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Biochim Biophys Acta. 2011 May;1814(5):724-30. doi: 10.1016/j.bbapap.2011.03.009. Epub 2011 Mar 23.

Structural difference of vasoactive intestinal peptide in two distinct membrane-mimicking environments.

Author information

1
Graduate School of Medicine, Kobe University, Chuo-ku, Kobe, Hyogo, Japan.

Abstract

Vasoactive intestinal peptide (VIP) is a 28-amino acid neuropeptide which belongs to a glucagon/secretin superfamily, the ligand of class II G protein-coupled receptors. Knowledge for the conformation of VIP bound to membrane is important because the receptor activation is initiated by membrane binding of VIP. We have previously observed that VIP-G (glycine-extended VIP) is unstructured in solution, as evidenced by the limited NMR chemical shift dispersion. In this study, we determined the three-dimensional structures of VIP-G in two distinct membrane-mimicking environments. Although these are basically similar structures composed of a disordered N-terminal region and a long α-helix, micelle-bound VIP-G has a curved α-helix. The side chains of residues Phe(6), Tyr(10), Leu(13), and Met(17) found at the concave face form a hydrophobic patch in the micelle-bound state. The structural differences in two distinct membrane-mimicking environments show that the micelle-bound VIP-G localized at the water-micelle boundary with these side chains toward micelle interior. In micelle-bound PACAP-38 (one of the glucagon/secretin superfamily peptide) structure, the identical hydrophobic residues form the micelle-binding interface. This result suggests that these residues play an important role for the membrane binding of VIP and PACAP.

PMID:
21439408
DOI:
10.1016/j.bbapap.2011.03.009
[Indexed for MEDLINE]

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