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Pluronic L-81 ameliorates diabetic symptoms in db/db mice through transcriptional regulation of microsomal triglyceride transfer protein
Authors:Wo-Shing Au  Li-Wei Lu  Sidney Tam  Otis King Hung Ko  Billy KC Chow  Ming-Liang He  Samuel S Ng  Chung-Man Yeung  Ching-Chiu Liu  Hsiang-Fu Kung  Marie C Lin
Affiliation:Wo-Shing Au;Li-Wei Lu;Sidney Tam;Otis King Hung Ko;Billy KC Chow;Ming-Liang He;Samuel S Ng;Chung-Man Yeung;Ching-Chiu Liu;Hsiang-Fu Kung;Marie C Lin
Abstract:AIM: To test whether oral L-81 treatment could improve the condition of mice with diabetes and to investigate how L-81 regulates microsomal triglyceride transfer protein (MTP) activity in the liver.METHODS: Genetically diabetic (db /db ) mice were fed on chow supplemented with or without L-81 for 4 wk. The body weight, plasma glucose level, plasma lipid profile, and adipocyte volume of the db /db mice were assessed after treatment. Toxicity of L-81 was also evaluated. To understand the molecular mechanism,HepG2 cells were treated with L-81 and the effects on apolipoprotein B (apoB) secretion and mRNA level of the MTP gene were assessed. RESULTS: Treatment of db /db mice with L-81 significantly reduced and nearly normalized their body weight, hyperphagia and polydipsia. L-81 also markedly decreased the fasting plasma glucose level, improved glucose tolerance, and attenuated the elevated levels of plasma cholesterol and triglyceride. At the effective dosage, little toxicity was observed. Treatment of HepG2 cells with L-81 not only inhibited apoB secretion, but also significantly decreased the mRNA level of the MTP gene. Similar to the action of insulin, L-81 exerted its effect on the MTP promoter. CONCLUSION: L-81 represents a promising candidate in the development of a selective insulin-mimetic molecule and an anti-diabetic agent.
Keywords:Pluronic L-81  db /db mice  Animal models  diabetes  Microsomal triglyceride protein
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