Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
Author
Journal
IF	>30 >20 >10 >5 all

Title	Fragment-based determination of a proteinase K structure from MicroED data using ARCIMBOLDO_SHREDDER.
Journal, issue, pages	Acta Crystallogr D Struct Biol, Vol. 76, Issue Pt 8, Page 703-712, Year 2020
Publish date	Aug 1, 2020
Authors	Logan S Richards / Claudia Millán / Jennifer Miao / Michael W Martynowycz / Michael R Sawaya / Tamir Gonen / Rafael J Borges / Isabel Usón / Jose A Rodriguez /
PubMed Abstract	Structure determination of novel biological macromolecules by X-ray crystallography can be facilitated by the use of small structural fragments, some of only a few residues in length, as effective ...Structure determination of novel biological macromolecules by X-ray crystallography can be facilitated by the use of small structural fragments, some of only a few residues in length, as effective search models for molecular replacement to overcome the phase problem. Independence from the need for a complete pre-existing model with sequence similarity to the crystallized molecule is the primary appeal of ARCIMBOLDO, a suite of programs which employs this ab initio algorithm for phase determination. Here, the use of ARCIMBOLDO is investigated to overcome the phase problem with the electron cryomicroscopy (cryoEM) method known as microcrystal electron diffraction (MicroED). The results support the use of the ARCIMBOLDO_SHREDDER pipeline to provide phasing solutions for a structure of proteinase K from 1.6 Å resolution data using model fragments derived from the structures of proteins sharing a sequence identity of as low as 20%. ARCIMBOLDO_SHREDDER identified the most accurate polyalanine fragments from a set of distantly related sequence homologues. Alternatively, such templates were extracted in spherical volumes and given internal degrees of freedom to refine towards the target structure. Both modes relied on the rotation function in Phaser to identify or refine fragment models and its translation function to place them. Model completion from the placed fragments proceeded through phase combination of partial solutions and/or density modification and main-chain autotracing using SHELXE. The combined set of fragments was sufficient to arrive at a solution that resembled that determined by conventional molecular replacement using the known target structure as a search model. This approach obviates the need for a single, complete and highly accurate search model when phasing MicroED data, and permits the evaluation of large fragment libraries for this purpose.
External links	Acta Crystallogr D Struct Biol / PubMed:32744252 / PubMed Central
Methods	EM (electron crystallography)
Resolution	1.6 Å
Structure data	21109 6v8r EMDB-21109, PDB-6v8r: Proteinase K Determined by MicroED Phased by ARCIMBOLDO_SHREDDER Method: EM (electron crystallography)
Chemicals	ChemComp-CA: Unknown entry ChemComp-HOH: WATER / Water
Source	parengyodontium album (fungus)
Keywords	HYDROLASE / ARCIMBOLDO / MicroED