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  • Systemic LSD1 Inhibition Prevents Aberrant Remodeling of Metabolism in Obesity.

Systemic LSD1 Inhibition Prevents Aberrant Remodeling of Metabolism in Obesity.

Diabetes (2022-09-27)
Bastian Ramms, Dennis P Pollow, Han Zhu, Chelsea Nora, Austin R Harrington, Ibrahim Omar, Philip L S M Gordts, Matthew Wortham, Maike Sander
ABSTRACT

The transition from lean to obese states involves systemic metabolic remodeling that impacts insulin sensitivity, lipid partitioning, inflammation, and glycemic control. Here, we have taken a pharmacological approach to test the role of a nutrient-regulated chromatin modifier, lysine-specific demethylase (LSD1), in obesity-associated metabolic reprogramming. We show that systemic administration of an LSD1 inhibitor (GSK-LSD1) reduces food intake and body weight, ameliorates nonalcoholic fatty liver disease (NAFLD), and improves insulin sensitivity and glycemic control in mouse models of obesity. GSK-LSD1 has little effect on systemic metabolism of lean mice, suggesting that LSD1 has a context-dependent role in promoting maladaptive changes in obesity. In analysis of insulin target tissues we identified white adipose tissue as the major site of insulin sensitization by GSK-LSD1, where it reduces adipocyte inflammation and lipolysis. We demonstrate that GSK-LSD1 reverses NAFLD in a non-hepatocyte-autonomous manner, suggesting an indirect mechanism potentially via inhibition of adipocyte lipolysis and subsequent effects on lipid partitioning. Pair-feeding experiments further revealed that effects of GSK-LSD1 on hyperglycemia and NAFLD are not a consequence of reduced food intake and weight loss. These findings suggest that targeting LSD1 could be a strategy for treatment of obesity and its associated complications including type 2 diabetes and NAFLD.

MATERIALS
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Brand
Product Description

Sigma-Aldrich
GSK-LSD1, ≥98% (HPLC)