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MSACompro: protein multiple sequence alignment using predicted secondary structure, solvent accessibility, and residue-residue contacts

Author: A Krogh
AN Tegge
C Notredame
CB Do
DF Feng
DG Higgins
DG Higgins
DG Higgins
DG Higgins
F Jeanmougin
F Wilcoxon
G Pollastri
GH Gonnet
GJ Barton
GP Raghava
GP Raghava
HY Zhou
J Cheng
J Heringa
J Pei
J Pei
J Pei
J Söding
J Söding
JD Thompson
JD Thompson
JD Thompson
JD Thompson
Jianlin Cheng
K Katoh
M Brudno
M Larkin
NK Kim
NS Boutonnet
O Poirot
O Poirot
PHA Sneath
R Chenna
R Durbin
RC Edgar
RC Edgar
RK Bradley
RS Amarendran
RS Amarendran
RS Amarendran
S Chikkagoudar
SE Brenner
SH Sze
T Kawabata
TL Bailey
U Roshan
V Walle
V Walle
Xin Deng
YC Liu
Publication venue: BioMed Central
Publication date: 01/01/2011
Field of study

Abstract Background Multiple Sequence Alignment (MSA) is a basic tool for bioinformatics research and analysis. It has been used essentially in almost all bioinformatics tasks such as protein structure modeling, gene and protein function prediction, DNA motif recognition, and phylogenetic analysis. Therefore, improving the accuracy of multiple sequence alignment is important for advancing many bioinformatics fields. Results We designed and developed a new method, MSACompro, to synergistically incorporate predicted secondary structure, relative solvent accessibility, and residue-residue contact information into the currently most accurate posterior probability-based MSA methods to improve the accuracy of multiple sequence alignments. The method is different from the multiple sequence alignment methods (e.g. 3D-Coffee) that use the tertiary structure information of some sequences since the structural information of our method is fully predicted from sequences. To the best of our knowledge, applying predicted relative solvent accessibility and contact map to multiple sequence alignment is novel. The rigorous benchmarking of our method to the standard benchmarks (i.e. BAliBASE, SABmark and OXBENCH) clearly demonstrated that incorporating predicted protein structural information improves the multiple sequence alignment accuracy over the leading multiple protein sequence alignment tools without using this information, such as MSAProbs, ProbCons, Probalign, T-coffee, MAFFT and MUSCLE. And the performance of the method is comparable to the state-of-the-art method PROMALS of using structural features and additional homologous sequences by slightly lower scores. Conclusion MSACompro is an efficient and reliable multiple protein sequence alignment tool that can effectively incorporate predicted protein structural information into multiple sequence alignment. The software is available at <url>http://sysbio.rnet.missouri.edu/multicom_toolbox/</url>.</p

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