PocketMatch: A new algorithm to compare binding sites in protein structures

A Argyrou; A Stark; AG Murzin; AT Laurie; B Huang; CA Orengo; F Glaser; G Dodson; G Ramachandraiah; GJ Kleywegt; HM Berman; JA Barker; JH Choi; Kalidas Yeturu; L Holm; M Jambon; Nagasuma Chandra; ND Gold; ND Gold; R Russell; R Wang; RA Laskowski; RJ Morris; S Schmitt; T Prasad; Y Kalidas

research

PocketMatch: A new algorithm to compare binding sites in protein structures

Authors: A Argyrou
A Stark
AG Murzin
AT Laurie
B Huang
CA Orengo
F Glaser
G Dodson
G Ramachandraiah
GJ Kleywegt
HM Berman
JA Barker
JH Choi
Kalidas Yeturu
L Holm
M Jambon
Nagasuma Chandra
ND Gold
ND Gold
R Russell
R Wang
RA Laskowski
RJ Morris
S Schmitt
T Prasad
Y Kalidas
Publication date: 1 January 2008
Publisher
Doi

Abstract

Background: Recognizing similarities and deriving relationships among protein molecules is a fundamental
requirement in present-day biology. Similarities can be present at various levels which can be detected through comparison of protein sequences or their structural folds. In some cases similarities obscure at these levels could be present merely in the substructures at their binding sites. Inferring functional similarities between protein molecules by comparing their binding sites is still largely exploratory and not as yet a routine protocol. One of
the main reasons for this is the limitation in the choice of appropriate analytical tools that can compare binding sites with high sensitivity. To benefit from the enormous amount of structural data that is being rapidly accumulated, it is essential to have high throughput tools that enable large scale binding site comparison.

Results: Here we present a new algorithm PocketMatch for comparison of binding sites in a frame invariant
manner. Each binding site is represented by 90 lists of sorted distances capturing shape and chemical nature of the site. The sorted arrays are then aligned using an incremental alignment method and scored to obtain PMScores for pairs of sites. A comprehensive sensitivity analysis and an extensive validation of the algorithm have been carried out. Perturbation studies where the geometry of a given site was retained but the residue types were changed randomly, indicated that chance similarities were virtually non-existent. Our analysis also demonstrates that shape information alone is insufficient to discriminate between diverse binding sites, unless
combined with chemical nature of amino acids.

Conclusions: A new algorithm has been developed to compare binding sites in accurate, efficient and
high-throughput manner. Though the representation used is conceptually simplistic, we demonstrate that along
with the new alignment strategy used, it is sufficient to enable binding comparison with high sensitivity. Novel methodology has also been presented for validating the algorithm for accuracy and sensitivity with respect to geometry and chemical nature of the site. The method is also fast and takes about 1/250th second for one comparison on a single processor. A parallel version on BlueGene has also been implemented