EMatch: Discovery of High Resolution Structural Homologues of Protein Domains in Intermediate Resolution Cryo-EM Maps

EMatch: Discovery of High Resolution Structural Homologues of Protein Domains in Intermediate Resolution Cryo-EM Maps

Cryo-EM has become an increasingly powerful technique for elucidating the structure, dynamics, and function of large flexible macromolecule assemblies that cannot be determined at atomic resolution. However, due to the relatively low resolution of cryo-EM data, a major challenge is to identify compo...

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Veröffentlicht in:IEEE/ACM transactions on computational biology and bioinformatics 2007-01, Vol.4 (1), p.28-39
Hauptverfasser: Lasker, K., Dror, O., Shatsky, M., Nussinov, R., Wolfson, H.J.
Format: Artikel
Sprache:eng
Schlagworte:
3D alignment of secondary structures
Adaptor Protein Complex 2 - chemistry
Adaptor Protein Complex 2 - ultrastructure
Algorithms
Assembly
Bioinformatics
Biomembranes
Chaperonin 60 - chemistry
Chaperonin 60 - ultrastructure
Computational Biology - methods
Cryoelectron Microscopy - methods
Crystallography
cyclic symmetry
Databases, Protein
Fitting
Image Processing, Computer-Assisted - methods
Inspection
intermediate resolution cryo-EM maps
macromolecular assemblies
Microscopy
Models, Molecular
Photosynthetic Reaction Center Complex Proteins - chemistry
Photosynthetic Reaction Center Complex Proteins - ultrastructure
Protein Structure, Secondary
Protein Structure, Tertiary
Proteins
Shape
Structural bioinformatics
Structural Homology, Protein
Triose-Phosphate Isomerase - chemistry
Triose-Phosphate Isomerase - ultrastructure
Visualization
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Beschreibung
Zusammenfassung:Cryo-EM has become an increasingly powerful technique for elucidating the structure, dynamics, and function of large flexible macromolecule assemblies that cannot be determined at atomic resolution. However, due to the relatively low resolution of cryo-EM data, a major challenge is to identify components of complexes appearing in cryo-EM maps. Here, we describe EMatch, a novel integrated approach for recognizing structural homologues of protein domains present in a 6-10 A resolution cryo-EM map and constructing a quasi-atomic structural model of their assembly. The method is highly efficient and has been successfully validated on various simulated data. The strength of the method is demonstrated by a domain assembly of an experimental cryo-EM map of native GroEL at 6 Aring resolution
ISSN:1545-5963
1557-9964
DOI:10.1109/TCBB.2007.1003