Coping with strong translational noncrystallographic symmetry and extreme anisotropy in molecular replacement with Phaser: human Rab27a

Data pathologies caused by effects such as diffraction anisotropy and translational noncrystallographic symmetry (tNCS) can dramatically complicate the solution of the crystal structures of macromolecules. Such problems were encountered in determining the structure of a mutant form of Rab27a, a member of the Rab GTPases. Mutant Rab27a constructs that crystallize in the free form were designed for use in the discovery of drugs to reduce primary tumour invasiveness and metastasis. One construct, hRab27aMut, crystallized within 24 h and diffracted to 2.82 Å resolution, with a unit cell possessing room for a large number of protein copies. Initial efforts to solve the structure using molecular replacement by Phaser were not successful. Analysis of the data set revealed that the crystals suffered from both extreme anisotropy and strong tNCS. As a result, large numbers of reflections had estimated standard deviations that were much larger than their measured intensities and their expected intensities, revealing problems with the use of such data at the time in Phaser. By eliminating extremely weak reflections with the largest combined effects of anisotropy and tNCS, these problems could be avoided, allowing a molecular-replacement solution to be found. The lessons that were learned in solving this structure have guided improvements in the numerical analysis used in Phaser, particularly in identifying diffraction measurements that convey very little information content. The calculation of information content could also be applied as an alternative to ellipsoidal truncation. The post-mortem analysis also revealed an oversight in accounting for measurement errors in the fast rotation function. While the crystal of mutant Rab27a is not amenable to drug screening, the structure can guide new modifications to obtain more suitable crystal forms.

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New crystal form of β-lactoglobulin

Journal of Dairy Research ◽

10.1017/s0022029900032118 ◽

1996 ◽

Vol 63 (4) ◽

pp. 575-584 ◽

Cited By ~ 6

Author(s):

Thales L. Rocha ◽

Sharon Brownlow ◽

Keith N. Saddler ◽

Linda A. Fothergill-Gilmore ◽

Lindsay Sawyer

Keyword(s):

Crystal Form ◽

Unit Cell ◽

Molecular Replacement ◽

Data Set ◽

Crystal Forms ◽

Milk Whey ◽

Cell Parameters ◽

X Ray Crystallography ◽

Replacement Solution ◽

Β Lactoglobulin

SummaryThe milk whey protein β-lactoglobulin has been isolated from ovine milk, purified and crystallized in a form suitable for X-ray crystallography. The crystals, which diffract to 1·9 Å resolution, belong to the trigonal space group P3121 with unit cell lengths a = b = 99·8 Å, c = 67·7 Å and unique angle γ = 120·0°. Although there have been many crystal forms reported for bovine β-lactoglobulin, none has been reported with these unit cell parameters. A preliminary native data set has been collected and a molecular replacement solution obtained, using the structure of dimeric bovine β-lactoglobulin as the search model. The importance of the ovine structure in relation to that of the bovine is discussed.

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On the application of the expected log-likelihood gain to decision making in molecular replacement

Acta Crystallographica Section D Structural Biology ◽

10.1107/s2059798318004357 ◽

2018 ◽

Vol 74 (4) ◽

pp. 245-255 ◽

Cited By ~ 13

Author(s):

Robert D. Oeffner ◽

Pavel V. Afonine ◽

Claudia Millán ◽

Massimo Sammito ◽

Isabel Usón ◽

...

Keyword(s):

Decision Making ◽

Measurement Errors ◽

Single Atom ◽

Molecular Replacement ◽

Acta Cryst ◽

Quickest Path ◽

Experimental Phasing ◽

Log Likelihood ◽

Replacement Solution ◽

Search Order

Molecular-replacement phasing of macromolecular crystal structures is often fast, but if a molecular-replacement solution is not immediately obtained the crystallographer must judge whether to pursue molecular replacement or to attempt experimental phasing as the quickest path to structure solution. The introduction of the expected log-likelihood gain [eLLG; McCoyet al.(2017),Proc. Natl Acad. Sci. USA,114, 3637–3641] has given the crystallographer a powerful new tool to aid in making this decision. The eLLG is the log-likelihood gain on intensity [LLGI; Read & McCoy (2016),Acta Cryst.D72, 375–387] expected from a correctly placed model. It is calculated as a sum over the reflections of a function dependent on the fraction of the scattering for which the model accounts, the estimated model coordinate error and the measurement errors in the data. It is shown how the eLLG may be used to answer the question `can I solve my structure by molecular replacement?'. However, this is only the most obvious of the applications of the eLLG. It is also discussed how the eLLG may be used to determine the search order and minimal data requirements for obtaining a molecular-replacement solution using a given model, and for decision making in fragment-based molecular replacement, single-atom molecular replacement and likelihood-guided model pruning.

