PCI-SS: MISO dynamic nonlinear protein secondary structure prediction

A Zemla; AA Schaffer; B Alberts; B Rost; B Rost; B Rost; BW Matthews; D Przybylski; DT Jones; G Pollastri; H Berman; JA Cuff; James R Green; JJ Ward; JR Green; JR Green; JR Green; JR Green; K Lin; LJ McGuffin; M Korenberg; M Ouali; M Shah; Michael J Korenberg; MJ Korenberg; MJ Korenberg; MJ Korenberg; MJ Korenberg; Mohammed O Aboul-Magd; R Adamczak; R David; RE Dorsey; S Montgomerie; VA Eyrich; W Kabsch

PCI-SS: MISO dynamic nonlinear protein secondary structure prediction

Authors: A Zemla
AA Schaffer
B Alberts
B Rost
B Rost
B Rost
BW Matthews
D Przybylski
DT Jones
G Pollastri
H Berman
JA Cuff
James R Green
JJ Ward
JR Green
JR Green
JR Green
JR Green
K Lin
LJ McGuffin
M Korenberg
M Ouali
M Shah
Michael J Korenberg
MJ Korenberg
MJ Korenberg
MJ Korenberg
MJ Korenberg
Mohammed O Aboul-Magd
R Adamczak
R David
RE Dorsey
S Montgomerie
VA Eyrich
W Kabsch
Publication date: 1 January 2009
Publisher: BioMed Central
Doi

Abstract

Abstract Background Since the function of a protein is largely dictated by its three dimensional configuration, determining a protein's structure is of fundamental importance to biology. Here we report on a novel approach to determining the one dimensional secondary structure of proteins (distinguishing α-helices, β-strands, and non-regular structures) from primary sequence data which makes use of Parallel Cascade Identification (PCI), a powerful technique from the field of nonlinear system identification. Results Using PSI-BLAST divergent evolutionary profiles as input data, dynamic nonlinear systems are built through a black-box approach to model the process of protein folding. Genetic algorithms (GAs) are applied in order to optimize the architectural parameters of the PCI models. The three-state prediction problem is broken down into a combination of three binary sub-problems and protein structure classifiers are built using 2 layers of PCI classifiers. Careful construction of the optimization, training, and test datasets ensures that no homology exists between any training and testing data. A detailed comparison between PCI and 9 contemporary methods is provided over a set of 125 new protein chains guaranteed to be dissimilar to all training data. Unlike other secondary structure prediction methods, here a web service is developed to provide both human- and machine-readable interfaces to PCI-based protein secondary structure prediction. This server, called PCI-SS, is available at <url>http://bioinf.sce.carleton.ca/PCISS</url>. In addition to a dynamic PHP-generated web interface for humans, a Simple Object Access Protocol (SOAP) interface is added to permit invocation of the PCI-SS service remotely. This machine-readable interface facilitates incorporation of PCI-SS into multi-faceted systems biology analysis pipelines requiring protein secondary structure information, and greatly simplifies high-throughput analyses. XML is used to represent the input protein sequence data and also to encode the resulting structure prediction in a machine-readable format. To our knowledge, this represents the only publicly available SOAP-interface for a protein secondary structure prediction service with published WSDL interface definition. Conclusion Relative to the 9 contemporary methods included in the comparison cascaded PCI classifiers perform well, however PCI finds greatest application as a consensus classifier. When PCI is used to combine a sequence-to-structure PCI-based classifier with the current leading ANN-based method, PSIPRED, the overall error rate (Q3) is maintained while the rate of occurrence of a particularly detrimental error is reduced by up to 25%. This improvement in BAD score, combined with the machine-readable SOAP web service interface makes PCI-SS particularly useful for inclusion in a tertiary structure prediction pipeline.</p