Sequence assignment for low-resolution modelling of protein crystal structures.

Journal: Acta crystallographica. Section D, Structural biology

Published Date: Aug 1, 2019

Abstract

The performance of automated model building in crystal structure determination usually decreases with the resolution of the experimental data, and may result in fragmented models and incorrect side-chain assignment. Presented here are new methods for machine-learning-based docking of main-chain fragments to the sequence and for their sequence-independent connection using a dedicated library of protein fragments. The combined use of these new methods noticeably increases sequence coverage and reduces fragmentation of the protein models automatically built with ARP/wARP.

Authors

Grzegorz Chojnowski

European Molecular Biology Laboratory, c/o DESY, Notkestrasse 85, 22607 Hamburg, Germany.
Joana Pereira

European Molecular Biology Laboratory, c/o DESY, Notkestrasse 85, 22607 Hamburg, Germany.
Victor S Lamzin

European Molecular Biology Laboratory, c/o DESY, Notkestrasse 85, 22607 Hamburg, Germany.

Keywords

Algorithms Amino Acid Sequence Crystallography, X-Ray Databases, Protein Datasets as Topic Machine Learning Molecular Docking Simulation Protein Conformation Proteins Software

External Resources

View on PubMed Access via DOI PubMed (31373574)

Sequence assignment for low-resolution modelling of protein crystal structures.

Abstract

Authors

Keywords

External Resources

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