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Strategies for the structural analysis of multi-protein complexes: Lessons from the 3D-Repertoire project.

J Struct Biol.. 2011-08;  175(2):147-58
Collinet B, Friberg A, Brooks MA, van den Elzen T, Henriot V, Dziembowski A, Graille M, Durand D, Leulliot N, Saint AndrÉ C, Lazar N, Sattler M, SÉraphin B, van Tilbeurgh H. a IBBMC-CNRS UMR8619, IFR 115, Bât. 430, Université Paris-Sud, 91405 Orsay, Franceb Institute of Structural Biology, Helmholtz Zentrum München, 85764 Neuherberg, Germanyc Biomolecular NMR and Munich Center for Integrated Protein Science, Department Chemie, Technische Universität München, 85747 Garching, Germanyd Equipe Labellisée La Ligue, Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Institut National de Sant&eacu
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摘要

Structural studies of multi-protein complexes, whether by X-ray diffraction, scattering, NMR spectroscopy or electron microscopy, require stringent quality control of the component samples. The inability to produce ‘keystone’ subunits in a soluble and correctly folded form is a serious impediment to the reconstitution of the complexes. Co-expression of the components offers a valuable alternative to the expression of single proteins as a route to obtain sufficient amounts of the sample of interest. Even in cases where milligram-scale quantities of purified complex of interest become available, there is still no guarantee that good quality crystals can be obtained. At this step, protein engineering o... More

关键词

Protein complex validation for structural biology; Limited proteolysis; Crystallography; NMR; SAXS; KEOPS/EKC; MAK; RES complex; Dom34; Hbs1; Trm8; Trm81; Trm112