| Literature DB >> 28460928 |
Juliette Caron1, Benoit Cudennec2, Dorothée Domenger1, Yanath Belguesmia1, Christophe Flahaut1, Mostafa Kouach3, Jean Lesage4, Jean-François Goossens3, Pascal Dhulster1, Rozenn Ravallec1.
Abstract
Dietary proteins have been reported to induce a strong feeling of satiety that has been partially explained by gut hormone level increase. Up to date, various protein hydrolysates have demonstrated in vitro and in vivo their potential to stimulate gut hormone secretion related to food intake decrease and their mechanisms of action have just started to be resolved. In this context, this study aimed at identifying new peptide sequences involved in gut hormone secretion released by protein in vitro gastrointestinal digestion. Targeted gut hormones were Cholecystokinin (CCK) and Glucagon-Like Peptide 1 (GLP-1). The activity of DPP-IV was also considered as it strongly modulates GLP-1 action. In a previous study, simulated digestion of dietary protein has generated hydrolysates with enhancing effect on CCK and GLP-1 secretion in STC-1 cells as well as DPP-IV inhibitory properties. Successive purification steps were performed to isolate peptide fractions involved in these bioactivities whose sequence was determined by LC-MS-MS. Three peptide sequences ANVST, TKAVEH and KAAVT were pointed out for their stimulating effects on GLP-1 secretion. The sequence VAAA was isolated for its DPP-IV inhibitory properties. Two peptide groups were strongly involved in CCK release sharing a certain occurrence of aromatic amino acid residues.Entities:
Keywords: Bioactive peptides; DPP-IV; Enteroendocrine cells; Gut hormones; Protein digestion
Year: 2016 PMID: 28460928 DOI: 10.1016/j.foodres.2016.08.033
Source DB: PubMed Journal: Food Res Int ISSN: 0963-9969 Impact factor: 6.475