Journal
JOURNAL OF DAIRY SCIENCE
Volume 100, Issue 5, Pages 3360-3372Publisher
ELSEVIER SCIENCE INC
DOI: 10.3168/jds.2016-12067
Keywords
bioactive milk peptide; beta-casein; beta-CN (94-123); intestinal protection
Funding
- Ingredia (Arras, France)
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beta-Casofensin is a bioactive milk peptide that modulates the intestinal barrier, particularly through its action on goblet cells. beta-Casofensin corresponds to fragment (f) 94-123 of the bovine beta-casein (beta-CN) A2 variant. Fifteen genetic variants of bovine beta-CN (A1-3, B-G, H1-2, I-L) are known, of which the A2, A1, and B forms are the most common. These variants differ from each other by the substitution of one or more amino acids, some of which are localized in f94 to 123. The aim of our study was to compare the intestinal effects of beta-casofensin A2 and its 3 main variants: A1. A3, and B. For this purpose, a solution (0.1 mu M; 10 mu L/g of body weight, postnatal d 10-20) containing beta-casofensin A2, one of its variants (A1, A3, or B), or drinking water (control; CT) was administered to rat pups orally. After euthanasia (postnatal d 20), intestinal segments were collected for biochemical and histochemical analysis and also used to determine paracellular permeability to fluorescein isothiocyanate-labeled 4-kDa dextrin in an Ussing chamber. We also studied the direct effects of beta-casofensin A2 and its A1 variant on the paracellular permeability of jejunum segments of adult rats. beta-Casofensin A2 and its B variant significantly increased the population of goblet cells compared with the CT, A1, and A3 groups. The mucin 2 mRNA level was significantly higher in the beta-casofensin A2 group than in the CT, A3, and B groups. Our results also revealed that the protein expression of zonula occludens-1 and occludin was reduced in the jejunum of rats in the A1, A3, and B groups compared with the CT group. However, the A1 variant was the only peptide to decrease jejunal permeability compared with the CT group. This variant, tested directly in the apical compartment of an Ussing chamber at a concentration of 0.1 nM, also reduced jejunal permeability. In conclusion, the substitution of a single amino acid alters the effect of beta-CN sequence f94 to 123 on goblet cells and on intestinal permeability. A. genetic polymorphism of beta-CN can affect the biological activity of peptides derived from this protein. These data should be taken into account in the production of bioactive foods.
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