Structure-function analysis of a phage display-derived peptide that binds to insulin-like growth factor binding protein 1

被引:36
|
作者
Skelton, NJ
Chen, YM
Dubree, N
Quan, C
Jackson, DY
Cochran, A
Zobel, K
Deshayes, K
Baca, M
Pisabarro, MT
Lowman, HB
机构
[1] Genentech Inc, Dept Prot Engn, S San Francisco, CA 94080 USA
[2] Genentech Inc, Dept Bioorgan Chem, S San Francisco, CA 94080 USA
关键词
D O I
10.1021/bi0103866
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Highly structured, peptide antagonists of the interaction between insulin-like growth factor 1 (IGF-I) and IGF binding protein 1 (IGFBP-1) have recently been discovered by phage display of naive peptide libraries [Lowman, H. B., et al. (1998) Biochemistry 37, 8870-8878]. We now report a detailed analysis of the features of this turn-helix peptide motif that are necessary for IGFBP-1 binding and structural integrity. Further rounds of phage randomization indicate the importance of residues contributing to a hydrophobic patch on one face of the helix. Alanine-scanning substitutions confirm that the hydrophobic residues are necessary for binding. However, structural analysis by NMR spectroscopy indicates that some of these analogues are less well folded. Structured, high-affinity analogues that lack the disulfide bond were prepared by introducing a covalent constraint between side chains at positions i and i + 7 or i + 8 within the helix. Analogues based on this scaffold demonstrate that a helical conformation is present in the bound state, and that hydrophobic side chains in this helix, and residues immediately preceding it, interact with IGFBP-1. By comparison of alanine scanning data for IGF-I and the turn-helix peptide, we propose a model for common surface features of these molecules that recognize IGFBP-1.
引用
收藏
页码:8487 / 8498
页数:12
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