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CryoEM architecture of a native stretch-sensitive membrane microdomain
by
Zou, Luoming
, Vanni, Stefano
, Loewith, Robbie
, Desfosses, Ambroise
, Alba, Josephine
, Roux, Aurélien
, Kefauver, Jennifer M.
, Hakala, Markku
, Espadas, Javier
, Estrozi, Leandro F.
, Tettamanti, Maria G.
in
Biophysics
2023
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CryoEM architecture of a native stretch-sensitive membrane microdomain
by
Zou, Luoming
, Vanni, Stefano
, Loewith, Robbie
, Desfosses, Ambroise
, Alba, Josephine
, Roux, Aurélien
, Kefauver, Jennifer M.
, Hakala, Markku
, Espadas, Javier
, Estrozi, Leandro F.
, Tettamanti, Maria G.
in
Biophysics
2023
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Do you wish to request the book?
CryoEM architecture of a native stretch-sensitive membrane microdomain
by
Zou, Luoming
, Vanni, Stefano
, Loewith, Robbie
, Desfosses, Ambroise
, Alba, Josephine
, Roux, Aurélien
, Kefauver, Jennifer M.
, Hakala, Markku
, Espadas, Javier
, Estrozi, Leandro F.
, Tettamanti, Maria G.
in
Biophysics
2023
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CryoEM architecture of a native stretch-sensitive membrane microdomain
Paper
CryoEM architecture of a native stretch-sensitive membrane microdomain
2023
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Overview
Biological membranes are partitioned into functional zones containing specific lipids and proteins, termed membrane microdomains. Their composition and organization remain controversial owing to a paucity of techniques that can visualize lipids in situ without disrupting their native behavior1,2. The yeast eisosome, a membrane compartment scaffolded by the BAR-domain proteins Pil1 and Lsp1, senses and responds to mechanical stress by flattening and releasing sequestered factors3–7. Here, we isolated native eisosomes as helical filaments of Pil1/Lsp1 lattice bound to plasma membrane lipids and solved their structures by helical reconstruction. We observe remarkable organization within the lipid bilayer density from which we could assign headgroups of PI(4,5)P2 and phosphatidylserine bound to Pil1/Lsp1 and a pattern of membrane voids, signatures of sterols, beneath an amphipathic helix. We verified these assignments using in vitro reconstitutions and molecular dynamics simulations. 3D variability analysis of the native eisosomes revealed a dynamic stretching of the Pil1/Lsp1 lattice that affects functionally important lipid sequestration, supporting a mechanism in which membrane stretching liberates lipids otherwise anchored by the Pil1/Lsp1 coat. Our results provide mechanistic insight into how eisosome BAR-domain proteins create a mechanosensitive membrane microdomain and, more globally, resolve long-standing controversies about the architecture and nature of lipid microdomains.
Publisher
Cold Spring Harbor Laboratory
Subject
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