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Phase perturbation as a means of electron density map quality evaluation

Journal of Applied Crystallography ◽

10.1107/s0021889807049898 ◽

2008 ◽

Vol 41 (1) ◽

pp. 31-37 ◽

Cited By ~ 1

Author(s):

Olga Kirillova

Keyword(s):

Electron Density ◽

Data Sets ◽

Molecular Replacement ◽

Data Set ◽

Density Maps ◽

Phase Perturbation ◽

Replacement Solution ◽

Electron Density Map ◽

Trial Phase

This paper describes a new means for evaluating the quality of crystallographic electron density maps. It has been found that a better data set possesses greater robustness against perturbations applied to the phases. Thus it allows recognition of a more precise phase set and provides a way to select the best or reject the worst from several noisy data sets derived from the same crystal structure. The results indicate that calculation of the correlations by the procedure described here can be useful in ranking electron density maps in this aspect of quality. The method suggested has potential use for selecting a better molecular replacement solution, as well as for evaluating trial phase sets inab initiophasing procedures.

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Crystallization and preliminary crystallographic analysis of poly(3-hydroxybutyrate) depolymerase fromBacillus thuringiensis

Acta Crystallographica Section F Structural Biology Communications ◽

10.1107/s2053230x14019347 ◽

2014 ◽

Vol 70 (10) ◽

pp. 1421-1423 ◽

Cited By ~ 1

Author(s):

Yung-Lin Wang ◽

Yi-Ting Lin ◽

Chia-Lin Chen ◽

Gwo-Chyuan Shaw ◽

Shwu-Huey Liaw

Keyword(s):

Crystal Structure ◽

Crystallographic Analysis ◽

Molecular Replacement ◽

X Ray Diffraction ◽

Data Set ◽

Cell Parameters ◽

Replacement Solution ◽

Potential Applications ◽

Polymer Biodegradation ◽

Key Enzyme

Poly[(R)-3-hydroxybutyrate] (PHB) is a microbial biopolymer that has been commercialized as biodegradable plastics. The key enzyme for the degradation is PHB depolymerase (PhaZ). A new intracellular PhaZ fromBacillus thuringiensis(BtPhaZ) has been screened for potential applications in polymer biodegradation. Recombinant BtPhaZ was crystallized using 25% polyethylene glycol 3350, 0.2 Mammonium acetate, 0.1 Mbis-tris pH 6.5 at 288 K. The crystals belonged to space groupP1, with unit-cell parametersa= 42.97,b= 83.23,c= 85.50 Å, α = 73.45, β = 82.83, γ = 83.49°. An X-ray diffraction data set was collected to 1.42 Å resolution with anRmergeof 6.4%. Unexpectedly, a molecular-replacement solution was obtained using the crystal structure ofStreptomyces lividanschloroperoxidase as a template, which shares 24% sequence identity to BtPhaZ. This is the first crystal structure of an intracellular poly(3-hydroxybutyrate) depolymerase.

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Expression, purification and crystallization of the SKICH domain of human TAX1BP1

Acta Crystallographica Section F Structural Biology Communications ◽

10.1107/s2053230x14006396 ◽

2014 ◽

Vol 70 (5) ◽

pp. 619-623 ◽

Cited By ~ 2

Author(s):

Yang Yang ◽

Guan Wang ◽

Xiaolan Huang ◽

Zhihua Du

Keyword(s):

Coiled Coil ◽

Molecular Replacement ◽

Data Set ◽

C Terminus ◽

Zinc Finger Motifs ◽

Coiled Coil Region ◽

Ubiquitin Binding ◽

N Terminus ◽

Replacement Solution

TAX1BP1 is a highly conserved, pleiotropic protein that plays many essential functions in human cells, including negative regulation of inflammatory and antimicrobial responses mediated by NF-κB and IRF3 signaling, inhibition of apoptosis, transcriptional coactivation and autophagyetc.TAX1BP1 contains a SKICH domain at the N-terminus, three coiled-coil domains in the middle and two ubiquitin-binding zinc-finger motifs at the C-terminus. The SKICH domain and the linker sequence between the SKICH domain and the coiled-coil region mediate interaction with ubiquitin-like proteins of the LC3/GABARAP family, which are autophagosome markers. For structure determination of the SKICH domain of TAX1BP1, a protein construct (amino acids 15–148) corresponding to the SKICH domain plus the linker region was expressed, purified and crystallized. A native diffraction data set has been collected to 1.9 Å resolution. A molecular-replacement solution has been found by using the structure of the SKICH domain of NDP52, a paralog of TAX1BP1.

