Journal
EMBO REPORTS
Volume 15, Issue 11, Pages 1154-1162Publisher
WILEY-BLACKWELL
DOI: 10.15252/embr.201439267
Keywords
cryo-electron microscopy; F-BAR protein pacsin2; F-actin binding; membrane sculpting
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Funding
- European Molecular Biology Organisation, Heidelberg, Germany
- TRIL fellowship from International Centre of Theoretical Physics, Trieste, Italy
- Federal Ministry of Economy, Family and Youth through 'Laura Bassi Centre of Expertise' initiative project [253275]
- Austrian Science Fund (FWF) [P22276]
- NIH [GM081303]
- University of Vienna
- Slovenian Research Agency
- Austrian Science Fund (FWF) [I1593] Funding Source: Austrian Science Fund (FWF)
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Two mechanisms have emerged as major regulators of membrane shape: BAR domain-containing proteins, which induce invaginations and protrusions, and nuclear promoting factors, which cause generation of branched actin filaments that exert mechanical forces on membranes. While a large body of information exists on interactions of BAR proteins with membranes and regulatory proteins of the cytoskeleton, little is known about connections between these two processes. Here, we show that the F-BAR domain protein pacsin2 is able to associate with actin filaments using the same concave surface employed to bind to membranes, while some other tested N-BAR and F-BAR proteins (endophilin, CIP4 and FCHO2) do not associate with actin. This finding reveals a new level of complexity in membrane remodeling processes.
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