4.7 Article

ZEAL: protein structure alignment based on shape similarity

BIOINFORMATICS (2021)

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Journal

BIOINFORMATICS
Volume 37, Issue 18, Pages 2874-2881

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/bioinformatics/btab205

Keywords

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Categories

Biochemical Research Methods Biotechnology & Applied Microbiology Computer Science, Interdisciplinary Applications Mathematical & Computational Biology Statistics & Probability

Funding

  1. European Research Council (ERC) under the European Union's Horizon 2020 research and innovation programme [771820]
  2. European Research Council (ERC) [771820] Funding Source: European Research Council (ERC)

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The study introduces ZEAL, an interactive tool for superimposing global and local protein structures based on their shape resemblance. ZEAL outperforms other methods for shape-based superposition and is particularly effective for comparing proteins with limited sequence and backbone-fold similarity. The tool can be used to study relationships between shape and protein function, with particularly common global surface shape similarity found among DNA binding proteins.
Motivation: Most protein-structure superimposition tools consider only Cartesian coordinates. Yet, much of biology happens on the surface of proteins, which is why proteins with shared ancestry and similar function often have comparable surface shapes. Superposition of proteins based on surface shape can enable comparison of highly divergent proteins, identify convergent evolution and enable detailed comparison of surface features and binding sites. Results: We present ZEAL, an interactive tool to superpose global and local protein structures based on their shape resemblance using 3D (Zernike-Canterakis) functions to represent the molecular surface. In a benchmark study of structures with the same fold, we show that ZEAL outperforms two other methods for shape-based superposition. In addition, alignments from ZEAL were of comparable quality to the coordinate-based superpositions provided by TM-align. For comparisons of proteins with limited sequence and backbone-fold similarity, where coordinate-based methods typically fail, ZEAL can often find alignments with substantial surface-shape correspondence. In combination with shape-based matching, ZEAL can be used as a general tool to study relationships between shape and protein function. We identify several categories of protein functions where global shape similarity is significantly more likely than expected by random chance, when comparing proteins with little similarity on the fold level. In particular, we find that global surface shape similarity is particular common among DNA binding proteins.

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