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Review
. 2003 Mar;28(3):137-44.
doi: 10.1016/S0968-0004(03)00026-4.

Membrane proteins: the 'Wild West' of structural biology

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Review

Membrane proteins: the 'Wild West' of structural biology

Jaume Torres et al. Trends Biochem Sci. 2003 Mar.

Erratum in

  • Trends Biochem Sci. 2003 Apr;28(4):174

Abstract

Historically, the task of determining the structure of membrane proteins has been hindered by experimental difficulties associated with their lipid-embedded domains. Here, we provide an overview of recently developed experimental and predictive tools that are changing our view of this largely unexplored territory - the 'Wild West' of structural biology. Crystallography, single-particle methods and atomic force microscopy are being used to study huge membrane proteins with increasing detail. Solid-state nuclear magnetic resonance strategies provide orientational constraints for structure determination of transmembrane (TM) alpha-helices and accurate measurements of intramolecular distances, even in very complex systems. Longer distance constraints are determined by site-directed spin-labelling electron paramagnetic resonance, but current labelling strategies still constitute some limitation. Other methods, such as site-specific infrared dichroism, enable orientational analysis of TM alpha-helices in aligned bilayers and, combined with novel computational and predictive tools that use evolutionary conservation data, are being used to analyze TM alpha-helical bundles.

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