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Phase II study of iproplatin (CHIP, JM-9) in advanced testicular cancers progressing after prior chemotherapy
Phase
II Study of Iproplatin
Advanced
Tes titular
(CHIP,
Cancers
JM-9)
Progressing
in After
Prior Chemotherapy MICHEL CLAVEL,* SILVIO MONFARDINI,? SIEGENTHALER,II JOSETTE RENARD,l
‘Centre Lebn Be’rard, F-69373 Hospital,
Montebello,
hleuchatel,
patients
General Hospital,
CH 2000 Neuchatel, Switzerland,
with advanced
The most severe toxicip
cycle of 240 and 180 mg/m2
dei Tumori, I-20133
was thrombocytopenia
No antitumor activig
pylamine
with two toxic deaths after a
occurred 6 weeks after the Jirst cycle while the tumor was was observed in this heavily pretreated population
(IV), CHIP, of cisplatin,
platinum
derivative
search
for a better
to the parent activity
of
although
I studies
and in Europe ranging
from
with
index
consisting
and doses
In all the studies,
in cumulative
other
myelosuppres-
skin rashes
dose
schedule,
repeated
rate was reported
carcinoma
including
to entry
in the study.
All ofthe
tumors
which
criteria
included cells
Patients
to or recurrent
therapy
containing
cisplatin. therapy
of a member
of the
4 weeks
preceding
Trials
Group,
program
with
treated
and resistant
pmol/l.
or radiation
disease-oriented
in previously
4
S25
paper
we decided phase reports
disseminated
to
that
had primary
the
testis.
status
23.5
of
provided
patients
creatininc
therapy
on
This
(WBC)
presence
the 4 weeks prior
from
serum
1
evi-
the
within
a performance
(in
the only
such as AFP and/
for the study
rising
2 130 X log/l,
in patients
was
markers
originated
proven with
or evaluable in whom
disease
were eligible
pati-
Early Clinical iproplatin.
Patients
pretreated
EORTC
large
every
2 diameters)
histologically teratocarcinoma
the level was clearly
blood
and rarely
(in
levels of serum
bilirubin
embark
icular
[2-41
had
lesions.
of progressive
elevated or PHCG,
schedules
cnts [5]. Based on this experience
conclusions
dence
with
in the U.S.A.
toxicity,
a single
a
significant,
was thrombocytopenia,
a high response ovarian
is
patients malignant
measurable diameter)
[ 11.
[5] used various toxicity
antitumor
selection
All eligible progressive
as compared The
animals
conducted
sion, gastrointestinal renal toxicity. Using
JM-91 is a quadrideveloped in the
20 to 380 mg/m’.
dose limiting toxicities
Patient
to be cross-resistant
in L 1210 leukemia
Phase
weeks,
in
found
of patients.
MATERIALS AND METHODS
compound.
iproplatin
it was
cisplatin
therapeutic
cisplatin
at a dose
or recurred after chemotherapy
[cis-dichloro-trans-hydroxy-bis-isopro-
valent
:Det Norske Radium
IEORTC Data Center, B-1000 Bruxelles. Be&urn and **Free University Hospital, NL-1081 HVAmsterdam, The Netherlands
INTRODUCTION IPROPLATIN
Milano, Itab,
respectively. Nausea and vomiting were almost universal but
mild in intensity. One renal failure progressing.
STANLEY KAYE,$ PIERRE
Glasgow G12 OYN, United Kingdom, [[Hipitaux de la Ville de
testicular cancer received iprojdatin
mg/m’ every 4 weeks. All the patients progressed
including cisplatin. jrst
Lyon, Cedex 08, France, tlstituto Narionale
Oslo 3, Norway, SGartnavel
Cadolles Pourtales,
Abstract-Twenty-two of 180-240
STEIN GUNDERSEN,:
MARTINE VAN GLABBEKEI and HERBERT M. PINEDO** on behalf of the EORTC Early Clinical Trials Group77
Entry
of O-2, white
X lO”/l,
platelets
S 150 pmol/l
and
had to be pretreated
after a previous
chemo-
No previous
chemo-
was allowed
the administration
within
the
of iproplatin.
