A protein crystallisation screening kit designed using polyethylene glycol as major precipitant

Liu, Yue; Zhang, Xianfang; Zhang, Chenyan; Guo, Yang; Xie, Shengshi; Zhou, Ren-Bin; Cheng, Qing-Di; Yan, Er-Kai; Liu, Yali; Lu, Xiaoli; Lu, Qi; Lu, Hui‐Meng; Ye, Ya-Jing; Yin, Da‐Chuan

doi:10.1039/c5ce00779h

Cited by 13 publications

(14 citation statements)

References 26 publications

(36 reference statements)

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“…The chemical ingredients in this screen included sodium formate, (NH 4 ) 2 SO 4 , MgCl 2 , potassium sodium tartrate, sodium malonate, Tacsimate, ethylene glycol, isopropanol, MPD, EDTA‐2Na, and glycine. Based on additional information from BMCD, a third kit was modified and created based on four different aspects, such as extending pH range, broadening types, and concentrations of precipitants, as well as increasing more effective additives, which showed better performance in screening hits than PEGRx HT or PEG/Ion HT …”

Section: New Progress In Crystallization Condition Screening Practicementioning

confidence: 99%

An Analysis on Commercial Screening Kits and Chemical Components in Biomacromolecular Crystallization Screening

Qin

Xie

Zhang

et al. 2019

Crystal Research and Technology

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Obtaining diffraction-quality crystals is still a bottleneck for biomacromolecular structure determination using X-ray diffraction. In practice, the bottleneck mainly comprises two aspects: difficulties in screening and in optimization, and both of them need screening kits. The paper aims at an investigation of the chemical components employed in 86 common commercial screening kits, and comparison with those in the Biological Macromolecules Crystallization Database (BMCD). First, the 86 screening kits are systematically analyzed in terms of design methods, classification, applicable scope, and manufacturing company. Second, the chemical components applied in these screening kits are investigated in detail in terms of the classification and utilization frequency, which are compared with those in BMCD. Third, four main chemical reagents of screening kits including salts, buffers, precipitants, and additives are analyzed in detail. The top ten utilized chemical components are listed. Last, the paper summarizes new progress and further innovation in crystallization condition screening practice and screening kits design. The analysis result would be a valuable reference for rational selection and design of screening kits, and even for personalized screening of a target biomacromolecule, which would provide new ideas to solve the bottleneck problem of biomacromolecular structure determination.

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Section: New Progress In Crystallization Condition Screening Practicementioning

confidence: 99%

An Analysis on Commercial Screening Kits and Chemical Components in Biomacromolecular Crystallization Screening

Qin

Xie

Zhang

et al. 2019

Crystal Research and Technology

Self Cite

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show abstract

“…Chemical agents that can precipitate or aggregate proteins are critical for protein crystallization; [34][35][36][37][38][39][40][41][42] yet, there is no theoretical or empirical set of rules to guide the choice of precipitants in crystallizing a specic protein. For this reason, chemical screening kits have been developed to screen for large sets of reagents and conditions for protein crystallization.…”

Section: Protein Aggregation Induced By 5 0 Dscgmentioning

confidence: 99%

“…For this reason, chemical screening kits have been developed to screen for large sets of reagents and conditions for protein crystallization. [34][35][36][37][38] Surprisingly, poly(ethylene glycol) (PEG) is oen one of the major components for these kits and research. [34][35][36][37] PEG does not denature proteins and presumably excludes proteins in the solution.…”

Section: Protein Aggregation Induced By 5 0 Dscgmentioning

confidence: 99%

“…[34][35][36][37][38] Surprisingly, poly(ethylene glycol) (PEG) is oen one of the major components for these kits and research. [34][35][36][37] PEG does not denature proteins and presumably excludes proteins in the solution. [39][40][41] Other non-denaturing chemicals such as cyclodextrins have also been used as nucleants for seeding protein aggregates and crystals.…”

Section: Protein Aggregation Induced By 5 0 Dscgmentioning

confidence: 99%

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Cromoglycate mesogen forms isodesmic assemblies promoted by peptides and induces aggregation of a range of proteins

2018

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“…However, X-ray sources do not provide enough capacity to produce detectable diff raction for a single protein molecule, also the success of X-ray crystallographic studies much depends on the quality of the crystals [4]. The way to obtain protein crystals is still a difficult problem for the structural determination of proteins due to its complexity and difficulties [5].…”

Section: Introductionmentioning

confidence: 99%

Research on Concanavalin A Crystallization in a Flow-Free Droplet-Based Device

Du¹,

Zhang²,

Ji³

et al. 2017

Proceedings of the 2nd International Conference on Biomedical and Biological Engineering 2017 (BBE 2017)

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Abstract. Protein crystallography is a very critical process that limits the development of pharmaceutical engineering. Microfluidic technology has provided an opportunity for protein crystallization. In this paper, a flow-free droplet-based device is presented for producing highly controlled crystals and fabrication of this device with polydimethylsiloxane (PDMS) is presented. The experiment was performed on the device and shows that the crystals of Con A and protein ligand (DK3) have a spherical structure.

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A protein crystallisation screening kit designed using polyethylene glycol as major precipitant

Cited by 13 publications

References 26 publications

An Analysis on Commercial Screening Kits and Chemical Components in Biomacromolecular Crystallization Screening

An Analysis on Commercial Screening Kits and Chemical Components in Biomacromolecular Crystallization Screening

Cromoglycate mesogen forms isodesmic assemblies promoted by peptides and induces aggregation of a range of proteins

Research on Concanavalin A Crystallization in a Flow-Free Droplet-Based Device

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