Bahaa Elgendy scite author profile

Fatty liver, which often accompanies obesity and type 2 diabetes, frequently leads to a much more debilitating hepatic disease including non-alcoholic steatohepatitis, cirrhosis, and hepatocellular carcinoma. Current pharmacological therapies lack conclusive efficacy and thus treatment options are limited. Novel therapeutics that suppress either hepatic lipogenesis and/or hepatic inflammation may be useful. Here, we describe the development of the first selective synthetic LXR inverse agonist (SR9238) and demonstrate that this compound effectively suppresses hepatic lipogenesis, inflammation, and hepatic lipid accumulation in a mouse model of non-alcoholic hepatosteatosis. SR9238 displays high potency for both LXRα and LXRβ (40-200 nM IC50) and was designed to display liver specificity so as to avoid potential side effects due to suppression of LXR in the periphery. Unexpectedly, treatment of diet-induced obese mice with SR9238 suppressed plasma cholesterol levels. These data indicate that liver-selective LXR inverse agonists may hold utility in the treatment of liver disease.

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Tautomerism in drug discovery

Katritzky

Hall

Elgendy

et al. 2010

J Comput Aided Mol Des

143

101

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Mitochondrial pyruvate carrier inhibitors improve metabolic parameters in diet-induced obese mice

Hodges

Jarasvaraparn

Ferguson

et al. 2022

Journal of Biological Chemistry

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Bahaa Elgendy

A Liver-Selective LXR Inverse Agonist That Suppresses Hepatic Steatosis

Tautomerism in drug discovery

Mitochondrial pyruvate carrier inhibitors improve metabolic parameters in diet-induced obese mice

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