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Neuroblastoma after childhood: prognostic relevance of segmental chromosome aberrations, ATRX protein status, and immune cell infiltration.
[alpha-thalassemia]
Neuroblastoma
(
NB
)
is
a
common
malignancy
in
children
but
rarely
occurs
during
adolescence
or
adulthood
.
This
subgroup
is
characterized
by
an
indolent
disease
course
,
almost
uniformly
fatal
,
yet
little
is
known
about
the
biologic
characteristics
.
The
aim
of
this
study
was
to
identify
differential
features
regarding
DNA
copy
number
alterations
,
α-thalassemia
/
mental
retardation
syndrome
X-
linked
(
ATRX
)
protein
expression
,
and
the
presence
of
tumor
-associated
inflammatory
cells
.
Thirty
-
one
NB
patients
older
than
10
years
who
were
included
in
the
Spanish
NB
Registry
were
considered
for
the
current
study
;
seven
young
and
middle
-aged
adult
patients
(
range
18
-
60
years
)
formed
part
of
the
cohort
.
We
performed
single
nucleotide
polymorphism
arrays
,
immunohistochemistry
for
immune
markers
(
CD
4
,
CD
8
,
CD
2
0
,
CD
11
b
,
CD
11
c
,
and
CD
68
)
,
and
ATRX
protein
expression
.
Assorted
genetic
profiles
were
found
with
a
predominant
presence
of
a
segmental
chromosome
aberration
(
SCA
)
profile
.
Preadolescent
and
adolescent
NB
tumors
showed
a
higher
number
of
SCA
,
including
17
q
gain
and
11
q
deletion
.
There
was
also
a
marked
infiltration
of
immune
cells
,
mainly
high
and
heterogeneous
,
in
young
and
middle
-aged
adult
tumors
.
ATRX
negative
expression
was
present
in
the
tumors
.
The
characteristics
of
preadolescent
,
adolescent
,
young
adult
,
and
middle
-aged
adult
NB
tumors
are
different
,
not
only
from
childhood
NB
tumors
but
also
from
each
other
.
Similar
examinations
of
a
larger
number
of
such
tumor
tissues
from
cooperative
groups
should
lead
to
a
better
older
age-dependent
tumor
pattern
and
to
innovative
,
individual
risk-adapted
therapeutic
approaches
for
these
patients
.
Diseases
Validation
Diseases presenting
"single nucleotide polymorphism arrays"
symptom
alpha-thalassemia
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