Faraj_2004_J.Lipid.Res_45_657

Reference

Title : ASP enhances in situ lipoprotein lipase activity by increasing fatty acid trapping in adipocytes - Faraj_2004_J.Lipid.Res_45_657
Author(s) : Faraj M , Sniderman AD , Cianflone K
Ref : J Lipid Res , 45 :657 , 2004
Abstract :

Acylation-stimulating protein (ASP) increases triglyceride (TG) storage (fatty acid trapping) in adipose tissue and plays an important role in postprandial TG clearance. We examined the capacity of ASP and insulin to stimulate the activity of lipoprotein lipase (LPL) and the trapping of LPL-derived nonesterified fatty acid (NEFA) in 3T3-L1 adipocytes. Although insulin increased total LPL activity (secreted and cell-associated; P < 0.001) in 3T3-L1 adipocytes, ASP moderately stimulated secreted LPL activity (P = 0.04; 5% of total LPL activity). Neither hormone increased LPL translocation from adipocytes to endothelial cells in a coculture system. However, ASP and insulin increased the V(max) of in situ LPL activity ([(3)H]TG synthetic lipoprotein hydrolysis and [(3)H]NEFA incorporation into adipocytes) by 60% and 41%, respectively (P

PubMedSearch : Faraj_2004_J.Lipid.Res_45_657
PubMedID: 14703506

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Citations formats

Faraj M, Sniderman AD, Cianflone K (2004)
ASP enhances in situ lipoprotein lipase activity by increasing fatty acid trapping in adipocytes
J Lipid Res 45 :657

Faraj M, Sniderman AD, Cianflone K (2004)
J Lipid Res 45 :657