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  Defining an essence of structure determining residue contacts in proteins

Sathyapriya, R., Duarte, J. M., Stehr, H., Filippis, I., & Lappe, M. (2009). Defining an essence of structure determining residue contacts in proteins. PLoS Computational Biology, 5(12), e1000584-e1000584. doi:10.1371/journal.pcbi.1000584.

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アイテムのパーマリンク: https://hdl.handle.net/11858/00-001M-0000-0010-7CB2-D 版のパーマリンク: https://hdl.handle.net/11858/00-001M-0000-0010-7CB3-B
資料種別: 学術論文
その他のタイトル : PLoS Comput Biol

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 作成者:
Sathyapriya, R.1, 著者           
Duarte, Jose M.1, 著者           
Stehr, Henning1, 著者           
Filippis, Ioannis2, 著者
Lappe, Michael1, 著者           
所属:
1Independent Junior Research Groups (OWL), Max Planck Institute for Molecular Genetics, Max Planck Society, ou_1433554              
2Max Planck Society, ou_persistent13              

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キーワード: -
 要旨: The network of native non-covalent residue contacts determines the three-dimensional structure of a protein. However, not all contacts are of equal structural significance, and little knowledge exists about a minimal, yet sufficient, subset required to define the global features of a protein. Characterisation of this “structural essence” has remained elusive so far: no algorithmic strategy has been devised to-date that could outperform a random selection in terms of 3D reconstruction accuracy (measured as the Ca RMSD). It is not only of theoretical interest (i.e., for design of advanced statistical potentials) to identify the number and nature of essential native contacts—such a subset of spatial constraints is very useful in a number of novel experimental methods (like EPR) which rely heavily on constraint-based protein modelling. To derive accurate three-dimensional models from distance constraints, we implemented a reconstruction pipeline using distance geometry. We selected a test-set of 12 protein structures from the four major SCOP fold classes and performed our reconstruction analysis. As a reference set, series of random subsets (ranging from 10% to 90% of native contacts) are generated for each protein, and the reconstruction accuracy is computed for each subset. We have developed a rational strategy, termed “cone-peeling” that combines sequence features and network descriptors to select minimal subsets that outperform the reference sets. We present, for the first time, a rational strategy to derive a structural essence of residue contacts and provide an estimate of the size of this minimal subset. Our algorithm computes sparse subsets capable of determining the tertiary structure at approximately 4.8 Å Ca RMSD with as little as 8% of the native contacts (Ca-Ca and Cb-Cb). At the same time, a randomly chosen subset of native contacts needs about twice as many contacts to reach the same level of accuracy. This “structural essence” opens new avenues in the fields of structure prediction, empirical potentials and docking.

資料詳細

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言語: eng - English
 日付: 2009-12-04
 出版の状態: 出版
 ページ: -
 出版情報: -
 目次: -
 査読: -
 識別子(DOI, ISBNなど): eDoc: 457366
DOI: 10.1371/journal.pcbi.1000584
URI: http://www.ploscompbiol.org/article/fetchObjectAttachment.action?uri=info%3Adoi%2F10.1371%2Fjournal.pcbi.1000584&representation=PDF
 学位: -

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出版物 1

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出版物名: PLoS Computational Biology
  出版物の別名 : PLoS Comput Biol
種別: 学術雑誌
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出版社, 出版地: -
ページ: - 巻号: 5 (12) 通巻号: - 開始・終了ページ: e1000584 - e1000584 識別子(ISBN, ISSN, DOIなど): ISSN: 1553-734X