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Shape Modeling and Matching in Protein Structure Identification. Sasakthi Abeysinghe, Tao Ju Washington University, St. Louis, USA Matthew Baker, Wah Chiu Baylor College of Medicine, Houston, USA. Shape Matching. Shape comparison How similar are shape A and shape B?
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Shape Modeling and Matching in Protein Structure Identification Sasakthi Abeysinghe, Tao Ju Washington University, St. Louis, USA Matthew Baker, Wah Chiu Baylor College of Medicine, Houston, USA
Shape Matching • Shape comparison • How similar are shape A and shape B? • Application: 3D model retrieval • Shape alignment • What is the best alignment of A onto B? • Application: object recognition and registration
Shape Matching • Shape comparison • How similar are shape A and shape B? • Application: 3D model retrieval • Shape alignment • What is the best alignment of A onto B? • Application: object recognition and registration 1D Protein Sequence 3D Protein Image
Structural Biology • Protein: a sequence of amino acids • Folds into a 3D structure in order to interact with other molecules • Protein function derived from its 3D structure • Identifying protein structure • Imaging methods: X-ray, NMR • Drawback: can not resolve large assemblies, like viruses. …
Domain Problem • Cryo-electron microscopy (Cryo-EM) • Produces 3D density volumes • Drawback: insufficient resolution to resolve atom locations • How to determine protein structure in a cryo-EM volume? ?
Shape Matching Formulation • Matching 1D protein sequence with 3D density volume • Intermediate goal: Matching alpha-helices • One of the basic building blocks in a protein • Identified as cylindrical densities in the volume [Baker 07] • How to align the protein sequence with the cryo-EM volume to match the two sets of helices? ? +
Method Overview • Compatible shape representation • 1D sequence and 3D volume as attributed relational graphs • Graph-based shape matching • A new constrained graph matching problem and an optimal solution • Error-tolerant (inexact) matching
Shape Representation • Protein sequence as attributed relation graph • An edge: a helix segment or a non-helix segment • Attribute: number of amino acids in the segment • A node: end of a helix of end of the sequence • Add additional edges that skip at most m helix segments • To allow matching with a cryo-EM volume that has missing helices
Shape Representation • Graph representation of Cryo-EM volume via skeletons • 3D Skeleton [Ju 06] builds connectivity among detected helices • An edge: a detected helix or a skeleton path between two helices • Attribute: length of the helix or skeleton path • A node: end of a helix of end of the protein • Add additional edges between helix-ends less than d apart • To account for missing helix connectivity in the skeleton
Shape Matching - Problem • Finding two matching chains of helices • Same number of edges • Alternating types between non-helix and helix • Minimal attribute matching error • Uniqueness of this problem: • Inexact: not all edges/nodes in the two graphs are used in the matched sequence • Constrained: the match must have a linear topology
Shape Matching - Review • Previous work on graph matching • Exact matching • Graph mono-morphism [Wong 90] • Sub-graph isomorphism [Ullmann 76, Cordella 99] • Inexact matching • A* search [Nilsson 80], simulated annealing [Herault 90], neural networks [Feng 94], probabilistic relaxation [Christmas 95], genetic algorithms [Wang 97], graph decomposition [Messmer 98] • All designed for un-constrained problems where there is no restriction on the topology of the matched sub-graphs.
Sequence Graph Volume Graph {1,1} Shape Matching - Method • Key idea: utilize the linearity of chains. • Performing depth-first tree-search • Append matching nodes to the incomplete chain with minimal matching error {2,5} 40 {2,2} 42 {2,3} 85 {2,4} 92 • A*-search • Reduce node expansion by estimating future matching error • Optimal if future error estimation is smaller than the actual error. • 3 future error functions are designed {3,5} 91 {3,3} 63 {3,4} 72 {3,4} 48 {3,2} 61 {4,3} 99 {4,5} 51 {6,6} 58
Experimental Setup • Test data • Simulated data: 8 proteins (taken from Protein Data Bank) • Authentic data: 3 proteins (produced at Baylor) • Test modes • Automatic • With a few user-specified helix correspondences • Validation with the actual helix correspondence • Produce a list of candidates sorted by their matching errors • Find out where the actual correspondence ranks in the list
Results - 1 • Bluetongue Virus (simulated, 10 helices, 0 missing) • Actual correspondence ranks #1 + Top Matching Sequence Cryo-EM volume and its skeleton
Results - 2 • Human Insulin Receptor (simulated, 9 helices, 1 missing) • Actual correspondence ranks #1 + + Top Matching Sequence Cryo-EM volume and its skeleton
Results - 3 • Bacteriophage P22 (authentic, 11 helices, 6 missing) • Actual correspondence ranks #4 + Top Matching Actual Correspondence Sequence Cryo-EM skeleton
Results - 4 • Triose Phosphate Isomerase (simulated, 12 helices, 3 missing) • Before user-specification: actual correspondence not in the candidate list • Given 2 specified helix pairs: actual correspondence ranks #9 + Top Matching Without user-specification Cryo-EM skeleton with 2 use-specified helix pairs Sequence Actual Correspondence
Result - Summary • Among the 11 proteins, the correct correspondence ranks among the candidate list computed by our method: • Top 1: 4 proteins • Within top 10: 2 proteins (1 simulated) • Top 1 after user-interaction: 2 proteins (both simulated) • 4 specified helix pairs in a 14/20-helix protein. • Within top 10 after user-interaction: 3 proteins • 2 specified helix pairs in a 6/9/12-helix protein • Performance • Under 4 seconds for proteins with 20 helices • Compare: [Wu 05] uses exhaustive search and takes 16 hours for finding correspondences in proteins with 8 helices
Conclusion • Formulate protein structure identification as shape matching • 1D protein sequence vs. 3D cryo-EM density volume • Compatible representation of disparate biological data as graphs • Formulate a constrained inexact matching problem and propose an optimal solution • Based on A*-search • Validation on simulated and authentic data
Future Work (Bio) • Incorporating beta-sheets for improved accuracy • Challenge: the match is no longer a linear chain • Integrating homology and ab initio modeling • Utilizing known 3D structure of segments • Refining the alignment by molecular energy minimization
Future Work (CS) • Faster graph matching algorithm • Explore variants of A*-search to reduce running time for larger proteins (>20 helices) • Better skeleton generation • Generate skeletons directly from gray-scale density volume for iso-value-independent representation • Utilize cell-complex-based skeleton for better skeleton geometry • Currently used for topology editing, see [Ju, Zhou and Hu. Siggraph 2007]
Pacific Graphics • Hawaii • 2007 • Oct 29 – Nov 2, in Maui, Hawaii Conference Chair: Ron Goldman Program co-chairs: Marc Alexa, Steven Gortler, Tao Ju
Results - 1 • Bluetongue Virus (simulated, 10 helices, 0 missing) • Actual correspondence ranks #1 + Top Matching Sequence Cryo-EM volume and its skeleton