THESIS
2015
xii, 41 pages : illustrations (chiefly color) ; 30 cm
Abstract
Argonaute (Ago) proteins and microRNAs (miRNA) are central components in RNA
interference, which is a key cellular mechanism for sequence-specific gene silencing. Despite
intensive studies, molecular mechanisms of how Ago recognizes miRNA remain largely elusive.
In this study, we propose a two-step mechanism for this molecular recognition: selective binding
followed by structural re-arrangement. Our model is based on the results of a combination of
Markov State Models (MSMs), large-scale protein-RNA docking, and molecular dynamics (MD)
simulations. Using MSMs, we identify an open state of apo human Ago-2 in fast equilibrium
with partially open and closed states. Conformations in this open state are featured by their
largely exposed binding grooves that can geometrically accommod...[
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Argonaute (Ago) proteins and microRNAs (miRNA) are central components in RNA
interference, which is a key cellular mechanism for sequence-specific gene silencing. Despite
intensive studies, molecular mechanisms of how Ago recognizes miRNA remain largely elusive.
In this study, we propose a two-step mechanism for this molecular recognition: selective binding
followed by structural re-arrangement. Our model is based on the results of a combination of
Markov State Models (MSMs), large-scale protein-RNA docking, and molecular dynamics (MD)
simulations. Using MSMs, we identify an open state of apo human Ago-2 in fast equilibrium
with partially open and closed states. Conformations in this open state are featured by their
largely exposed binding grooves that can geometrically accommodate miRNA as indicated in our
protein-RNA docking studies. miRNA may then selectively bind to these open conformations.
Upon the initial binding, the complex may perform further structural re-arrangement as shown in
our MD simulations and eventually reach the stable binary complex structure. Our results
provide novel insights in Ago-miRNA recognition mechanisms and our methodology holds great
potential to be widely applied in the studies of other important molecular recognition systems.
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