Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.

The Escherichia coli chemotaxis network is a model system for biological signal processing. In E. coli, transmembrane receptors responsible for signal transduction assemble into large clusters containing several thousand proteins. These sensory clusters have been observed at cell poles and future di...

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Main Authors: Derek Greenfield, Ann L McEvoy, Hari Shroff, Gavin E Crooks, Ned S Wingreen, Eric Betzig, Jan Liphardt
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-06-01
Series:PLoS Biology
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/19547746/?tool=EBI
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spelling doaj-49fd1db97573496b88357e96626b5b572021-07-02T16:28:58ZengPublic Library of Science (PLoS)PLoS Biology1544-91731545-78852009-06-0176e100013710.1371/journal.pbio.1000137Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.Derek GreenfieldAnn L McEvoyHari ShroffGavin E CrooksNed S WingreenEric BetzigJan LiphardtThe Escherichia coli chemotaxis network is a model system for biological signal processing. In E. coli, transmembrane receptors responsible for signal transduction assemble into large clusters containing several thousand proteins. These sensory clusters have been observed at cell poles and future division sites. Despite extensive study, it remains unclear how chemotaxis clusters form, what controls cluster size and density, and how the cellular location of clusters is robustly maintained in growing and dividing cells. Here, we use photoactivated localization microscopy (PALM) to map the cellular locations of three proteins central to bacterial chemotaxis (the Tar receptor, CheY, and CheW) with a precision of 15 nm. We find that cluster sizes are approximately exponentially distributed, with no characteristic cluster size. One-third of Tar receptors are part of smaller lateral clusters and not of the large polar clusters. Analysis of the relative cellular locations of 1.1 million individual proteins (from 326 cells) suggests that clusters form via stochastic self-assembly. The super-resolution PALM maps of E. coli receptors support the notion that stochastic self-assembly can create and maintain approximately periodic structures in biological membranes, without direct cytoskeletal involvement or active transport.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/19547746/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Derek Greenfield
Ann L McEvoy
Hari Shroff
Gavin E Crooks
Ned S Wingreen
Eric Betzig
Jan Liphardt
spellingShingle Derek Greenfield
Ann L McEvoy
Hari Shroff
Gavin E Crooks
Ned S Wingreen
Eric Betzig
Jan Liphardt
Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
PLoS Biology
author_facet Derek Greenfield
Ann L McEvoy
Hari Shroff
Gavin E Crooks
Ned S Wingreen
Eric Betzig
Jan Liphardt
author_sort Derek Greenfield
title Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
title_short Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
title_full Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
title_fullStr Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
title_full_unstemmed Self-organization of the Escherichia coli chemotaxis network imaged with super-resolution light microscopy.
title_sort self-organization of the escherichia coli chemotaxis network imaged with super-resolution light microscopy.
publisher Public Library of Science (PLoS)
series PLoS Biology
issn 1544-9173
1545-7885
publishDate 2009-06-01
description The Escherichia coli chemotaxis network is a model system for biological signal processing. In E. coli, transmembrane receptors responsible for signal transduction assemble into large clusters containing several thousand proteins. These sensory clusters have been observed at cell poles and future division sites. Despite extensive study, it remains unclear how chemotaxis clusters form, what controls cluster size and density, and how the cellular location of clusters is robustly maintained in growing and dividing cells. Here, we use photoactivated localization microscopy (PALM) to map the cellular locations of three proteins central to bacterial chemotaxis (the Tar receptor, CheY, and CheW) with a precision of 15 nm. We find that cluster sizes are approximately exponentially distributed, with no characteristic cluster size. One-third of Tar receptors are part of smaller lateral clusters and not of the large polar clusters. Analysis of the relative cellular locations of 1.1 million individual proteins (from 326 cells) suggests that clusters form via stochastic self-assembly. The super-resolution PALM maps of E. coli receptors support the notion that stochastic self-assembly can create and maintain approximately periodic structures in biological membranes, without direct cytoskeletal involvement or active transport.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/19547746/?tool=EBI
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