Model of SNARE-mediated membrane adhesion kinetics.

SNARE proteins are conserved components of the core fusion machinery driving diverse membrane adhesion and fusion processes in the cell. In many cases micron-sized membranes adhere over large areas before fusion. Reconstituted in vitro assays have helped isolate SNARE mechanisms in small membrane ad...

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Main Authors: Jason M Warner, Erdem Karatekin, Ben O'Shaughnessy
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-08-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2715897?pdf=render
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spelling doaj-bbf4e2e39c2c41a2bd5541f7081f06332020-11-25T01:36:30ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-08-0148e637510.1371/journal.pone.0006375Model of SNARE-mediated membrane adhesion kinetics.Jason M WarnerErdem KaratekinBen O'ShaughnessySNARE proteins are conserved components of the core fusion machinery driving diverse membrane adhesion and fusion processes in the cell. In many cases micron-sized membranes adhere over large areas before fusion. Reconstituted in vitro assays have helped isolate SNARE mechanisms in small membrane adhesion-fusion and are emerging as powerful tools to study large membrane systems by use of giant unilamellar vesicles (GUVs). Here we model SNARE-mediated adhesion kinetics in SNARE-reconstituted GUV-GUV or GUV-supported bilayer experiments. Adhesion involves many SNAREs whose complexation pulls apposing membranes into contact. The contact region is a tightly bound rapidly expanding patch whose growth velocity v(patch) increases with SNARE density Gamma(snare). We find three patch expansion regimes: slow, intermediate, fast. Typical experiments belong to the fast regime where v(patch) ~ (Gamma(snare)(2/3) depends on SNARE diffusivities and complexation binding constant. The model predicts growth velocities ~10 - 300 microm/s. The patch may provide a close contact region where SNAREs can trigger fusion. Extending the model to a simple description of fusion, a broad distribution of fusion times is predicted. Increasing SNARE density accelerates fusion by boosting the patch growth velocity, thereby providing more complexes to participate in fusion. This quantifies the notion of SNAREs as dual adhesion-fusion agents.http://europepmc.org/articles/PMC2715897?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jason M Warner
Erdem Karatekin
Ben O'Shaughnessy
spellingShingle Jason M Warner
Erdem Karatekin
Ben O'Shaughnessy
Model of SNARE-mediated membrane adhesion kinetics.
PLoS ONE
author_facet Jason M Warner
Erdem Karatekin
Ben O'Shaughnessy
author_sort Jason M Warner
title Model of SNARE-mediated membrane adhesion kinetics.
title_short Model of SNARE-mediated membrane adhesion kinetics.
title_full Model of SNARE-mediated membrane adhesion kinetics.
title_fullStr Model of SNARE-mediated membrane adhesion kinetics.
title_full_unstemmed Model of SNARE-mediated membrane adhesion kinetics.
title_sort model of snare-mediated membrane adhesion kinetics.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-08-01
description SNARE proteins are conserved components of the core fusion machinery driving diverse membrane adhesion and fusion processes in the cell. In many cases micron-sized membranes adhere over large areas before fusion. Reconstituted in vitro assays have helped isolate SNARE mechanisms in small membrane adhesion-fusion and are emerging as powerful tools to study large membrane systems by use of giant unilamellar vesicles (GUVs). Here we model SNARE-mediated adhesion kinetics in SNARE-reconstituted GUV-GUV or GUV-supported bilayer experiments. Adhesion involves many SNAREs whose complexation pulls apposing membranes into contact. The contact region is a tightly bound rapidly expanding patch whose growth velocity v(patch) increases with SNARE density Gamma(snare). We find three patch expansion regimes: slow, intermediate, fast. Typical experiments belong to the fast regime where v(patch) ~ (Gamma(snare)(2/3) depends on SNARE diffusivities and complexation binding constant. The model predicts growth velocities ~10 - 300 microm/s. The patch may provide a close contact region where SNAREs can trigger fusion. Extending the model to a simple description of fusion, a broad distribution of fusion times is predicted. Increasing SNARE density accelerates fusion by boosting the patch growth velocity, thereby providing more complexes to participate in fusion. This quantifies the notion of SNAREs as dual adhesion-fusion agents.
url http://europepmc.org/articles/PMC2715897?pdf=render
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AT erdemkaratekin modelofsnaremediatedmembraneadhesionkinetics
AT benoshaughnessy modelofsnaremediatedmembraneadhesionkinetics
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