| Literature DB >> 7749917 |
Q X Hua1, S N Gozani, R E Chance, J A Hoffmann, B H Frank, M A Weiss.
Abstract
We have determined the structure of a metastable disulphide isomer of human insulin. Although not observed for proinsulin folding or insulin-chain recombination, the isomer retains ordered secondary structure and a compact hydrophobic core. Comparison with native insulin reveals a global rearrangement in the orientation of A- and B-chains. One face of the protein's surface is nevertheless in common between native and non-native structures. This face contains receptor-binding determinants, rationalizing the partial biological activity of the isomer. Structures of native and non-native disulphide isomers also define alternative three-dimensional templates. Threading of insulin-like sequences provide an experimental realization of the inverse protein-folding problem.Entities:
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Year: 1995 PMID: 7749917 DOI: 10.1038/nsb0295-129
Source DB: PubMed Journal: Nat Struct Biol ISSN: 1072-8368