Advanced solid-state NMR techniques for characterization of membrane protein structure and dynamics: application to Anabaena Sensory Rhodopsin.

J Magn Reson

Department of Physics and Biophysics Interdepartmental Group, University of Guelph, Guelph, Ontario N1G 2W1, Canada. Electronic address:

Published: April 2015

AI Article Synopsis

  • Solid-state NMR (SSNMR) is a key tool for studying membrane proteins (MPs), revealing high-resolution structures and models of α-helical MPs through recent advancements in techniques and instrumentation.
  • Challenges in determining MP structures include the need to maintain lipid presence, the predominance of specific secondary structures, differing dynamics, and local disorganization in loop regions.
  • This article highlights efforts to uncover the structure and dynamics of Anabaena Sensory Rhodopsin, a 7-transmembrane protein, and discusses various SSNMR methods suitable for studying this protein and others similar to G-protein coupled receptors.

Article Abstract

Studies of the structure, dynamics, and function of membrane proteins (MPs) have long been considered one of the main applications of solid-state NMR (SSNMR). Advances in instrumentation, and the plethora of new SSNMR methodologies developed over the past decade have resulted in a number of high-resolution structures and structural models of both bitopic and polytopic α-helical MPs. The necessity to retain lipids in the sample, the high proportion of one type of secondary structure, differential dynamics, and the possibility of local disorder in the loop regions all create challenges for structure determination. In this Perspective article we describe our recent efforts directed at determining the structure and functional dynamics of Anabaena Sensory Rhodopsin, a heptahelical transmembrane (7TM) protein. We review some of the established and emerging methods which can be utilized for SSNMR-based structure determination, with a particular focus on those used for ASR, a bacterial protein which shares its 7TM architecture with G-protein coupled receptors.

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Source
http://dx.doi.org/10.1016/j.jmr.2014.11.017DOI Listing

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