378 research outputs found
Intracellular transport driven by cytoskeletal motors: General mechanisms and defects
Cells are strongly out-of-equilibrium systems driven by continuous energy
supply. They carry out many vital functions requiring active transport of
various ingredients and organelles, some being small, others being large. The
cytoskeleton, composed of three types of filaments, determines the shape of the
cell and plays a role in cell motion. It also serves as a road network for the
so-called cytoskeletal motors. These molecules can attach to a cytoskeletal
filament, perform directed motion, possibly carrying along some cargo, and then
detach. It is a central issue to understand how intracellular transport driven
by molecular motors is regulated, in particular because its breakdown is one of
the signatures of some neuronal diseases like the Alzheimer.
We give a survey of the current knowledge on microtubule based intracellular
transport. We first review some biological facts obtained from experiments, and
present some modeling attempts based on cellular automata. We start with
background knowledge on the original and variants of the TASEP (Totally
Asymmetric Simple Exclusion Process), before turning to more application
oriented models. After addressing microtubule based transport in general, with
a focus on in vitro experiments, and on cooperative effects in the
transportation of large cargos by multiple motors, we concentrate on axonal
transport, because of its relevance for neuronal diseases. It is a challenge to
understand how this transport is organized, given that it takes place in a
confined environment and that several types of motors moving in opposite
directions are involved. We review several features that could contribute to
the efficiency of this transport, including the role of motor-motor
interactions and of the dynamics of the underlying microtubule network.
Finally, we discuss some still open questions.Comment: 74 pages, 43 figure
Anomalous transport in the crowded world of biological cells
A ubiquitous observation in cell biology is that diffusion of macromolecules
and organelles is anomalous, and a description simply based on the conventional
diffusion equation with diffusion constants measured in dilute solution fails.
This is commonly attributed to macromolecular crowding in the interior of cells
and in cellular membranes, summarising their densely packed and heterogeneous
structures. The most familiar phenomenon is a power-law increase of the MSD,
but there are other manifestations like strongly reduced and time-dependent
diffusion coefficients, persistent correlations, non-gaussian distributions of
the displacements, heterogeneous diffusion, and immobile particles. After a
general introduction to the statistical description of slow, anomalous
transport, we summarise some widely used theoretical models: gaussian models
like FBM and Langevin equations for visco-elastic media, the CTRW model, and
the Lorentz model describing obstructed transport in a heterogeneous
environment. Emphasis is put on the spatio-temporal properties of the transport
in terms of 2-point correlation functions, dynamic scaling behaviour, and how
the models are distinguished by their propagators even for identical MSDs.
Then, we review the theory underlying common experimental techniques in the
presence of anomalous transport: single-particle tracking, FCS, and FRAP. We
report on the large body of recent experimental evidence for anomalous
transport in crowded biological media: in cyto- and nucleoplasm as well as in
cellular membranes, complemented by in vitro experiments where model systems
mimic physiological crowding conditions. Finally, computer simulations play an
important role in testing the theoretical models and corroborating the
experimental findings. The review is completed by a synthesis of the
theoretical and experimental progress identifying open questions for future
investigation.Comment: review article, to appear in Rep. Prog. Phy
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