/dl, other medical illness, pregnancy, use of drug (weight loss drug, diabetes medication), alcohol consumption >30 g per day were excluded. We measured the BMI (height and weight), Sirolimus AST/ALT, r-GTP, albumin, bilirubin and cholesterol level at 0 and 10 weeks. Each participant underwent two consecutive unenhanced CT for assessing the liver and visceral fat content at 0 and 10 weeks. Results: Seventy-five percent patients have decreased the body weight. The mean weight change over 10-week period was 2.3 kg. Percent weight reduction from baseline correlated significantly with improved liver chemistry (p = 0.008), improvements in the degree of hepatic steatosis by housfiled

unit (p < 0.001), and decreased visceral fat ratio (p < 0.001). Conclusion: Weight reduction leads to decreased the aminotrasferase levels, visceral fat ratio and improved the steatohepatitis in NASH. Key Word(s): 1. steatohepatitis; 2. weight reduction; Presenting Author: HU CHANGJIANG Additional Authors: HE SHI-MING Corresponding Author: HU CHANGJIANG, HE SHI-MING Affiliations: Department of Gastroenterology, XinQiao Hospital; Department of Biochemistry and Molecular Biology, College of Basic Medical Sciences Objective: Liver X receptors (LXRs), including LXRα and LXRβ isoforms, play important roles in the metabolic regulation of glucose, cholesterol and lipid. Moreover, activation of LXRs also represses the expression of Cyclin D1 and B1, and thus suppresses the proliferation of multiple cancer cells, but the relevant mechanism is not

well known. Forkhead Box M1 (FOXM1) selleck inhibitor is a proliferation-specific member of forkhead box family, which is highly expressed in proliferating normal cells and numerous cancer cells. FOXM1 directly activates transcription of Cyclin D1 and B1, resulting in the enhancement of cell cycle progression and cell proliferation. However, it is unclear whether LXRs are involved in the regulation of FOXM1. In the present study, we demonstrated that specific LXRs agonists downregulated expressions of FOXM1, Cyclin D1 and B1 in hepatocellular carcinoma (HCC) cells, which led to cell cycle and cell proliferation arrest. Methods: We used knockdown of FOXM1, Reporter assays, electrophoretic mobility shift assay (EMSA) and chromatin immunoprecipitation (ChIP) assays. FOXM1 expression in liver tissues was also inhibited in the mice fed with LXRs agonists.

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