27,395 research outputs found
Computational studies of biomembrane systems: Theoretical considerations, simulation models, and applications
This chapter summarizes several approaches combining theory, simulation and
experiment that aim for a better understanding of phenomena in lipid bilayers
and membrane protein systems, covering topics such as lipid rafts, membrane
mediated interactions, attraction between transmembrane proteins, and
aggregation in biomembranes leading to large superstructures such as the light
harvesting complex of green plants. After a general overview of theoretical
considerations and continuum theory of lipid membranes we introduce different
options for simulations of biomembrane systems, addressing questions such as:
What can be learned from generic models? When is it expedient to go beyond
them? And what are the merits and challenges for systematic coarse graining and
quasi-atomistic coarse grained models that ensure a certain chemical
specificity
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Modeling membrane nanotube morphology: the role of heterogeneity in composition and material properties.
Membrane nanotubes are dynamic structures that may connect cells over long distances. Nanotubes are typically thin cylindrical tubes, but they may occasionally have a beaded architecture along the tube. In this paper, we study the role of membrane mechanics in governing the architecture of these tubes and show that the formation of bead-like structures along the nanotubes can result from local heterogeneities in the membrane either due to protein aggregation or due to membrane composition. We present numerical results that predict how membrane properties, protein density, and local tension compete to create a phase space that governs the morphology of a nanotube. We also find that there exists a discontinuity in the energy that impedes two beads from fusing. These results suggest that the membrane-protein interaction, membrane composition, and membrane tension closely govern the tube radius, number of beads, and the bead morphology
Lipid-protein interaction induced domains: kinetics and conformational changes in multicomponent vesicles
The spatio-temporal organization of proteins and the associated morphological
changes in membranes are of importance in cell signaling. Several mechanisms
that promote the aggregation of proteins at low cell surface concentrations
have been investigated in the past. We show, using Monte Carlo simulations,
that the affinity of proteins for specific lipids can hasten its aggregation
kinetics. The lipid membrane is modeled as a dynamically triangulated surface
with the proteins defined as in-plane fields at the vertices. We show that,
even at low protein concentrations, strong lipid-protein interactions can
result in large protein clusters indicating a route to lipid mediated signal
amplification. At high protein concentrations the domains form buds similar to
that seen in lipid-lipid interaction induced phase separation. Protein
interaction induced domain budding is suppressed when proteins act as
anisotropic inclusions and exhibit nematic orientational order. The kinetics of
protein clustering and resulting conformational changes are shown to be
significantly different for the isotropic and anisotropic curvature inducing
proteins.Comment: 22pages, 12 figure
Dynamin recruitment by clathrin coats: a physical step?
Recent structural findings have shown that dynamin, a cytosol protein playing
a key-role in clathrin-mediated endocytosis, inserts partly within the lipid
bilayer and tends to self-assemble around lipid tubules. Taking into account
these observations, we make the hypothesis that individual membrane inserted
dynamins imprint a local cylindrical curvature to the membrane. This imprint
may give rise to long-range mechanical forces mediated by the elasticity of the
membrane. Calculating the resulting many-body interaction between a collection
of inserted dynamins and a membrane bud, we find a regime in which the dynamins
are elastically recruited by the bud to form a collar around its neck, which is
reminiscent of the actual process preempting vesicle scission. This physical
mechanism might therefore be implied in the recruitment of dynamins by clathrin
coats.Comment: 11 pages, 6 figures, to appear in C.R.A.S. ser II
Cooperative Gating and Spatial Organization of Membrane Proteins through Elastic Interactions
Biological membranes are elastic media in which the presence of a
transmembrane protein leads to local bilayer deformation. The energetics of
deformation allow two membrane proteins in close proximity to influence each
other's equilibrium conformation via their local deformations, and spatially
organize the proteins based on their geometry. We use the mechanosensitive
channel of large conductance (MscL) as a case study to examine the implications
of bilayer-mediated elastic interactions on protein conformational statistics
and clustering. The deformations around MscL cost energy on the order of 10 kT
and extend ~3nm from the protein edge, as such elastic forces induce
cooperative gating and we propose experiments to measure these effects.
Additionally, since elastic interactions are coupled to protein conformation,
we find that conformational changes can severely alter the average separation
between two proteins. This has important implications for how conformational
changes organize membrane proteins into functional groups within membranes.Comment: 12 pages, 6 figures, 63 references, submitted to PLoS Computational
Biolog
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