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Protein structure search and local structure characterization

Author: A Andreeva
AC Camproux
AG de Brevern
AG de Brevern
AG de Brevern
AR Ortiz
B Offmann
B Rost
C Benros
C Bystroff
CA Orengo
D Baker
E Appella
F Birzele
F Guyon
G Pollastri
HM Berman
IN Shindyalo
J Garnier
J Schuchhardt
J Vesanto
JA Hartigan
JM Yang
JS Fetrow
L Holm
M Carpentier
M Dudev
M Tyagi
M Tyagi
M Tyagi
NJ Mulder
O Sander
R Unger
S Henikoff
Shih-Yen Ku
T Madej
TL Bailey
TM Mitchell
TN Petersen
U Hobohm
VS Gowri
W Humphrey
WM Zheng
WR Pearson
Y Liu
Y Ye
Yuh-Jyh Hu
Publication venue: BioMed Central
Publication date: 01/01/2008
Field of study

Abstract Background Structural similarities among proteins can provide valuable insight into their functional mechanisms and relationships. As the number of available three-dimensional (3D) protein structures increases, a greater variety of studies can be conducted with increasing efficiency, among which is the design of protein structural alphabets. Structural alphabets allow us to characterize local structures of proteins and describe the global folding structure of a protein using a one-dimensional (1D) sequence. Thus, 1D sequences can be used to identify structural similarities among proteins using standard sequence alignment tools such as BLAST or FASTA. Results We used self-organizing maps in combination with a minimum spanning tree algorithm to determine the optimum size of a structural alphabet and applied the k-means algorithm to group protein fragnts into clusters. The centroids of these clusters defined the structural alphabet. We also developed a flexible matrix training system to build a substitution matrix (TRISUM-169) for our alphabet. Based on FASTA and using TRISUM-169 as the substitution matrix, we developed the SA-FAST alignment tool. We compared the performance of SA-FAST with that of various search tools in database-scale search tasks and found that SA-FAST was highly competitive in all tests conducted. Further, we evaluated the performance of our structural alphabet in recognizing specific structural domains of EGF and EGF-like proteins. Our method successfully recovered more EGF sub-domains using our structural alphabet than when using other structural alphabets. SA-FAST can be found at <url>http://140.113.166.178/safast/</url>. Conclusion The goal of this project was two-fold. First, we wanted to introduce a modular design pipeline to those who have been working with structural alphabets. Secondly, we wanted to open the door to researchers who have done substantial work in biological sequences but have yet to enter the field of protein structure research. Our experiments showed that by transforming the structural representations from 3D to 1D, several 1D-based tools can be applied to structural analysis, including similarity searches and structural motif finding.</p

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