Journal
MAGNETIC RESONANCE IN CHEMISTRY
Volume 44, Issue -, Pages S177-S184Publisher
JOHN WILEY & SONS LTD
DOI: 10.1002/mrc.1825
Keywords
fast NMR; hydrogen exchange; NOE; proteins; proteomics; proton spin diffusion
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Structure elucidation of proteins by either NMR or X-ray crystallography often requires the screening of a large number of samples for promising protein constructs and optimum solution conditions. For large-scale screening of protein samples in solution, robust methods are needed that allow a rapid assessment of the folding of a polypeptide under diverse sample conditions. Here we present HET-SOFAST NMR, a highly sensitive new method for semi-quantitative characterization of the structural compactness and heterogeneity of polypeptide chains in solution. On the basis of one-dimensional H-1 HET-SOFAST NMR data, obtained on well-folded, molten globular, partially- and completely unfolded proteins, we define empirical thresholds that can be used as quantitative benchmarks for protein compactness. For N-15-enriched protein samples, two-dimensional H-1-N-15 HET-SOFAST correlation spectra provide site-specific information about the structural heterogeneity along the polypeptide chain. Copyright (C) 2006 John Wiley & Sons, Ltd.
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