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Molecular Pharmacology, Vol 19, 302-306, Copyright © 1981 by the American Society for Pharmacology and Experimental Therapeutics
-Endorphin Analogues in Cerebroside Sulfate
Solution
1 Cardiovascular Research Institute and Langley Porter Psychiatric Institute, University of California, San Francisco,
California 94143, The Salk Institute, San Diego, California 92138, and Peninsula Laboratory, Belmont, California 94002
The conformation of synthetic 
-endorphin fragments in cerebroside sulfate solutions was
studied by circular dichroism. The lipid was solubilized by the inert nonionic surfactant
cetylpoly(oxyethylene) ether to facilitate optical measurements. All peptides show an
aperiodic conformation in water. Addition of cerebroside sulfate induces a partial helical
structure for human peptides, h-endorphin(14-31), (17-31), and (1-5)-(16-31), and
porcine peptides, p-endorphin(1-25) and (6-31), but 
-endorphin, 
-endorphin, and h-endorphin(1-19), (6-17), (22-31), and (26-31) remain unordered in the lipid solution.
Thus, the helical segment in , -endorphin is deduced to be in the middle region of the
parent molecule, probably involving two to three helical turns of approximately eight to
nine amino acid residues between residues 13 and 24. This helical segment may bring the
active sites of the otherwise flexible polypeptide to a correct geometry in the lipid
environment in order to express its biological activity.
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