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Literature DB >> 18550820

Transmembrane segment enhanced labeling as a tool for the backbone assignment of alpha-helical membrane proteins.

Sina Reckel¹, Solmaz Sobhanifar, Birgit Schneider, Friederike Junge, Daniel Schwarz, Florian Durst, Frank Löhr, Peter Güntert, Frank Bernhard, Volker Dötsch.

Abstract

Recent advances in cell-free expression protocols have opened a new avenue toward high-resolution structural investigations of membrane proteins by x-ray crystallography and NMR spectroscopy. One of the biggest challenges for liquid-state NMR-based structural investigations of membrane proteins is the significant peak overlap in the spectra caused by large line widths and limited chemical shift dispersion of alpha-helical proteins. Contributing to the limited chemical shift dispersion is the fact that approximately 60% of the amino acids in transmembrane regions consist of only six different amino acid types. This principle disadvantage, however, can be exploited to aid in the assignment of the backbone resonances of membrane proteins; by (15)N/(13)C-double-labeling of these six amino acid types, sequential connectivities can be obtained for large stretches of the transmembrane segments where number and length of stretches consisting exclusively of these six amino acid types are enhanced compared with the remainder of the protein. We show by experiment as well as by statistical analysis that this labeling scheme provides a large number of sequential connectivities in transmembrane regions and thus constitutes a tool for the efficient assignment of membrane protein backbone resonances.

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Year: 2008 PMID： 18550820 PMCID： PMC2448825 DOI： 10.1073/pnas.0710843105

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

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