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Lateral sorting in model membranes by cholesterol-mediated hydrophobic matching.

Proc Natl Acad Sci U S A.. 2011-10; 
Kaiser HJ, Or?owski A, Róg T, Nyholm TK, Chai W, Feizi T, Lingwood D, Vattulainen I, Simons K. Max Planck Institute for Molecular Cell Biology and Genetics, Pfotenhauerstr 108, 01307 Dresden, Germany.
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摘要

Theoretical studies predict hydrophobic matching between transmembrane domains of proteins and bilayer lipids to be a physical mechanism by which membranes laterally self-organize. We now experimentally study the direct consequences of mismatching of transmembrane peptides of different length with bilayers of different thicknesses at the molecular level. In both model membranes and simulations we show that cholesterol critically constrains structural adaptations at the peptide-lipid interface under mismatch. These constraints translate into a sorting potential and lead to selective lateral segregation of peptides and lipids according to their hydrophobic length.

关键词

mattress model;membrane domain;proteinClipid interaction;self-assembly;annular lipid