Your search keyword '"PDB-REDO"' showing total 2 results

1. New restraints and validation approaches for nucleic acid structures in PDB-REDO.

Author

de Vries I, Kwakman T, Lu XJ, Hekkelman ML, Deshpande M, Velankar S, Perrakis A, and Joosten RP

Subjects

Models, Molecular, Computational Biology methods, Nucleic Acid Conformation, Nucleic Acids chemistry, Software

Abstract

The quality of macromolecular structure models crucially depends on refinement and validation targets, which optimally describe the expected chemistry. Commonly used software for these two procedures has been designed and developed in a protein-centric manner, resulting in relatively few established features for the refinement and validation of nucleic acid-containing structure models. Here, new nucleic acid-specific approaches implemented in PDB-REDO are described, including a new restraint model using noncovalent geometries (base-pair hydrogen bonding and base-pair stacking) as refinement targets. New validation routines are also presented, including a metric for Watson-Crick base-pair geometry normality (Z bpG ). Applying the PDB-REDO pipeline with the new restraint model to the whole Protein Data Bank (PDB) demonstrates an overall positive effect on the quality of nucleic acid-containing structure models. Finally, we discuss examples of improvements in the geometry of specific nucleic acid structures in the PDB. The new PDB-REDO models and pipeline are available at https://pdb-redo.eu/., (open access.)

Published

2021

2. Building and rebuilding N-glycans in protein structure models.

Author

van Beusekom B, Wezel N, Hekkelman ML, Perrakis A, Emsley P, and Joosten RP

Subjects

Carbohydrate Sequence, Crystallography, X-Ray methods, Humans, Models, Molecular, Carbohydrate Conformation, Databases, Protein, Glycoproteins chemistry, Polysaccharides chemistry, Protein Conformation

Abstract

N-Glycosylation is one of the most common post-translational modifications and is implicated in, for example, protein folding and interaction with ligands and receptors. N-Glycosylation trees are complex structures of linked carbohydrate residues attached to asparagine residues. While carbohydrates are typically modeled in protein structures, they are often incomplete or have the wrong chemistry. Here, new tools are presented to automatically rebuild existing glycosylation trees, to extend them where possible, and to add new glycosylation trees if they are missing from the model. The method has been incorporated in the PDB-REDO pipeline and has been applied to build or rebuild 16 452 carbohydrate residues in 11 651 glycosylation trees in 4498 structure models, and is also available from the PDB-REDO web server. With better modeling of N-glycosylation, the biological function of this important modification can be better and more easily understood., (open access.)

Published

2019