Protein crowding and lipid complexity influence the nanoscale dynamic organization of ion channels in cell membranes

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作者
Anna L. Duncan
Tyler Reddy
Heidi Koldsø
Jean Hélie
Philip W. Fowler
Matthieu Chavent
Mark S. P. Sansom
机构
[1] University of Oxford,Department of Biochemistry
[2] T-6,undefined
[3] MS K710,undefined
[4] Los Alamos National Laboratory,undefined
[5] D. E. Shaw Research,undefined
[6] 120 W 45th St.,undefined
[7] Semmle,undefined
[8] Blue Boar Court,undefined
[9] 9 Alfred St,undefined
[10] Nuffield Department of Medicine,undefined
[11] University of Oxford,undefined
[12] John Radcliffe Hospital,undefined
[13] IPBS-CNRS,undefined
来源
Scientific Reports | / 7卷
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摘要
Cell membranes are crowded and complex environments. To investigate the effect of protein-lipid interactions on dynamic organization in mammalian cell membranes, we have performed coarse-grained molecular dynamics simulations containing >100 copies of an inwardly rectifying potassium (Kir) channel which forms specific interactions with the regulatory lipid phosphatidylinositol 4,5-bisphosphate (PIP2). The tendency of protein molecules to cluster has the effect of organizing the membrane into dynamic compartments. At the same time, the diversity of lipids present has a marked effect on the clustering behavior of ion channels. Sub-diffusion of proteins and lipids is observed. Protein crowding alters the sub-diffusive behavior of proteins and lipids such as PIP2 which interact tightly with Kir channels. Protein crowding also affects bilayer properties, such as membrane undulations and bending rigidity, in a PIP2-dependent manner. This interplay between the diffusion and the dynamic organization of Kir channels may have important implications for channel function.
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