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Polymers and Self Assembly: From Biology to Nanomaterials

Monday Speaker Abstracts

How to Build a Septin Filament

Richard Garratt

.

University of Sao Paulo, Brazil

Monomeric septins polymerize into membrane associating hetero-filaments which are involved

in membrane remodelling events and barrier formation. The human genome includes 13 genes

coding for septins that can be divided into four different groups leading to hundreds of different

possible combinations for hetero-filament formation. The filaments themselves are stabilized via

two different types of inter-subunit interface (G and NC) which alternate along the main axis. In

an attempt to understand the rules which underpin spontaneous filament assembly we have used

crystallographic approaches allied to a series of complementary biophysical techniques. In

essence, the problem of self assembly can be reduced to understanding the structural basis for

specificity at each of the five different interfaces which appear between individual septins along

a filament composed of four different monomers. We demonstrate that a C-terminal coiled-coil

domain is important for the recognition of partner septins at one of the NC interfaces as well as

contributing to the formation of higher-order assemblies. Studies of septins bound to both GTP

and GDP show that the two types of interface are interconnected as a result of an unexpected

shift in the register of a central β-sheet strand on GTP hydrolysis. This is predicted to affect

membrane binding. In summary, our data suggest mechanisms for self-assembly, filament

bundling and the importance of GTP binding and hydrolysis for membrane association.

phosphorylated by S-phase cyclin-Cdk1-Cks1. The processivity is modulated by

phosphorylation/dephosphorylation of a priming site and a diversional site by two kinases and a

phosphatase of stress pathways. Both the priming site and the diversional site compete for

binding to Cks1. This mechanism demonstrates how external signals can be integrated into the

Cdk1 control system via multi-branched signal-processing modules based on multisite

phosphorylation networks. Such transistor-like modules are possibly ubiquitous and could

regulate many cellular events.

The Varied Geometries of ParM Cytomotive Filaments in Bacterial Plasmid Segregation

Robert Robinson

Institute for Molecular & Cell Biology, Singapore

No abstract