Characterization of beta-lactotensin, a bioactive peptide derived from bovine beta-lactoglobulin, as a neurotensin agonist.

Biosci Biotechnol Biochem

Division of Food Science and Biotechnology, Graduate School of Agriculture, Kyoto University, Uji, Kyoto 611-0011, Japan.

Published: April 2003

AI Article Synopsis

  • beta-Lactotensin (beta-LT) is an ileum-contracting peptide from bovine beta-lactoglobulin, which selectively acts on the NT2 receptor while neurotensin selectively targets the NT1 receptor.
  • Beta-LT causes an increase in blood pressure (hypertension) in rats, contrasting with neurotensin's effect of lowering blood pressure (hypotension).
  • The hypertensive effects of beta-LT were confirmed to involve the NT2 receptor, while the NT1 and NT2 receptors have opposing effects on blood pressure regulation.

Article Abstract

beta-Lactotensin (beta-LT: His-Ile-Arg-Leu) is an ileum-contracting peptide derived from residues No. 146-149 of bovine beta-lactoglobulin. The ileum-contracting activity of beta-LT was blocked by the NT1 antagonist SR48692. beta-LT was selective for the neurotensin NT2 receptor while neurotensin was selective for the NT1 receptor. beta-LT is the first natural ligand showing selectivity for the NT2 receptor. beta-LT showed hypertensive activity after intravenous administration at a dose of 30 mg/kg in conscious rats, while neurotensin showed hypotensive activity. The hypertensive activity of beta-LT was blocked by levocabastine (1 mg/kg, i.v.), an NT2 antagonist. SR48692, which blocked the hypotensive activity of neurotensin, had no effect on the hypertensive activity of beta-LT. These results suggest that the hypertensive activity of beta-LT is mediated by the NT2 receptor. It was concluded that the NT1 and NT2 receptors mediate the opposite effect on blood pressure.

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Source
http://dx.doi.org/10.1271/bbb.67.940DOI Listing

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