Drug and treatment
II
Vials
our test-
cancer.
Accepted 5 April 1988.
containing
50 mg of iproplatin
to1 were solution
reconstituted with and then further
isotonic 60 min.
saline for intravenous No further hydration
and manni-
50 ml of isotonic saline diluted in 1000 ml of administration was administered.
over
At the start of the study, the dose of iproplatin given was 240 mg/m2 but this was subsequently
ttOthcr participants (in orderofparticipation): Win’l‘en Bokkel Huinink, Amsterdam, ‘I‘he Netherlands; Rem Abeie, Geneva, Switzerland; Franc0 Cavalli, Bellinzona, Switzerland; Eduard Holdcner, St Gallen. Switzerland; Olhjorn Klepp, Trondheim, Norway.
reduced suppression 1345
to
180 mg/m’
because
in the first
14 patients
of severe
myelo-
treated.
Treat-
M. Clavel et al.
1346 ment
courses
case
of myelosuppression
were
rescheduled
repeated
treatment
maximum
(WHO)
occurred.
when
unless
of new lesions
gressive
disease),
iproplatin
stopped.
Otherwise,
qualify
and partial
standard
criteria.
eligible
the study
from
Table
1 shows
patients. progressive
were
entered
ofall the eligible patient
prior
Seven
received
majority
nantly
embryonal
carcinoma
five a raised
received two The
and
three first
starting
the
eight
considered
a definite
tumor,
three a raised
alone.
Fourteen
AFP
patients
three
received severe
of
the
not
patients,
a clear
definite
progression
cycle was completed.
2 shows
the lowest
blood
patients
penia;
suffered
toxicity
was observed, a first
dose
four evaluable
patients
were
for
tumor
2 (2-2.9)
degree
WBC
count
and
1 (1-1.9).
was much
more
severe.
count
higher
100 X lo”/1 after the first course
than
while four had the lowest 99 X log/l, two below patient
of
value:
four between
had a platelet
between
50 X 10’1
20 and
49 X log/1
20 X log/l. died.
men containing
He was a 29-year-old treated
240 mg/m2,
After
he
toxicity
with a nadir
pneumonia.
Leucopenia
developed and
platelet
0: 10 1: 7 2: 5
*All patients were previously treated by chemotherapy cisplatin [median number of drugs: 6 (4-g)].
regi-
the first iproplatin a
grade
delayed count
3
thrombo-
of 9 X log/l,3 he started broncho-
was not observed
amongst
the eight patients who receiued a starting dose of 180 mg/
another
(20-5;
Prior surgery curative palliative
patient,
by a chemotherapy
six drugs.
nausea-vomiting
year-old index
Among
only four patients
however,
was
still
a sig-
problem.
a life threatening
Performance
3 and
However,
A nadir platelet count between 50 and 99 was observed in two patients after the first cycle, while
22
Number
of leuco-
between
14 patients,
nificant
Table 1. Characteristics of eligible patient?
for white
with the day
these
dose of
a modest
five had a lowest
One
as a
values
together
In 14 patients receiving 240 mg/m’ as a starting dose, six patients had no evidence of leucopenia while
m2. Thrombocytopenia,
Median age in years Range
4
of nadir.
and
patients
240 mg/m2
received
being
second
in progression.
showed
Antitumor response as
as
and were
cytopenia
22 eligible
during
the treatment
weeks after the treatment. At that stage, gastro-intestinal bleeding and fatal
Among
a
tumor
out of the study.
180 mg/m’.
considered
after
were considered during
stopped
as being
patient
Table
1 and
five received
remaining
patients
4
was
received
progression
and dropped
PS = 1, previously
dose; because
next
then
evidence
of treatment
thrombocytopenia
cycles. 14 patients
any
progressed
interval,
3.9 X log/l,
predomi-
of the primary
+ AFP,
HCG
patients
?? one
eight 15
intention.
(16) had
only one cycle of iproplatin,
cycles,
received
the
HCG
contain-
radiotherapy.
of the patients
seven had a raised alone,
previous
had
surgery,
aim, seven with palliative
patients
(WHO
a prior regimen
undergone
with a curative The
into
All of the patients
despite
and
blood cells and thrombocytes,
non-eligible
All had
with
after the third
the characteristics
disease
ing cisplatin.
first this
Toxicip
patients
iproplatin.
