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  • Molecular basis for SNX-BAR-mediated assembly of distinct endosomal sorting tubules.

Molecular basis for SNX-BAR-mediated assembly of distinct endosomal sorting tubules.

The EMBO journal (2012-10-23)
Jan R T van Weering, Richard B Sessions, Colin J Traer, Daniel P Kloer, Vikram K Bhatia, Dimitrios Stamou, Sven R Carlsson, James H Hurley, Peter J Cullen
ABSTRACT

Sorting nexins (SNXs) are regulators of endosomal sorting. For the SNX-BAR subgroup, a Bin/Amphiphysin/Rvs (BAR) domain is vital for formation/stabilization of tubular subdomains that mediate cargo recycling. Here, by analysing the in vitro membrane remodelling properties of all 12 human SNX-BARs, we report that some, but not all, can elicit the formation of tubules with diameters that resemble sorting tubules observed in cells. We reveal that SNX-BARs display a restricted pattern of BAR domain-mediated dimerization, and by resolving a 2.8 Å structure of a SNX1-BAR domain homodimer, establish that dimerization is achieved in part through neutralization of charged residues in the hydrophobic BAR-dimerization interface. Membrane remodelling also requires functional amphipathic helices, predicted to be present in all SNX-BARs, and the formation of high order SNX-BAR oligomers through selective 'tip-loop' interactions. Overall, the restricted and selective nature of these interactions provide a molecular explanation for how distinct SNX-BAR-decorated tubules are nucleated from the same endosomal vacuole, as observed in living cells. Our data provide insight into the molecular mechanism that generates and organizes the tubular endosomal network.

MATERIALS
Product Number
Brand
Product Description

Avanti
Brain Extract Total, Avanti Research - A Croda Brand
Avanti
Brain Extract Total, Avanti Research - A Croda Brand
Sigma-Aldrich
Brain Extract from bovine brain, Type I, Folch Fraction I
Sigma-Aldrich
GeneJuice® Transfection Reagent, Non-lipid based chemical transfection reagent optimized for maximum transfection efficiency, ease-of-use, and minimal cytotoxicity on a wide variety of mammalian cells.