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Automated multi-model reconstruction from single-particle electron microscopy data.


ABSTRACT: Biological macromolecules can adopt multiple conformational and compositional states due to structural flexibility and alternative subunit assemblies. This structural heterogeneity poses a major challenge in the study of macromolecular structure using single-particle electron microscopy. We propose a fully automated, unsupervised method for the three-dimensional reconstruction of multiple structural models from heterogeneous data. As a starting reference, our method employs an initial structure that does not account for any heterogeneity. Then, a multi-stage clustering is used to create multiple models representative of the heterogeneity within the sample. The multi-stage clustering combines an existing approach based on Multivariate Statistical Analysis to perform clustering within individual Euler angles, and a newly developed approach to sort out class averages from individual Euler angles into homogeneous groups. Structural models are computed from individual clusters. The whole data classification is further refined using an iterative multi-model projection-matching approach. We tested our method on one synthetic and three distinct experimental datasets. The tests include the cases where a macromolecular complex exhibits structural flexibility and cases where a molecule is found in ligand-bound and unbound states. We propose the use of our approach as an efficient way to reconstruct distinct multiple models from heterogeneous data.

SUBMITTER: Shatsky M 

PROVIDER: S-EPMC2841227 | biostudies-literature | 2010 Apr

REPOSITORIES: biostudies-literature

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Automated multi-model reconstruction from single-particle electron microscopy data.

Shatsky Maxim M   Hall Richard J RJ   Nogales Eva E   Malik Jitendra J   Brenner Steven E SE  

Journal of structural biology 20100118 1


Biological macromolecules can adopt multiple conformational and compositional states due to structural flexibility and alternative subunit assemblies. This structural heterogeneity poses a major challenge in the study of macromolecular structure using single-particle electron microscopy. We propose a fully automated, unsupervised method for the three-dimensional reconstruction of multiple structural models from heterogeneous data. As a starting reference, our method employs an initial structure  ...[more]

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