Amphipathic motifs in BAR domains are essential for membrane curvature sensing
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Amphipathic motifs in BAR domains are essential for membrane curvature sensing. / Bhatia, Vikram K; Madsen, Kenneth L; Bolinger, Pierre-Yves; Kunding, Andreas; Hedegård, Per; Gether, Ulrik; Stamou, Dimitrios.
In: EMBO Journal, Vol. 28, No. 21, 2009, p. 3303-3314.Research output: Contribution to journal › Journal article › Research › peer-review
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TY - JOUR
T1 - Amphipathic motifs in BAR domains are essential for membrane curvature sensing
AU - Bhatia, Vikram K
AU - Madsen, Kenneth L
AU - Bolinger, Pierre-Yves
AU - Kunding, Andreas
AU - Hedegård, Per
AU - Gether, Ulrik
AU - Stamou, Dimitrios
N1 - Keywords: Acyltransferases; Animals; Brain Chemistry; Cattle; Gene Expression; Lipid Bilayers; Liposomes; Membrane Proteins; Microscopy, Fluorescence; Models, Biological; Nerve Tissue Proteins; Protein Binding; Protein Structure, Secondary; Protein Structure, Tertiary; Rats
PY - 2009
Y1 - 2009
N2 - BAR (Bin/Amphiphysin/Rvs) domains and amphipathic alpha-helices (AHs) are believed to be sensors of membrane curvature thus facilitating the assembly of protein complexes on curved membranes. Here, we used quantitative fluorescence microscopy to compare the binding of both motifs on single nanosized liposomes of different diameters and therefore membrane curvature. Characterization of members of the three BAR domain families showed surprisingly that the crescent-shaped BAR dimer with its positively charged concave face is not able to sense membrane curvature. Mutagenesis on BAR domains showed that membrane curvature sensing critically depends on the N-terminal AH and furthermore that BAR domains sense membrane curvature through hydrophobic insertion in lipid packing defects and not through electrostatics. Consequently, amphipathic motifs, such as AHs, that are often associated with BAR domains emerge as an important means for a protein to sense membrane curvature. Measurements on single liposomes allowed us to document heterogeneous binding behaviour within the ensemble and quantify the influence of liposome polydispersity on bulk membrane curvature sensing experiments. The latter results suggest that bulk liposome-binding experiments should be interpreted with great caution.
AB - BAR (Bin/Amphiphysin/Rvs) domains and amphipathic alpha-helices (AHs) are believed to be sensors of membrane curvature thus facilitating the assembly of protein complexes on curved membranes. Here, we used quantitative fluorescence microscopy to compare the binding of both motifs on single nanosized liposomes of different diameters and therefore membrane curvature. Characterization of members of the three BAR domain families showed surprisingly that the crescent-shaped BAR dimer with its positively charged concave face is not able to sense membrane curvature. Mutagenesis on BAR domains showed that membrane curvature sensing critically depends on the N-terminal AH and furthermore that BAR domains sense membrane curvature through hydrophobic insertion in lipid packing defects and not through electrostatics. Consequently, amphipathic motifs, such as AHs, that are often associated with BAR domains emerge as an important means for a protein to sense membrane curvature. Measurements on single liposomes allowed us to document heterogeneous binding behaviour within the ensemble and quantify the influence of liposome polydispersity on bulk membrane curvature sensing experiments. The latter results suggest that bulk liposome-binding experiments should be interpreted with great caution.
U2 - 10.1038/emboj.2009.261
DO - 10.1038/emboj.2009.261
M3 - Journal article
C2 - 19816406
VL - 28
SP - 3303
EP - 3314
JO - E M B O Journal
JF - E M B O Journal
SN - 0261-4189
IS - 21
ER -
ID: 21593567