4.7 Review

Fake It 'Till You Make It-The Pursuit of Suitable Membrane Mimetics for Membrane Protein Biophysics

期刊

出版社

MDPI
DOI: 10.3390/ijms22010050

关键词

membrane protein; lipid bilayer; membrane mimetic

资金

  1. EMBO Long-Term Fellowship [ALTF 413-2018]
  2. Swedish Research Council (Vetenskapsradet Starting Grant) [2016-04721]
  3. Knut och AliceWallenberg Foundation through aWallenberg Academy Fellowship [2016.0163]
  4. Wallenberg Centre for Molecular and Translational Medicine, University of Gothenburg, Sweden
  5. Swedish Research Council [2016-04721] Funding Source: Swedish Research Council

向作者/读者索取更多资源

Membrane proteins are evolved to reside in the hydrophobic lipid bilayers of cellular membranes, bridging different aqueous compartments separated by the membrane and dynamically interacting with their surrounding lipid environment. This interaction not only stabilizes membrane proteins, but also influences their folding, structure, and function.
Membrane proteins evolved to reside in the hydrophobic lipid bilayers of cellular membranes. Therefore, membrane proteins bridge the different aqueous compartments separated by the membrane, and furthermore, dynamically interact with their surrounding lipid environment. The latter not only stabilizes membrane proteins, but directly impacts their folding, structure and function. In order to be characterized with biophysical and structural biological methods, membrane proteins are typically extracted and subsequently purified from their native lipid environment. This approach requires that lipid membranes are replaced by suitable surrogates, which ideally closely mimic the native bilayer, in order to maintain the membrane proteins structural and functional integrity. In this review, we survey the currently available membrane mimetic environments ranging from detergent micelles to bicelles, nanodiscs, lipidic-cubic phase (LCP), liposomes, and polymersomes. We discuss their respective advantages and disadvantages as well as their suitability for downstream biophysical and structural characterization. Finally, we take a look at ongoing methodological developments, which aim for direct in-situ characterization of membrane proteins within native membranes instead of relying on membrane mimetics.

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