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Crystallization and preliminary X-ray diffraction studies of human catalase

Acta Crystallographica Section D Biological Crystallography ◽

10.1107/s0907444999009695 ◽

1999 ◽

Vol 55 (9) ◽

pp. 1614-1615 ◽

Cited By ~ 3

Author(s):

R. A. P. Nagem ◽

E. A. L. Martins ◽

V. M. Gonçalves ◽

R. Aparício ◽

I. Polikarpov

Keyword(s):

Search Model ◽

Molecular Replacement ◽

X Ray Diffraction ◽

Beef Liver ◽

X Ray ◽

Diffusion Technique ◽

Cell Dimensions ◽

Synchrotron Radiation Diffraction ◽

Replacement Solution ◽

Unit Cell Dimensions

The enzyme catalase (H2O2–H2O2 oxidoreductase; E.C. 11.1.6) was purified from haemolysate of human placenta and crystallized using the vapour-diffusion technique. Synchrotron-radiation diffraction data have been collected to 1.76 Å resolution. The enzyme crystallized in the space group P212121, with unit-cell dimensions a = 83.6, b = 139.4, c = 227.5 Å. A molecular-replacement solution of the structure has been obtained using beef liver catalase (PDB code 4blc) as a search model.

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Osmotically inactive sodium and potassium storage: lessons learned from the Edelman and Boling data

AJP Renal Physiology ◽

10.1152/ajprenal.00215.2016 ◽

2016 ◽

Vol 311 (3) ◽

pp. F539-F547 ◽

Cited By ~ 10

Author(s):

Minhtri K. Nguyen ◽

Dai-Scott Nguyen ◽

Minh-Kevin Nguyen

Keyword(s):

Linear Regression ◽

Measurement Errors ◽

Linear Regression Analysis ◽

Sodium Concentration ◽

Lessons Learned ◽

Dynamic Changes ◽

Data Set ◽

Storage Pool ◽

Total Body ◽

Sodium And Potassium

Because changes in the plasma water sodium concentration ([Na+]pw) are clinically due to changes in the mass balance of Na+, K+, and H2O, the analysis and treatment of the dysnatremias are dependent on the validity of the Edelman equation in defining the quantitative interrelationship between the [Na+]pw and the total exchangeable sodium (Nae), total exchangeable potassium (Ke), and total body water (TBW) (Edelman IS, Leibman J, O'Meara MP, Birkenfeld LW. J Clin Invest 37: 1236–1256, 1958): [Na+]pw = 1.11(Nae + Ke)/TBW − 25.6. The interrelationship between [Na+]pw and Nae, Ke, and TBW in the Edelman equation is empirically determined by accounting for measurement errors in all of these variables. In contrast, linear regression analysis of the same data set using [Na+]pw as the dependent variable yields the following equation: [Na+]pw = 0.93(Nae + Ke)/TBW + 1.37. Moreover, based on the study by Boling et al. (Boling EA, Lipkind JB. 18: 943–949, 1963), the [Na+]pw is related to the Nae, Ke, and TBW by the following linear regression equation: [Na+]pw = 0.487(Nae + Ke)/TBW + 71.54. The disparities between the slope and y-intercept of these three equations are unknown. In this mathematical analysis, we demonstrate that the disparities between the slope and y-intercept in these three equations can be explained by how the osmotically inactive Na+ and K+ storage pool is quantitatively accounted for. Our analysis also indicates that the osmotically inactive Na+ and K+ storage pool is dynamically regulated and that changes in the [Na+]pw can be predicted based on changes in the Nae, Ke, and TBW despite dynamic changes in the osmotically inactive Na+ and K+ storage pool.

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Russian Regional Politicians’ Income and Property Declarations: a Pilot Study and Quality Assessment of Administrative Data

Sociological Journal ◽

10.19181/socjour.2021.27.3.8422 ◽

2021 ◽

Vol 27 (3) ◽

pp. 8-34

Author(s):

Tatyana Cherkashina

Keyword(s):

