4.7 Article

Multiresolution persistent homology for excessively large biomolecular datasets

Journal

JOURNAL OF CHEMICAL PHYSICS
Volume 143, Issue 13, Pages -

Publisher

AMER INST PHYSICS
DOI: 10.1063/1.4931733

Keywords

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Funding

  1. NSF [DMS-1160352, IIS-1302285]
  2. MSU Center for Mathematical Molecular Biosciences initiative
  3. NIH [R01GM-090208]
  4. Div Of Information & Intelligent Systems
  5. Direct For Computer & Info Scie & Enginr [1302285] Funding Source: National Science Foundation

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Although persistent homology has emerged as a promising tool for the topological simplification of complex data, it is computationally intractable for large datasets. We introduce multiresolution persistent homology to handle excessively large datasets. We match the resolution with the scale of interest so as to represent large scale datasets with appropriate resolution. We utilize flexibilityrigidity index to access the topological connectivity of the data set and define a rigidity density for the filtration analysis. By appropriately tuning the resolution of the rigidity density, we are able to focus the topological lens on the scale of interest. The proposed multiresolution topological analysis is validated by a hexagonal fractal image which has three distinct scales. We further demonstrate the proposed method for extracting topological fingerprints from DNA molecules. In particular, the topological persistence of a virus capsid with 273 780 atoms is successfully analyzed which would otherwise be inaccessible to the normal point cloud method and unreliable by using coarse-grained multiscale persistent homology. The proposed method has also been successfully applied to the protein domain classification, which is the first time that persistent homology is used for practical protein domain analysis, to our knowledge. The proposed multiresolution topological method has potential applications in arbitrary data sets, such as social networks, biological networks, and graphs. (C) 2015 AIP Publishing LLC.

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