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Different altered pattern expression of genes related to apoptosis in isolated methylmalonic aciduria cblB type and combined with homocystinuria cblC type.
[homocystinuria without methylmalonic aciduria]
An
increased
reactive
oxygen
species
(
ROS
)
production
and
apoptosis
rate
have
been
associated
with
several
disorders
involved
in
cobalamin
metabolism
,
including
isolated
methylmalonic
aciduria
(
MMA
)
cblB
type
and
MMA
combined
with
homocystinuria
(
MMAHC
)
cblC
type
.
Given
the
relevance
of
p
38
and
JNK
kinases
in
stress-response
,
their
activation
in
fibroblasts
from
a
spectrum
of
patients
(
mut
,
cblA
,
cblB
,
cblC
and
cblE
)
was
analyzed
revealing
an
increased
expression
of
the
phosphorylated-forms
,
specially
in
cblB
and
cblC
cell
lines
that
presented
the
highest
ROS
and
apoptosis
levels
.
To
gain
further
insight
into
the
molecular
mechanisms
responsible
for
the
enhanced
apoptotic
process
observed
in
cblB
and
cblC
fibroblasts
,
we
evaluated
the
expression
pattern
of
84
apoptosis-related
genes
by
quantitative
real-time
PCR
.
An
elevated
number
of
pro-apoptotic
genes
were
overexpressed
in
cblC
cells
showing
a
higher
rate
of
apoptosis
compared
to
cblB
and
control
samples
.
Additionally
,
apoptosis
appears
to
be
mainly
triggered
through
the
extrinsic
pathway
in
cblC
,
while
the
intrinsic
pathway
was
primarily
activated
in
cblB
cells
.
The
differences
observed
regarding
the
apoptosis
rate
and
preferred
pathway
between
cblB
and
cblC
patients
,
who
both
built
up
methylmalonic
acid
,
might
be
explained
by
the
accumulated
homocysteine
in
the
cblC
group
.
The
loss
of
MMACHC
function
in
cblC
patients
might
be
partially
responsible
for
the
oxidative
stress
and
apoptosis
processes
observed
in
these
cell
lines
.
Our
results
suggest
that
ROS
production
may
represent
a
genetic
modifier
of
the
phenotype
and
support
the
potential
of
using
antioxidants
as
a
novel
therapeutic
strategy
to
improve
the
severe
neurological
outcome
of
these
rare
diseases
.
Diseases
Validation
Diseases presenting
"elevated number"
symptom
homocystinuria without methylmalonic aciduria
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