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The design, synthesis, and crystallization of an alpha-helical peptide

✍ Scribed by David Eisenberg; William Wilcox; Steven M. Eshita; Peter M. Pryciak; Siew Peng Ho; William F. Degrado


Book ID
105358357
Publisher
John Wiley and Sons
Year
1986
Tongue
English
Weight
740 KB
Volume
1
Category
Article
ISSN
0887-3585

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✦ Synopsis


Twelve- and sixteen-residue peptides have been designed to form tetrameric alpha-helical bundles. Both peptides are capable of folding into amphiphilic alpha-helices, with leucyl residues along one face and glutamyl and lysyl residues along the opposite face. Four such amphiphilic alpha-helices are capable of forming a noncovalently bonded tetramer. Neighboring helices run in antiparallel directions in the design, so that the complex has 222 symmetry. In the designed tetramer, the leucyl side chains interdigitate in the center in a hydrophobic interaction, and charged side chains are exposed to the solvent. The designed 12-mer (ALPHA-1) has been synthesized, and it forms helical aggregates in aqueous solution as judged by circular dichroic spectroscopy. It has also been crystallized and characterized by x-ray diffraction. The crystal symmetry is compatible with (but does not prove) the design. The design can be extended to a four-alpha-helical bundle formed from a single polypeptide by adding three peptide linkers.


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