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With the aim of providing a deeper insight into possible mechanisms
of biological self-organization, this thesis presents new
approaches to describe the process of self-assembly and the impact
of spatial organization on the function of membrane proteins, from
a statistical physics point of view. It focuses on three important
scenarios: the assembly of membrane proteins, the collective
response of mechanosensitive channels and the function of the twin
arginine translocation (Tat) system. Using methods from equilibrium
and non-equilibrium statistical mechanics, general conclusions were
drawn that demonstrate the importance of the protein-protein
interactions. Namely, in the first part a general aggregation
dynamics model is formulated, and used to show that fragmentation
crucially affects the efficiency of the self-assembly process of
proteins. In the second part, by mapping the membrane-mediated
forces into a simplified many-body system, the dynamic and
equilibrium behaviour of interacting mechanosensitive channels is
derived, showing that protein agglomeration strongly impacts its
desired function. The final part develops a model that incorporates
both the agglomeration and transport function of the Tat system,
thereby providing a comprehensive description of this
self-organizing process.
With the aim of providing a deeper insight into possible mechanisms
of biological self-organization, this thesis presents new
approaches to describe the process of self-assembly and the impact
of spatial organization on the function of membrane proteins, from
a statistical physics point of view. It focuses on three important
scenarios: the assembly of membrane proteins, the collective
response of mechanosensitive channels and the function of the twin
arginine translocation (Tat) system. Using methods from equilibrium
and non-equilibrium statistical mechanics, general conclusions were
drawn that demonstrate the importance of the protein-protein
interactions. Namely, in the first part a general aggregation
dynamics model is formulated, and used to show that fragmentation
crucially affects the efficiency of the self-assembly process of
proteins. In the second part, by mapping the membrane-mediated
forces into a simplified many-body system, the dynamic and
equilibrium behaviour of interacting mechanosensitive channels is
derived, showing that protein agglomeration strongly impacts its
desired function. The final part develops a model that incorporates
both the agglomeration and transport function of the Tat system,
thereby providing a comprehensive description of this
self-organizing process.
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