Maria Ildiko Zavodszky
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Maria Ildiko Zavodszky
Professional Interests
We are developing a new method for
modeling protein and ligand main-chain
flexibility and show its ability to model fully
flexible molecular recognition. Flexibility
analysis of the target protein is performed
using the graph-theoretic algorithm FIRST.
The available conformational space of the
predicted flexible regions is then explored
with ROCK by random-walk sampling of the
rotatable bonds. ROCK directly identifies
and samples correlated motions by
preserving the covalent and non-covalent
bond-network of the protein. ROCK is
unique in its ability to handle coupled ring
systems and guarantees conformers with
good stereochemistry without requiring
expensive energy minimization. A
representative set of the conformational
ensemble generated this way can be used as
targets for docking with SLIDE, which
handles flexibility of protein and ligand side
chains. ROCK can be used to model not only the flexibility of proteins but also that of large
cyclic and polycyclic ligands. This combined approach is used to perform fully flexible docking.
Several questions can be addressed using this approach: (1) How much flexibility of the
interacting molecules is tolerated without hindering molecular recognition? (2) How does ligand
binding change the flexibility of the protein? (3) How are flexibility changes propagated from
one part of the protein to another?
more flexible more rigid