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Serum VEGF-D a concentration as a biomarker of lymphangioleiomyomatosis severity and treatment response: a prospective analysis of the Multicenter International Lymphangioleiomyomatosis Efficacy of Sirolimus (MILES) trial.
[lymphangioleiomyomatosis]
VEGF-D
is
a
lymphangiogenic
growth
factor
that
has
a
key
role
in
tumour
metastasis
.
Serum
VEGF-D
concentrations
are
increased
in
most
patients
with
lymphangioleiomyomatosis
,
a
rare
neoplasm
associated
with
mTOR-activating
tuberous
sclerosis
gene
mutations
,
lymphadenopathy
,
metastatic
spread
,
and
pulmonary
cyst
formation
.
We
used
data
from
the
Multicenter
International
Lymphangioleiomyomatosis
Efficacy
of
Sirolimus
(
MILES
)
trial
to
assess
the
usefulness
of
serum
VEGF-D
concentration
as
a
marker
of
severity
and
therapeutic
response
to
sirolimus
in
patients
with
lymphangioleiomyomatosis
.
In
the
MILES
trial
,
patients
with
lymphangioleiomyomatosis
who
had
forced
expiratory
volume
in
1
second
(
FEV
1
)
of
70
%
or
less
of
predicted
were
randomly
assigned
(
1
:
1
)
to
12
months
masked
treatment
with
sirolimus
or
placebo
.
Serum
VEGF-D
concentrations
were
measured
at
baseline
,
6
months
,
and
12
months
.
We
used
a
linear
regression
model
to
assess
associations
of
baseline
VEGF-D
concentrations
with
markers
of
disease
severity
,
and
a
linear
mixed
effects
model
to
assess
the
associations
of
VEGF-D
concentrations
with
between-group
differences
in
clinical
,
physiological
,
and
patient-reported
outcomes
.
We
included
42
patients
from
the
placebo
group
and
45
from
the
sirolimus
group
in
our
analysis
.
Baseline
VEGF-D
concentrations
in
individual
patients
varied
from
0
·
34
ng
/
mL
to
16
·
7
ng
/
mL
.
Baseline
VEGF-D
concentrations
were
higher
in
patients
who
needed
supplemental
oxygen
than
in
those
who
did
not
need
supplemental
oxygen
(
1
·
7
ng
/
mL
[
IQR
0
·
99
–
3
·
36
]
vs
0
·
84
ng
/
mL
[
0
·
52
–
1
·
39
]
;
p
<
0
·
0001
)
and
in
those
who
had
a
bronchodilator
response
than
in
those
who
did
not
(
2
·
01
ng
/
mL
[
0
·
99
–
2
·
86
]
vs
1
·
00
ng
/
mL
[
0
·
61
–
2
·
15
]
;
0
·
0273
)
.
Median
serum
VEGF-D
concentrations
were
similar
at
baseline
in
the
sirolimus
and
placebo
groups
,
and
fell
from
baseline
at
6
and
12
months
in
the
sirolimus
group
but
remained
roughly
stable
in
the
placebo
group
.
Each
one
-unit
increase
in
baseline
log
(
VEGF-D
)
was
associated
with
a
between-group
difference
in
baseline-
to
-
12
-
month
FEV
1
change
of
134
mL
(
p
=
0
·
0007
)
.
In
the
sirolimus
group
,
improvement
in
baseline-
to
-
12
-
month
FEV
1
occurred
in
15
of
23
(
65
%
)
VEGF-D
responders
(
ie
,
those
in
whom
baseline-
to
-
12
-
month
VEGF-D
concentrations
decreased
by
more
than
they
did
in
any
patients
in
the
placebo
group
)
and
four
of
15
(
27
%
)
VEGF-D
non-responders
(
p
=
0
·
0448
)
.
Serum
VEGF-D
is
a
biologically
plausible
and
useful
biomarker
in
lymphangioleiomyomatosis
that
correlates
with
disease
severity
and
treatment
response
.
Measurement
of
serum
VEGF-D
concentrations
could
inform
the
risk–benefit
analysis
of
sirolimus
therapy
in
patients
with
lymphangioleiomyomatosis
and
reduce
the
numbers
of
patients
needed
for
clinical
trials
.
National
Institutes
of
Health
,
US
Department
of
Defense
.
Diseases
Validation
Diseases presenting
"metastatic spread"
symptom
lymphangioleiomyomatosis
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