Modelling covalent linkages in CCP4

Author:

Nicholls Robert A.ORCID,Joosten Robbie P.ORCID,Long FeiORCID,Wojdyr MarcinORCID,Lebedev AndreyORCID,Krissinel Eugene,Catapano LucreziaORCID,Fischer MarcusORCID,Emsley Paul,Murshudov Garib N.ORCID

Abstract

In this contribution, the current protocols for modelling covalent linkages within the CCP4 suite are considered. The mechanism used for modelling covalent linkages is reviewed: the use of dictionaries for describing changes to stereochemistry as a result of the covalent linkage and the application of link-annotation records to structural models to ensure the correct treatment of individual instances of covalent linkages. Previously, linkage descriptions were lacking in quality compared with those of contemporary component dictionaries. Consequently, AceDRG has been adapted for the generation of link dictionaries of the same quality as for individual components. The approach adopted by AceDRG for the generation of link dictionaries is outlined, which includes associated modifications to the linked components. A number of tools to facilitate the practical modelling of covalent linkages available within the CCP4 suite are described, including a new restraint-dictionary accumulator, the Make Covalent Link tool and AceDRG interface in Coot, the 3D graphical editor JLigand and the mechanisms for dealing with covalent linkages in the CCP4i2 and CCP4 Cloud environments. These integrated solutions streamline and ease the covalent-linkage modelling workflow, seamlessly transferring relevant information between programs. Current recommended practice is elucidated by means of instructive practical examples. By summarizing the different approaches to modelling linkages that are available within the CCP4 suite, limitations and potential pitfalls that may be encountered are highlighted in order to raise awareness, with the intention of improving the quality of future modelled covalent linkages in macromolecular complexes.

Funder

Medical Research Council

Biotechnology and Biological Sciences Research Council

CCP4

Horizon 2020 Framework Programme

American Lebanese Syrian Associated Charities

Publisher

International Union of Crystallography (IUCr)

Subject

Structural Biology

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