AI Article Synopsis
- The study used comparative molecular field analysis (CoMFA) to analyze the relationship between the structure of SH2-binding phosphopeptides and their biological activity.
- Two alignment methods were tested, with alignment II showing better correlation (r² = 0.961) and predictivity (cross-validated r² = 0.682) by focusing on the binding positions in SH2 complexes.
- The findings indicated that modifying the size and charge of phosphopeptides, informed by CoMFA contour maps, could enhance their binding affinities.
Article Abstract
A comparative molecular field analysis (CoMFA) was carried out to investigate quantitative structure-activity relationships for SH2-binding phosphopeptides. Two alignment rules were applied in our CoMFA model. The phosphopeptide backbone atoms were used for superposition in alignment I and the backbone atoms of peptide-binding residues of SH2-phosphopeptide complexes were used in alignment II to consider the position of phosphopeptides in SH2-binding sites. The higher correlation and predictivity in alignment II (r(2) value of 0.961 and cross-validated r(2) value of 0.682) suggest that the consideration of peptide-binding position at the binding sites gives rise to better results when the ligand-receptor complex structure is considered. In addition, CoMFA contour and electrostatic maps were well accorded with the experimental results in which the replacement of N-terminal residues with an acetyl group reduced the binding affinity. Therefore, the modification of molecular size and charge of phosphopeptides can be carried out based on these contour maps in order to increase binding affinities.
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| http://dx.doi.org/10.1016/s0006-291x(03)00932-x | DOI Listing |
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