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Binding of toremifene to plasma proteins
108s
C-028 BINDING
OF TOREMIFENE
SipilB,
H., NBntb,V.
Central The
Hospital,
in vitro
(300
000
strong
protein
x g,
unlabeled
was
bound
the
of
of
toremifene
cold
phoresis
toremifene
to
sensitive total
fractionate
tion
and
bound
about
2X
different
and
The
Of
by
University
by ultracentrifugation be used
and
to agarose
Localized 6X
99.7X
by
500
gel
using
ng/ml
electroposition-
by staining.Of
to
to
drug.
visualized
about
due
together
radioactivity
3H-toremifene
was
albumin,
total
exposed
were
not
3H-Toremifene
unlabeled
adding
were
proteins to
the
of the
radioactivity
the
Turku
could
membranes.
used.
samptes
bound
pre-alpha,-globulin
measured methods
and
studied
serum
that was
was
concentration
proteins. 92%
serum
was
Center,and
Finland.
filtration
filters
was
The
After
radioactivity
human
51700 nglml
proteins
different
Turku,
and
on the
Research
Ltd.,
assayed
plasma.
counter.
to
all
500,
standard
in
dialysis
to
50,
to to
Group
Chemistry.
toremifene
independent
proportional
protein
of
toremifene
proteins
Binding
Clinical
Equilibrium
toremifene,
to
t. Farmos
of
binding
6.5 hours). of
PROTEINS
Kangas,
Oepartment
adsorption
with
TO PLASMA and
the
beta-l-globulin
frac-
fraction_
c-029 TOLERANCE
AND EFFICACY
Stamm H.,
Roth
Kantonsspital
From
20
1985
with
or
100
to
August
to
DROLOXIFENE
He il
H. J.*,
Basle,
1986
droloxifene
after
sodium,
Stab
Frauenklinik,
single
laboratory
eight
IN
PATIENTS
WITH
ADVANCED BREAST CANCER
M. *
Switzerland;
*Klinge
postmenopausal
investigate
were
Tolerance
dose:
There
parameters
potassium,
hormones
A.,
Pharms
patients
tolerance,
kinetics
no effects
on vital
with and
GmbH,
advanced
8000
Miinchen,
breast
efficacy
after
cancer
single
F.R.G.
were
enrolled
and multiple
in
oral
phase
doses
X/II
with
mq tablets.
Tolerance Standard
OF THE ANTIESTROGEN
Almendral
Easel,
March
studies
R.,
calcium
were
such
as we.ll
as
SGOT,
SGPT,
Y-GT,
cosgulogremand
BY
functions LDH,
CPK,
hemograms
and
no reports
crestinine,
were
not
on any
urea,
affected.
other
serious
total bilirubin, Also no clinically
side
effectu.
blood glucose, relevant chanqss
observed.
after
multiple
doses:
Again
tulerance
was
excellent
and
the
only
occasional
side
effect
observed
were
hot
flushes. Efficacy
of
because the
of
treatment: death
response
over
was
22 months
months remission
Also
present
OF therapy stable
local of
were
start
Clinically
developed
screlosis
tumors
after
20 mg daily.
she
with
weeks
possible.
at
before
Measurable
four
with
is
20 mq one The
lesions,
five
to
evident
patient third
now holding
patients.
refusion
disease
recurxwrxe.
most
in
or
in
had
further
a patient
with
of
of
In
with
could
three
isolated
node
mstastases
a period
patients
therapy.
a remission
patient on over
Three
continue
diffuse
metastases
OF the
16 months
be
evaluated
evaluation lung
over
sternum
under
not
patients
a period
of
experiences
treatment
of
metastases
with
11
partial 100
mg daily.
c-030 OROLOXiFENE: Ahlemann
INTERMITTENT
L.M.,
Heil
Kcankenhiiuser In
a pilot
des phase
day
with
100
All
patients
til
day
Besides
the tumor
as
3/1O In
disease
study
under
10
disease
end
experienced
complete
was
a period
until
LOdenscheid, cancer
a positive for week
* Klinge
were
receptor
response four,
investigations
treated
and
at
tolerance
in
were
performed
GmbH, 8000
intermittently
status
then
Pharma
the
wary
monthly
Mijnchen
every
time
of
day
after
80,
second
primary
F.R.G.
or
third
operation.
start
of
therapy
un-
intervals. and
endocrine,
standard
laboratory
as
monitored. of
diagnosed
of
breast
had
monitored
remissions
remission over
were
intervals
wre
5880
metastatic
patients
pharmacokinetic
parameters
treatment
All
weekly
assessment
partial
with
p.o.
in
BREAST CANCER
Strshlentherapie,
patients
associated
patients
METASTATIC
Kreises,
evaluable
clinical
IN
H..J.*
droloxifene
thereafter
patients four
II
had
THERAPY Stab
MBrkischen
mq of
seven,
well
M.:
seven
osseous with
months.
and
soft
a duration In
two
tissue
metastasis
between
patients
3 and
the
tumor
fasting
7+ months. was
between
6 and
One patient
progressive
had
despite
19+
months.
stable
antiestrogenic
treatment. Tolerance Time
of
courses
disease
before
droloxifene of
the clinical
tumor
treatment
was
associated confirmation
excellent, antigens
,
thus
hot
flushes
were
213
ceees
reflected being
helpful
in
observed with
predicting
occasionally
complete response
in
remission to
therapy.
some patients. and
both
cases
of
progressive
of
C-028 BINDING
OF TOREMIFENE
SipilB,
H., NBntb,V.
