Scientists
at The Scripps Research Institute have determined the three-dimensional atomic
structure of a human protein that is centrally involved in regulating the
activities of cells. Knowing the precise structure of this protein paves the way
for scientists to understand a process known as RNA-silencing and to harness it
to treat diseases.
"Biologists have known about RNA-silencing for
only a decade or so, but it's already clear that there's an enormous untapped
potential here for new therapies," said Ian MacRae, an assistant professor
at Scripps Research and senior author of the new report.
The new report, which appeared on April 26, 2012 in
the journal Science's advance online publication, Science Express, focuses on
Argonaute2. This protein can effectively "silence" a gene by
intercepting and slicing the gene's RNA transcripts before they are translated
into working proteins.
Interception and Destruction of Messages
When a gene that codes for a protein is active in a
cell, its information is transcribed from DNA form into lengths of nucleic acid
called messenger RNA (mRNA). If all goes well, these coded mRNA signals make
their way to the cell's protein-factories, which use them as templates to
synthesize new proteins. RNA-silencing, also called RNA interference (RNAi), is
the interception and destruction of these messages -- and as such, is a
powerful and specific regulator of cell activity, as well as a strong defender
against viral genes.
The silencing process requires not only an Argonaute
protein but also a small length of guide RNA, known as a short-interfering RNA
or microRNA. The guide RNA fits into a slot on Argonaute and serves as a target
recognition device. Like a coded strip of VelcroTM, it latches onto a specific
mRNA target whose sequence is the chemical mirror image, or
"complement," of its own -- thus bringing Argonaute into contact with
its doomed prey.
Argonaute2 is not the only type of human Argonaute
protein, but it seems to be the only one capable of destroying target RNA directly.
"If the guide RNA is completely complementary to the target RNA,
Argonaute2 will cleave the mRNA, and that will elicit the degradation of the
fragments and the loss of the genetic message," said Nicole Schirle, the
graduate student in MacRae's laboratory who was lead author of the paper.
Aimed at disease-causing genes or even a cell's own
overactive guide RNAs, RNA-silencing could be a powerful therapeutic weapon. In
principle, one needs only to inject target-specific guide RNAs, and these will
link up with Argonaute proteins in cells to find and destroy the target RNAs.
Scientists have managed to do this successfully with relatively accessible
target cells, such as in the eye. But they have found it difficult to develop
guide RNAs that can get from the bloodstream into distant tissues and still
function.
"You have to modify the guide RNA, in some way
to get it through the blood and into cells, but as soon as you start modifying
it, you disrupt its ability to interact with Argonaute," said MacRae. Knowing
the precise structure of Argonaute should enable researchers to clear this
hurdle by designing better guide RNA.
More Points for Manipulation
Previous structural studies have focused mostly on
Argonaute proteins from bacteria and other lower organisms, which have key
differences from their human counterparts. Schirle was able to produce the
comparatively large and complex human Argonaute2 and to manipulate it into
forming crystals for X-ray crystallography analysis -- a feat that structural
biologists have wanted to achieve for much of the past decade. "It was
just excellent and diligent crystallography on her part," said MacRae.
The team's analysis of Argonaute2's structure
revealed that it has the same basic set of working parts as bacterial Argonaute
proteins, except that they are arranged somewhat differently. Also, key parts
of Argonaute2 have extra loops and other structures, not seen on bacterial
versions, which may play roles in binding to guide RNA. Finally, Argonaute2 has
what appear to be binding sites for additional co-factor proteins that are
thought to perform other destructive operations on the target mRNA.
"Basically, this Argonaute protein is more
sophisticated than its bacterial cousins; it has more bells and whistles, which
give us more points for manipulation. With this structure solved, we no longer
need to use the prokaryotic structures to guess at what human Argonaute
proteins look like," MacRae said.
He and Schirle and others in the lab now are
analyzing the functions of Argonaute2's substructures, as well as looking for
ways to design better therapeutic guide RNAs.
"Now with the structural data, we can see what
synthetic guide RNAs will work with Argonaute and what won't," MacRae
said. "We might even be able to make guide RNAs that can outcompete
natural ones."
The research was funded by the National Institute of
General Medical Sciences, part of the National Institutes of Health.
ScienceDaily
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