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Curvature induction and membrane remodeling by FAM134B reticulon homology domain assist selective ER-phagy.

Nat Commun. 2019-05; 
BhaskaraRamachandra M,GrumatiPaolo,Garcia-PardoJavier,KalayilSissy,Covarrubias-PintoAdriana,ChenWenbo,KudryashevMikhail,DikicIvan,HummerGer
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Codon Optimization The codon-optimized synthetic gene of FAM134B was produced by GenScript. Get A Quote

摘要

FAM134B/RETREG1 is a selective ER-phagy receptor that regulates the size and shape of the endoplasmic reticulum. The structure of its reticulon-homology domain (RHD), an element shared with other ER-shaping proteins, and the mechanism of membrane shaping remain poorly understood. Using molecular modeling and molecular dynamics (MD) simulations, we assemble a structural model for the RHD of FAM134B. Through MD simulations of FAM134B in flat and curved membranes, we relate the dynamic RHD structure with its two wedge-shaped transmembrane helical hairpins and two amphipathic helices to FAM134B functions in membrane-curvature induction and curvature-mediated protein sorting. FAM134B clustering, as expecte... More

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