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The consensus-based approach for gene/enzyme replacement therapies and crystallization strategies: the case of human alanine-glyoxylate aminotransferase.
[primary hyperoxaluria type 1]
Protein
stability
is
a
fundamental
issue
in
biomedical
and
biotechnological
applications
of
proteins
.
Among
these
applications
,
gene
-
and
enzyme-replacement
strategies
are
promising
approaches
to
treat
inherited
diseases
that
may
benefit
from
protein
engineering
techniques
,
even
though
these
beneficial
effects
have
been
largely
unexplored
.
In
the
present
study
we
apply
a
sequence-alignment
statistics
procedure
(
consensus-based
approach
)
to
improve
the
activity
and
stability
of
the
human
AGT
(
alanine-glyoxylate
aminotransferase
)
protein
,
an
enzyme
which
causes
PH
1
(
primary
hyperoxaluria
type
Â
I
)
upon
mutation
.
By
combining
only
five
consensus
mutations
,
we
obtain
a
variant
(
AGT
-RHEAM
)
with
largely
enhanced
in
Â
vitro
thermal
and
kinetic
stability
,
increased
activity
,
and
with
no
side
effects
on
foldability
and
peroxisomal
targeting
in
mammalian
cells
.
The
structure
of
AGT
-RHEAM
reveals
changes
at
the
dimer
interface
and
improved
electrostatic
interactions
responsible
for
increased
kinetic
stability
.
Consensus-based
variants
maintained
the
overall
protein
fold
,
crystallized
more
easily
and
improved
the
expression
as
soluble
proteins
in
two
different
systems
[
AGT
and
CIPK
24
(
CBL
-interacting
serine
/
threonine-protein
kinase
)
SOS
2
(
salt
-overly-sensitive
2
)
]
.
Thus
the
consensus-based
approach
also
emerges
as
a
simple
and
generic
strategy
to
increase
the
crystallization
success
for
hard-
to
-get
protein
targets
as
well
as
to
enhance
protein
stability
and
function
for
biomedical
applications
.
Diseases
Validation
Diseases presenting
"hyperoxaluria"
symptom
cystinuria
neonatal adrenoleukodystrophy
primary hyperoxaluria type 1
This symptom has already been validated