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Computational analysis of deleterious missense mutations in aspartoacylase that cause Canavan's disease.
[canavan disease]
In
this
work
,
the
most
detrimental
missense
mutations
of
aspartoacylase
that
cause
Canavan
's
disease
were
identified
computationally
and
the
substrate
binding
efficiencies
of
those
missense
mutations
were
analyzed
.
Out
of
30
missense
mutations
,
I
-Mutant
2
.
0
,
SIFT
and
PolyPhen
programs
identified
22
variants
that
were
less
stable
,
deleterious
and
damaging
respectively
.
Subsequently
,
modeling
of
these
22
variants
was
performed
to
understand
the
change
in
their
conformations
with
respect
to
the
native
aspartoacylase
by
computing
their
root
mean
squared
deviation
(
RMSD
)
.
Furthermore
,
the
native
protein
and
the
22
mutants
were
docked
with
the
substrate
NAA
(
N-Acetyl-Aspartic
acid
)
to
explain
the
substrate
binding
efficiencies
of
those
detrimental
missense
mutations
.
Among
the
22
mutants
,
the
docking
studies
identified
that
15
mutants
caused
lower
binding
affinity
for
NAA
than
the
native
protein
.
Finally
,
normal
mode
analysis
determined
that
the
loss
of
binding
affinity
of
these
15
mutants
was
caused
by
altered
flexibility
in
the
amino
acids
that
bind
to
NAA
compared
with
the
native
protein
.
Thus
,
the
present
study
showed
that
the
majority
of
the
substrate-binding
amino
acids
in
those
15
mutants
displayed
loss
of
flexibility
,
which
could
be
the
theoretical
explanation
of
decreased
binding
affinity
between
the
mutant
aspartoacylases
and
NAA
.
Diseases
Validation
Diseases presenting
"altered flexibility in the amino acids that bind"
symptom
canavan disease
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