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Calculating optimal surveillance for detection of von Hippel-Lindau-related manifestations.
[von hippel-lindau disease]
von
Hippel-
Lindau
(
VHL
)
mutation
carriers
develop
benign
and
malignant
tumors
,
requiring
regular
surveillance
.
The
aim
of
this
study
was
to
calculate
the
optimal
organ-
specific
age
to
initiate
surveillance
and
optimal
intervals
to
detect
initial
and
subsequent
VHL
-related
manifestations
.
In
this
study
,
we
compare
these
results
with
the
current
VHL
surveillance
guidelines
.
We
collected
data
from
82
VHL
mutation
carriers
in
the
Dutch
VHL
surveillance
program
.
The
cumulative
proportion
of
carriers
diagnosed
with
a
first
VHL
-related
manifestation
was
estimated
by
the
Kaplan-
Meier
method
.
The
Poisson
distribution
model
was
used
to
calculate
average
time
to
detection
of
the
first
VHL
-related
manifestation
and
subsequent
manifestations
.
We
used
this
to
calculate
the
optimal
organ-
specific
age
to
initiate
surveillance
and
the
surveillance
interval
that
results
in
a
detection
probability
of
5
%
.
The
calculated
organ-
specific
ages
to
initiate
surveillance
were
0
years
(
birth
)
for
adrenal
glands
,
7
years
for
the
retina
,
14
years
for
the
cerebellum
,
15
years
for
the
spinal
cord
,
16
years
for
pancreas
,
and
18
years
for
the
kidneys
.
The
calculated
surveillance
intervals
were
4
years
for
the
adrenal
glands
,
biennially
for
the
retina
and
pancreas
,
and
annually
for
the
cerebellum
,
spinal
cord
,
and
kidneys
.
Compared
with
current
VHL
guidelines
,
the
calculated
starting
age
of
surveillance
was
6
years
later
for
the
retina
and
5
years
earlier
for
adrenal
glands
.
The
surveillance
intervals
were
two
times
longer
for
the
retina
and
four
times
longer
for
the
adrenal
glands
.
To
attain
a
5
%
detection
probability
rate
per
organ
,
our
mathematical
model
indicates
that
several
modifications
of
current
VHL
surveillance
guidelines
should
be
considered
.
Diseases
Validation
Diseases presenting
"malignant tumors"
symptom
adrenal incidentaloma
cholangiocarcinoma
coats disease
cowden syndrome
cushing syndrome
dedifferentiated liposarcoma
dentinogenesis imperfecta
esophageal carcinoma
focal myositis
junctional epidermolysis bullosa
liposarcoma
pleomorphic liposarcoma
von hippel-lindau disease
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