Pilot Study ◽

Data Quality ◽

Quality Assessment ◽

Administrative Data ◽

Measurement Errors ◽

Private Property ◽

Research Data ◽

Quality Of Data ◽

Data Set ◽

Research Problems

The article presents the experience of converting non-targeted administrative data into research data, using as an example data on the income and property of deputies from local legislative bodies of the Russian Federation for 2019, collected as part of anticorruption operations. This particular empirical fragment was selected for the pilot study of administrative data, which includes assessing the possibility of integrating scattered fragments of information into a single database, assessing quality of data and their relevance for solving research problems, particularly analysis of high-income strata and the apparent trends towards individualization of private property. The system of indicators for assessing data quality includes their timeliness, availability, interpretability, reliability, comparability, coherence, errors of representation and measurement, and relevance. In the case of the data set in question, measurement errors are more common than representation errors. Overall the article emphasizes the notion that introducing new non-target data into circulation requires their preliminary testing, while data quality assessment becomes distributed both in time and between different subjects. The transition from created data to «obtained» data shifts the functions of evaluating its quality from the researcher-creator to the researcheruser. And though in this case data quality is in part ensured by the legal support for their production, the transformation of administrative data into research data involves assessing a variety of quality measurements — from availability to uniformity and accuracy.

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DUACS DT2014: the new multi-mission altimeter data set reprocessed over 20 years

Ocean Science ◽

10.5194/os-12-1067-2016 ◽

2016 ◽

Vol 12 (5) ◽

pp. 1067-1090 ◽

Cited By ~ 180

Author(s):

Marie-Isabelle Pujol ◽

Yannice Faugère ◽

Guillaume Taburet ◽

Stéphanie Dupuy ◽

Camille Pelloquin ◽

...

Keyword(s):

Measurement Errors ◽

Large Scale ◽

Temporal Correlation ◽

Error Reduction ◽

Internal Tides ◽

Global Ocean ◽

Altimeter Data ◽

Data Set ◽

Error Budget ◽

Spatial Coverage

Abstract. The new DUACS DT2014 reprocessed products have been available since April 2014. Numerous innovative changes have been introduced at each step of an extensively revised data processing protocol. The use of a new 20-year altimeter reference period in place of the previous 7-year reference significantly changes the sea level anomaly (SLA) patterns and thus has a strong user impact. The use of up-to-date altimeter standards and geophysical corrections, reduced smoothing of the along-track data, and refined mapping parameters, including spatial and temporal correlation-scale refinement and measurement errors, all contribute to an improved high-quality DT2014 SLA data set. Although all of the DUACS products have been upgraded, this paper focuses on the enhancements to the gridded SLA products over the global ocean. As part of this exercise, 21 years of data have been homogenized, allowing us to retrieve accurate large-scale climate signals such as global and regional MSL trends, interannual signals, and better refined mesoscale features.An extensive assessment exercise has been carried out on this data set, which allows us to establish a consolidated error budget. The errors at mesoscale are about 1.4 cm2 in low-variability areas, increase to an average of 8.9 cm2 in coastal regions, and reach nearly 32.5 cm2 in high mesoscale activity areas. The DT2014 products, compared to the previous DT2010 version, retain signals for wavelengths lower than ∼  250 km, inducing SLA variance and mean EKE increases of, respectively, +5.1 and +15 %. Comparisons with independent measurements highlight the improved mesoscale representation within this new data set. The error reduction at the mesoscale reaches nearly 10 % of the error observed with DT2010. DT2014 also presents an improved coastal signal with a nearly 2 to 4 % mean error reduction. High-latitude areas are also more accurately represented in DT2014, with an improved consistency between spatial coverage and sea ice edge position. An error budget is used to highlight the limitations of the new gridded products, with notable errors in areas with strong internal tides.

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A model of the distribution and metabolism of corticotropin-releasing factor

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.1988.254.1.e104 ◽

1988 ◽

Vol 254 (1) ◽

pp. E104-E112

Author(s):

B. Candas ◽

J. Lalonde ◽

M. Normand

Keyword(s):

Measurement Errors ◽

Compartment Model ◽

Corticotropin Releasing Factor ◽

Data Sets ◽

Data Set ◽

Rapid Injection ◽

Three Compartment Model ◽

Rival Models ◽

Sampling Schedule ◽

Selection Of

The aim of this study is the selection of the number of compartments required for a model to represent the distribution and metabolism of corticotropin-releasing factor (CRF) in rats. The dynamics of labeled rat CRF were measured in plasma for seven rats after a rapid injection. The sampling schedule resulted from the combination of the two D-optimal sampling sets of times corresponding to both rival models. This protocol improved the numerical identifiability of the parameters and consequently facilitated the selection of the relevant model. A three-compartment model fits adequately to the seven individual dynamics and better represents four of them compared with the lower-order model. It was demonstrated, using simulations in which the measurement errors and the interindividual variability of the parameters are included, that his four-to-seven ratio of data sets is consistent with the relevance of the three-compartment model for every individual kinetic data set. Kinetic and metabolic parameters were then derived for each individual rat, their values being consistent with the prolonged effects of CRF on pituitary-adrenocortical secretion.

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