Localization of Protein Aggregation in Escherichia coli Is Governed by Diffusion and Nucleoid Macromolecular Crowding Effect
Authored by Hugues Berry, Anne-Sophie Coquel, Jean-Pascal Jacob, Mael Primet, Alice Demarez, Mariella Dimiccoli, Thomas Julou, Lionel Moisan, Ariel B Lindner
Date Published: 2013
DOI: 10.1371/journal.pcbi.1003038
Sponsors:
French National Research Agency (ANR)
French National Institute for Research in Computer Science and Control
Platforms:
MATLAB
Model Documentation:
Other Narrative
Mathematical description
Model Code URLs:
http://www.lri.fr/~hansen/cmaes_inmatlab.html
Abstract
Aggregates of misfolded proteins are a hallmark of many age-related
diseases. Recently, they have been linked to aging of Escherichia coli
(E. coli) where protein aggregates accumulate at the old pole region of
the aging bacterium. Because of the potential of E. coli as a model
organism, elucidating aging and protein aggregation in this bacterium
may pave the way to significant advances in our global understanding of
aging. A first obstacle along this path is to decipher the mechanisms by
which protein aggregates are targeted to specific intercellular
locations. Here, using an integrated approach based on individual-based
modeling, time-lapse fluorescence microscopy and automated image
analysis, we show that the movement of aging-related protein aggregates
in E. coli is purely diffusive (Brownian). Using single-particle
tracking of protein aggregates in live E. coli cells, we estimated the
average size and diffusion constant of the aggregates. Our results
provide evidence that the aggregates passively diffuse within the cell, with diffusion constants that depend on their size in agreement with the
Stokes-Einstein law. However, the aggregate displacements along the cell
long axis are confined to a region that roughly corresponds to the
nucleoid-free space in the cell pole, thus confirming the importance of
increased macromolecular crowding in the nucleoids. We thus used 3D
individual-based modeling to show that these three ingredients
(diffusion, aggregation and diffusion hindrance in the nucleoids) are
sufficient and necessary to reproduce the available experimental data on
aggregate localization in the cells. Taken together, our results
strongly support the hypothesis that the localization of aging-related
protein aggregates in the poles of E. coli results from the coupling of
passive diffusion-aggregation with spatially non-homogeneous
macromolecular crowding. They further support the importance of ``soft''
intracellular structuring (based on macromolecular crowding) in
diffusion-based protein localization in E. coli.
Tags
algorithms
Inheritance
bacteria
morphogenesis
Quality-control
Dna
Budding yeast
Asymmetric segregation
Cell-division
Compaction