Assignment Strategies for Large Proteins by Magic-Angle Spinning NMR: The 21-kDa Disulfide-Bond-Forming Enzyme DsbA

Sperling, Lindsay J.; Berthold, Deborah A.; Sasser, Terry; Jeisy-Scott, Victoria; Rienstra, Chad M.

doi:10.1016/j.jmb.2010.04.012

Cited by 65 publications

(75 citation statements)

References 84 publications

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“…The sequential resonance assignment is the basis of all further ssNMR spectroscopic studies (Pauli et al 2001;Schuetz et al 2010;Shi et al 2009;Sperling et al 2010). An important step was the development of efficient 15 N-13 C SPECIFIC-CP transfer which is widely used today (Baldus et al 1998).…”

Section: Introductionmentioning

confidence: 99%

BSH-CP based 3D solid-state NMR experiments for protein resonance assignment

et al. 2014

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We have recently presented band-selective homonuclear cross-polarization (BSH-CP) as an efficient method for CO-CA transfer in deuterated as well as protonated solid proteins. Here we show how the BSH-CP CO-CA transfer block can be incorporated in a set of threedimensional (3D) solid-state NMR (ssNMR) pulse schemes tailored for resonance assignment of proteins at high static magnetic fields and moderate magic-angle spinning rates. Due to the achieved excellent transfer efficiency of 33 % for BSH-CP, a complete set of 3D spectra needed for unambiguous resonance assignment could be rapidly recorded within 1 week for the model protein ubiquitin. Thus we expect that BSH-CP could replace the typically used CO-CA transfer schemes in well-established 3D ssNMR approaches for resonance assignment of solid biomolecules.

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Section: Introductionmentioning

confidence: 99%

BSH-CP based 3D solid-state NMR experiments for protein resonance assignment

et al. 2014

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“…The resonance assignment of proteins with more than 200 residues is now feasible using uniformly labeled samples, with the 33 kDa C-terminal domain of the yeast prion Ure2p (285 residues) presently being the largest system with extensive de novo assignments in the solid state . Other large systems with extensive resonance assignments include HET-s(1-227) (Schuetz et al 2010) and DsbA (223 residues) (Sperling et al 2010;Shi et al 2010). An important limitation is the need to acquire data showing a sufficiently high signal-to-noise ratio of the relevant cross peaks for each of the 3D spectra required for the assignment process (Schuetz et al 2010;Habenstein et al 2011).…”

Section: Introductionmentioning

confidence: 99%

Properties of the DREAM scheme and its optimization for application to proteins

et al. 2012

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The DREAM scheme is an efficient adiabatic homonuclear polarization-transfer method suitable for multi-dimensional experiments in biomolecular solid-state NMR. The bandwidth and dynamics of the polarization transfer in the DREAM experiment depend on a number of experimental and spin-system parameters. In order to obtain optimal results, the dependence of the cross-peak intensity on these parameters needs to be understood and carefully controlled. We introduce a simplified model to semi-quantitatively describe the polarization-transfer patterns for the relevant spin systems. Numerical simulations for all natural amino acids (except tryptophane) show the dependence of the cross-peak intensities as a function of the radio-frequency-carrier position. This dependency can be used as a guide to select the desired conditions in protein spectroscopy. Practical guidelines are given on how to set up a DREAM experiment for optimized Cα/Cβ transfer, which is important in sequential assignment experiments.

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“…This method creates proteins which are alternately labeled with 13 C patterns which do not contain adjacent 13 C labels in most amino acids [29]. This improves the resolution of individual resonances due to the suppression of many one-bond J-couplings, simplifies the overall spectra due to the reduction of the number of resonances, and specifically facilitates the assignment of the aromatic side chains [30,31]. These benefits were all observed in ASR, and experiments preformed on samples grown on alternately labeled glycerols allowed us to extend the assignments to a total of 206 of the 229 residues [32].…”

Section: Spectroscopic Assignmentsmentioning

confidence: 99%