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Detecting Repetitions and Periodicities in Proteins by Tiling the Structural Space
Author(s) -
R. Gonzalo Parra,
Rocío Espada,
Ignacio E. Sánchez,
Manfred J. Sippl,
Diego U. Ferreiro
Publication year - 2013
Publication title -
the journal of physical chemistry b
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.864
H-Index - 392
eISSN - 1520-6106
pISSN - 1520-5207
DOI - 10.1021/jp402105j
Subject(s) - energy landscape , tessellation (computer graphics) , space (punctuation) , folding (dsp implementation) , sequence space , metric (unit) , computer science , energy (signal processing) , variety (cybernetics) , sequence (biology) , quantitative biology , protein folding , computational biology , function (biology) , theoretical computer science , combinatorics , mathematics , biology , evolutionary biology , pure mathematics , genetics , geometry , artificial intelligence , biochemistry , banach space , operations management , statistics , electrical engineering , economics , engineering , operating system
The notion of energy landscapes provides conceptual tools for understanding the complexities of protein folding and function. Energy landscape theory indicates that it is much easier to find sequences that satisfy the "Principle of Minimal Frustration" when the folded structure is symmetric (Wolynes, P. G. Symmetry and the Energy Landscapes of Biomolecules. Proc. Natl. Acad. Sci. U.S.A. 1996, 93, 14249-14255). Similarly, repeats and structural mosaics may be fundamentally related to landscapes with multiple embedded funnels. Here we present analytical tools to detect and compare structural repetitions in protein molecules. By an exhaustive analysis of the distribution of structural repeats using a robust metric, we define those portions of a protein molecule that best describe the overall structure as a tessellation of basic units. The patterns produced by such tessellations provide intuitive representations of the repeating regions and their association toward higher order arrangements. We find that some protein architectures can be described as nearly periodic, while in others clear separations between repetitions exist. Since the method is independent of amino acid sequence information, we can identify structural units that can be encoded by a variety of distinct amino acid sequences.

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