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Publication Abstract from PubMed

Sulfur is critical for the correct structure and proper function of proteins. Yet, lacking a sensitive enough isotope, nuclear magnetic resonance (NMR) experiments are unable to deliver for sulfur in proteins the usual wealth of chemical, dynamic, and structural information. This limitation can be circumvented by substituting sulfur with selenium, which has similar physicochemical properties and minimal impact on protein structures but possesses an NMR compatible isotope ((77)Se). Here we exploit the sensitivity of (77)Se NMR to the nucleus' chemical milieu and use selenomethionine as a probe for its proteinaceous environment. However, such selenium NMR spectra of proteins currently resist a reliable interpretation because systematic connections between variations of system variables and changes in (77)Se NMR parameters are still lacking. To start narrowing this knowledge gap, we report here on a biological (77)Se magnetic resonance data bank based on a systematically designed library of GB1 variants in which a single selenomethionine was introduced at different locations within the protein. We recorded the resulting isotropic (77)Se chemical shifts and relaxation times for six GB1 variants by solution-state (77)Se NMR. For four of the GB1 variants we were also able to determine the chemical shift anisotropy tensor of SeM by solid-state (77)Se NMR. To enable interpretation of the NMR data, the structures of five of the GB1 variants were solved by X-ray crystallography to a resolution of 1.2 A, allowing us to unambiguously determine the conformation of the selenomethionine. Finally, we combine our solution- and solid-state NMR data with the structural information to arrive at general insights regarding the execution and interpretation of (77)Se NMR experiments that exploit selenomethionine to probe proteins.

(77)Se NMR Probes the Protein Environment of Selenomethionine.,Chen Q, Xu S, Lu X, Boeri MV, Pepelyayeva Y, Diaz EL, Soni SD, Allaire M, Forstner MB, Bahnson BJ, Rozovsky S J Phys Chem B. 2020 Jan 7. doi: 10.1021/acs.jpcb.9b07466. PMID:31846581^[1]

From MEDLINE®/PubMed®, a database of the U.S. National Library of Medicine.