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Literature DB >> 25195913

Molecular replacement with a large number of molecules in the asymmetric unit.

Chacko Jobichen¹, Kunchithapadam Swaminathan¹.

Abstract

The exponential increase in protein structures deposited in the Protein Data Bank (PDB) has resulted in the elucidation of most, if not all, protein folds, thus making molecular replacement (MR) the most frequently used method for structure determination. A survey of the PDB shows that most of the structures determined by molecular replacement contain less than ten molecules in the asymmetric unit and that it is predominantly virus and ribosome structures that contain more than 20 molecules in the asymmetric unit. While the success of the MR method depends on several factors, such as the homology and the size of an input model, it is also a well known fact that this method can become significantly difficult in cases with a large number of molecules in the asymmetric unit, higher crystallographic symmetry and tight packing. In this paper, five representative structures containing 16-18 homomeric molecules in the asymmetric unit and the strategies that have been used to solve these structures are described. The difficulties faced and the lessons learned from these structure-determination efforts will be useful for selected and similar future situations with a large number of molecules in the asymmetric unit.

Keywords: large number of molecules in the asymmetric unit; molecular replacement; strategies for structure determination

Mesh：

Year: 2014 PMID： 25195913 PMCID： PMC4157440 DOI： 10.1107/S2053230X14014381

Source DB: PubMed Journal: Acta Crystallogr F Struct Biol Commun ISSN： 2053-230X Impact factor: 1.056

18 in total

1. The Protein Data Bank.

Authors: H M Berman; J Westbrook; Z Feng; G Gilliland; T N Bhat; H Weissig; I N Shindyalov; P E Bourne
Journal: Nucleic Acids Res Date: 2000-01-01 Impact factor: 16.971

2. Validation of the catalytic mechanism of Escherichia coli purine nucleoside phosphorylase by structural and kinetic studies.

Authors: Goran Mikleušević; Zoran Stefanić; Marta Narczyk; Beata Wielgus-Kutrowska; Agnieszka Bzowska; Marija Luić
Journal: Biochimie Date: 2011-06-13 Impact factor: 4.079

3. Solvent content of protein crystals.

Authors: B W Matthews
Journal: J Mol Biol Date: 1968-04-28 Impact factor: 5.469

4. The structure of pyruvate kinase from Leishmania mexicana reveals details of the allosteric transition and unusual effector specificity.

Authors: D J Rigden; S E Phillips; P A Michels; L A Fothergill-Gilmore
Journal: J Mol Biol Date: 1999-08-20 Impact factor: 5.469

5. Structural characterization of nitrosomonas europaea cytochrome c-552 variants with marked differences in electronic structure.

Authors: Mehmet Can; Jolanta Krucinska; Giorgio Zoppellaro; Niels H Andersen; Joseph E Wedekind; Hans-Petter Hersleth; K Kristoffer Andersson; Kara L Bren
Journal: Chembiochem Date: 2013-07-31 Impact factor: 3.164

6. Structural and biophysical characterization of Mycobacterium tuberculosis dodecin Rv1498A.

Authors: Fengxia Liu; Junhui Xiong; Sundaramurthy Kumar; Chunyan Yang; Shengxiang Ge; Shaowei Li; Ningshao Xia; Kunchithapadam Swaminathan
Journal: J Struct Biol Date: 2011-04-24 Impact factor: 2.867

7. The structure of nitric oxide synthase oxygenase domain and inhibitor complexes.

Authors: B R Crane; A S Arvai; R Gachhui; C Wu; D K Ghosh; E D Getzoff; D J Stuehr; J A Tainer
Journal: Science Date: 1997-10-17 Impact factor: 47.728

8. PHENIX: a comprehensive Python-based system for macromolecular structure solution.

Authors: Paul D Adams; Pavel V Afonine; Gábor Bunkóczi; Vincent B Chen; Ian W Davis; Nathaniel Echols; Jeffrey J Headd; Li-Wei Hung; Gary J Kapral; Ralf W Grosse-Kunstleve; Airlie J McCoy; Nigel W Moriarty; Robert Oeffner; Randy J Read; David C Richardson; Jane S Richardson; Thomas C Terwilliger; Peter H Zwart
Journal: Acta Crystallogr D Biol Crystallogr Date: 2010-01-22

Molecular replacement with a large number of molecules in the asymmetric unit.

1. The Protein Data Bank.

2. Validation of the catalytic mechanism of Escherichia coli purine nucleoside phosphorylase by structural and kinetic studies.

3. Solvent content of protein crystals.

4. The structure of pyruvate kinase from Leishmania mexicana reveals details of the allosteric transition and unusual effector specificity.

5. Structural characterization of nitrosomonas europaea cytochrome c-552 variants with marked differences in electronic structure.

6. Structural and biophysical characterization of Mycobacterium tuberculosis dodecin Rv1498A.

7. The structure of nitric oxide synthase oxygenase domain and inhibitor complexes.

8. PHENIX: a comprehensive Python-based system for macromolecular structure solution.

9. Dodecins: a family of lumichrome binding proteins.

10. Phaser crystallographic software.

1. ErbB3-binding protein 1 (EBP1) represses HNF4α-mediated transcription and insulin secretion in pancreatic β-cells.

2. Ten things I `hate' about refinement.