Characterization of Tyr‐Leu‐Gly, a novel anxiolytic‐like peptide released from bovine αS‐casein

We found previously that dipeptide YL exhibits orally active anxiolytic activity comparable to diazepam. The YL sequence is often observed in the primary structure of natural food proteins. In the present study, we investigated whether YL and YL analogues are released from bovine αS‐casein by gastro...

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Bibliographic Details
Published in:The FASEB journal 2013-07, Vol.27 (7), p.2911-2917
Main Authors: Mizushige, Takafumi, Sawashi, Yurina, Yamada, Ayako, Kanamoto, Ryuhei, Ohinata, Kousaku
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Animals
Anti-Anxiety Agents - chemistry
Anti-Anxiety Agents - metabolism
Anti-Anxiety Agents - pharmacology
Benzazepines - pharmacology
Bicuculline - pharmacology
Carboxypeptidases - metabolism
Caseins - chemistry
Caseins - metabolism
Cattle
Dose-Response Relationship, Drug
gastrointestinal protease
Gastrointestinal Tract - enzymology
Male
Maze Learning - drug effects
Mice
Molecular Sequence Data
Motor Activity - drug effects
neurotransmitter
Oligopeptides - chemistry
Oligopeptides - metabolism
Pancreatic Elastase - metabolism
Pancreatin - metabolism
Pepsin A - metabolism
Peptide Hydrolases - metabolism
Piperazines - pharmacology
Receptor, Serotonin, 5-HT1A - metabolism
Receptors, Dopamine D1 - metabolism
Receptors, GABA-A - metabolism
tripeptide
Trypsin - metabolism
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Summary:We found previously that dipeptide YL exhibits orally active anxiolytic activity comparable to diazepam. The YL sequence is often observed in the primary structure of natural food proteins. In the present study, we investigated whether YL and YL analogues are released from bovine αS‐casein by gastrointestinal proteases. YLG, corresponding to αS1‐casein (aa 91–93), was more effectively released from αS‐casein than YL by pepsin‐pancreatin digestion, mimicking gastrointestinal enzymatic conditions. Using the synthetic model peptide, we determined that trypsin cleaved the N terminus of YLG, and elastase and carboxypeptidase contributed to cleave the C‐terminus. YLG exhibited orally active anxiolytic‐like activity in the elevated plus maze and open‐field tests in mice. The anxiolytic‐like activity of YLG was inhibited by WAY100135, SCH23390 or bicuculline, antagonists of serotonin 5‐HT1A, dopamine D1, and GABAA receptors, respectively; however, YLG had no affinity for these receptors. The pepsin‐pancreatin digest of αS‐Casein also exhibited anxiolytic‐like activity. Meanwhile, anxiolytic‐like activity of α‐casozepine, an αS1‐casein‐derived decapeptide with YL sequence in the N terminus, was blocked by WAY100135, SCH23390, or bicuculline, equally to YLG and YL; however, it was not detected in the pepsin‐pancreatic digest. Taken together, we found that YLG is released after pepsin‐pancreatic digestion of αS‐casein and exhibits potent anxiolytic‐like activity via activation of serotonin, dopamine, and the GABA receptor system.—Mizushige, T., Sawashi, Y., Yamada, A., Kanamoto, R., Ohinata, K. Characterization of Tyr‐Leu‐Gly, a novel anxiolytic‐like peptide released from bovine αS‐casein. FASEB J. 27, 2911‐2917 (2013). www.fasebj.org
ISSN:0892-6638
1530-6860
DOI:10.1096/fj.12-225474