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Formation of membrane ridges and scallops by the F-BAR protein Nervous Wreck. | LitMetric

AI Article Synopsis

  • Eukaryotic cells rely on F-BAR domain proteins, which are capable of bending membranes for shaping cellular compartments, but their varying membrane-deforming activities are not fully understood.
  • The Nwk protein's F-BAR domain forms a unique zigzag structure that enhances its ability to create distinct membrane shapes, differing from other F-BAR proteins.
  • This study reveals how structural features of the Nwk F-BAR domain contribute to its membrane sculpting abilities, highlighting a new aspect of how F-BAR proteins can induce various membrane curvatures.

Article Abstract

Eukaryotic cells are defined by extensive intracellular compartmentalization, which requires dynamic membrane remodeling. FER/Cip4 homology-Bin/amphiphysin/Rvs (F-BAR) domain family proteins form crescent-shaped dimers, which can bend membranes into buds and tubules of defined geometry and lipid composition. However, these proteins exhibit an unexplained wide diversity of membrane-deforming activities in vitro and functions in vivo. We find that the F-BAR domain of the neuronal protein Nervous Wreck (Nwk) has a novel higher-order structure and membrane-deforming activity that distinguishes it from previously described F-BAR proteins. The Nwk F-BAR domain assembles into zigzags, creating ridges and periodic scallops on membranes in vitro. This activity depends on structural determinants at the tips of the F-BAR dimer and on electrostatic interactions of the membrane with the F-BAR concave surface. In cells, Nwk-induced scallops can be extended by cytoskeletal forces to produce protrusions at the plasma membrane. Our results define a new F-BAR membrane-deforming activity and illustrate a molecular mechanism by which positively curved F-BAR domains can produce a variety of membrane curvatures. These findings expand the repertoire of F-BAR domain mediated membrane deformation and suggest that unique modes of higher-order assembly can define how these proteins sculpt the membrane.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3727933PMC
http://dx.doi.org/10.1091/mbc.E13-05-0271DOI Listing

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