Zhang_2024_Food.Chem_460_140708

Reference

Title : Residue profiles of peptides with cholesterol esterase and pancreatic lipase inhibitory activities through virtual screening and sequence analysis - Zhang_2024_Food.Chem_460_140708
Author(s) : Zhang Z , Jiang S , Li Y , Xie D , Li JX
Ref : Food Chem , 460 :140708 , 2024
Abstract :

The detailed characterization of the structural features of peptides targeting cholesterol esterase (CEase) or pancreatic lipase (PPL) will benefit the management of hyperlipidemia and obesity. This study employed the Glide SP (standard precision)-peptide method to predict the binding modes of 20(2) dipeptides and 20(3) tripeptides to these targets, correlating residue composition and position with binding energy. Strong preferences for Trp, Phe, and Tyr were observed at all positions of potential inhibitory peptides, whereas negatively charged residues Glu and Asp were disfavored. Notably, Arg and aromatic rings significantly influenced the peptide conformation at the active site. Tripeptide IWR demonstrated the high efficacy, with IC(50) values of 0.214 mg/mL for CEase and 0.230 mg/mL for PPL. Five novel IWR scaffold-tetrapeptides exhibited promising inhibitory activity. Non-covalent interactions and energy contributions dominated the formation of stable complexes. Our results provide insights for the development of new sequences or peptide-like molecules with enhanced inhibitory activity.

PubMedSearch : Zhang_2024_Food.Chem_460_140708
PubMedID: 39096803

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Citations formats

Zhang Z, Jiang S, Li Y, Xie D, Li JX (2024)
Residue profiles of peptides with cholesterol esterase and pancreatic lipase inhibitory activities through virtual screening and sequence analysis
Food Chem 460 :140708

Zhang Z, Jiang S, Li Y, Xie D, Li JX (2024)
Food Chem 460 :140708