Central The
Hospital,
in vitro
(300
000
strong
protein
x g,
unlabeled
was
bound
the
of
of
toremifene
cold
phoresis
toremifene
to
sensitive total
fractionate
tion
and
bound
about
2X
different
and
The
Of
by
University
by ultracentrifugation be used
and
to agarose
Localized 6X
99.7X
by
500
gel
using
ng/ml
electroposition-
by staining.Of
to
to
drug.
visualized
about
due
together
radioactivity
3H-toremifene
was
albumin,
total
exposed
were
not
3H-Toremifene
unlabeled
adding
were
proteins to
the
of the
radioactivity
the
Turku
could
membranes.
used.
samptes
bound
pre-alpha,-globulin
measured methods
and
studied
serum
that was
was
concentration
proteins. 92%
serum
was
Center,and
Finland.
filtration
filters
was
The
After
radioactivity
human
51700 nglml
proteins
different
Turku,
and
on the
Research
Ltd.,
assayed
plasma.
counter.
to
all
500,
standard
in
dialysis
to
50,
to to
Group
Chemistry.
toremifene
independent
proportional
protein
of
toremifene
proteins
Binding
Clinical
Equilibrium
toremifene,
to
t. Farmos
of
binding
6.5 hours). of
PROTEINS
Kangas,
Oepartment
adsorption
with
TO PLASMA and
the
beta-l-globulin
frac-
fraction_
c-029 TOLERANCE
AND EFFICACY
Stamm H.,
Roth
Kantonsspital
From
20
1985
with
or
100
to
August
to
DROLOXIFENE
He il
H. J.*,
Basle,
1986
droloxifene
after
sodium,
Stab
Frauenklinik,
single
laboratory
eight
IN
PATIENTS
WITH
ADVANCED BREAST CANCER
M. *
Switzerland;
*Klinge
postmenopausal
investigate
were
Tolerance
dose:
There
parameters
potassium,
hormones
A.,
Pharms
patients
tolerance,
kinetics
no effects
on vital
with and
GmbH,
advanced
8000
Miinchen,
breast
efficacy
after
cancer
single
F.R.G.
were
enrolled
and multiple
in
oral
phase
doses
X/II
with
mq tablets.
Tolerance Standard
OF THE ANTIESTROGEN
Almendral
Easel,
March
studies
R.,
calcium
were
such
as we.ll
as
SGOT,
SGPT,
Y-GT,
cosgulogremand
BY
functions LDH,
CPK,
hemograms
and
no reports
crestinine,
were
not
on any
urea,
affected.
other
serious
total bilirubin, Also no clinically
side
effectu.
blood glucose, relevant chanqss
observed.
after
multiple
doses:
Again
tulerance
was
excellent
and
the
only
occasional
side
effect
observed
were
hot
flushes. Efficacy
of
because the
of
treatment: death
response
over
was
22 months
months remission
Also
present
OF therapy stable
local of
were
start
Clinically
developed
screlosis
tumors
after
20 mg daily.
she
with
weeks
possible.
at
before
Measurable
four
with
is
20 mq one The
lesions,
five
to
evident
patient third
now holding
patients.
refusion
disease
recurxwrxe.
most
in
or
in
had
further
a patient
with
of
of
In
with
could
three
isolated
node
mstastases
a period
patients
therapy.
a remission
patient on over
Three
continue
diffuse
metastases
OF the
16 months
be
evaluated
evaluation lung
over
sternum
under
not
patients
a period
of
experiences
treatment
of
metastases
with
11
partial 100
mg daily.
c-030 OROLOXiFENE: Ahlemann
INTERMITTENT
L.M.,
Heil
Kcankenhiiuser In
a pilot
des phase
day
with
100
All
patients
til
day
Besides
the tumor
as
3/1O In
disease
study
under
10
disease
end
experienced
complete
was
a period
until
LOdenscheid, cancer
a positive for week
* Klinge
were
receptor
response four,
investigations
treated
and
at
tolerance
in
were
performed
GmbH, 8000
intermittently
status
then
Pharma
the
wary
monthly
Mijnchen
every
time
of
day
after
80,
second
primary
F.R.G.
or
third
operation.
start
of
therapy
un-
intervals. and
endocrine,
standard
laboratory
as
monitored. of
diagnosed
of
breast
had
monitored
remissions
remission over
were
intervals
wre
5880
metastatic
patients
pharmacokinetic
parameters
treatment
All
weekly
assessment
partial
with
p.o.
in
BREAST CANCER
Strshlentherapie,
patients
associated
patients
METASTATIC
Kreises,
evaluable
clinical
IN
H..J.*
droloxifene
thereafter
patients four
II
had
THERAPY Stab
MBrkischen
mq of
seven,
well
M.:
seven
osseous with
months.
and
soft
a duration In
two
tissue
metastasis
between
patients
3 and
the
tumor
fasting
7+ months. was
between
6 and
One patient
progressive
had
despite
19+
months.
stable
antiestrogenic
treatment. Tolerance Time
of
courses
disease
before
droloxifene of
the clinical
tumor
treatment
was
associated confirmation
excellent, antigens
,
thus
hot
flushes
were
213
ceees
reflected being
helpful
in
observed with
predicting
occasionally
complete response
in
remission to
therapy.
some patients. and
both
cases
of
progressive
of