?? five
change
11 institutions.
PS 3) received
without
10 patients
weeks
response.
One additional
cycle
early progression
RESULTS Twenty-two
of iproplatin
as pro-
to
the
case,
reduction. ??
responses No
were considered
courses
the first 4 weeks
that was insufficient
within
In one
as no change
two
lesions was
death
treatment.
disease. ?? two patients
pati-
administration
shrinkage
for a 50% partial
(defined
to early
because of severe with progressive
third
In the
of the indicator
complete
with
a tumor
These
due following
considered to be a toxic death myelosuppresion in association
courses
progressions.
or the appearance
response weeks
of progressive
after one course. of 25%
defined
Organiz-
iproplatin
as early
a
myelosuppression
case of an increase
were
for
to 80% or
Health
4
clear evidence
considered
indicated
was
World
of two
was apparent
were
In the
postponed
3 or
A minimum
disease
4 weeks. retreatment
Dose adjustments
grade
were intended, ents
was
of 2 weeks.
60% were performed ation
every when
22 15 7 including
previously
patient
thrombocytopenia
occurred
receiving
180 mg/m*.
with
a PS of 1, who
patient treated
with
six different
in
He was a 48had
drugs.
been After
2
weeks of treatment with a dose of 180 mg/m* he developed thrombocytopenia with a nadir platelet count of 20, inducing a fatal upper gastro-intestinal bleeding despite intensive platelet transfusion. The non-hematological observed are listed in Table occurred almost universally
toxicities which were 3. Nausea and vomiting after iproplatin admin-
1347
Iproplatin in Advanced Testicular Cancers Table 2. Hematological
toxicity Nadir values
WBC x lo”/1 240 mg/m’ starting
X lo”/1
dose
1st course Median Range Day of nadir
4.2 (6.2-1.8) 20 (534)
Overall Median Range
3.1 (5.1-1.8)
180 mg/n?
Platelets
starting
(2K9, 20 (7-31)
dose
1st course Median Range Day of nadir
3.9 (2.4-9.5) 13 (G-21)
Overall Median Range
(2.4-9.5)
(31Y75, 13 (12-14)
54* (175-16)
3.9
*Two toxic deaths from thrombocytopenia. Table 3. Non-hematological
20 9 1 1 1
Nausea-vomiting Diarrhea Mucositis Drug fever Renal failure
istration,
of mild
or moderate
was observed
in almost
mildly.
grade
Other
intensity.
1 and 2 toxicities
1
prior m2
drug
patient,
renal
toxicity
previously
Bleomycin (240 mg/m’),
After
he
treatment. clear
At that
progression.
the fatal sidered
a fatal
cisplatin,
developed
toxicity;
VP 16,
During
after
from
grade
3 *weeks,
renal
failure
time tumor Although
indicators it is not clear
grade
4 renal
3 and
3
dose
the platebleeding. he
penia reported
the
of short
after showed
a
whether
and death.
in one case Thus
to 180 mg/m’.
by the vast majority duration
the
In spite
this
initial of this
of patients
and qualitatively
but were
less severe
than
with cisplatin. With
weekly
this case was contoxicity.
failure
occurred
was not proven
Phase II trials of new drugs in testicular cancer are difficult to accomplish because of the extent of
was
thrombocytopenia
a second toxic death due to thrombocytoNausea and vomiting were was noted.
any renal function
DISCUSSION
without
myelosuppression
developed
patient’s
reduced
dose was 240 mg/
intravenously
4, respectively,
to the
was
reduction
toxicity,
6 weeks
graded
given
Two patients
persisted
treatment
a
hematological
issue was drug-related, as a WHO
4 weeks
all of the patients. starting
Drug-induced
marked.
in a 30-year-old
was 2.7 X lo’/1 and he started
recovering
developed
with
Ifosfamide.
nausea-vomiting lets count
occurred
treated
and
every
in virtually
the iproplatin
hydration.
fever and mucositis. A severe
treatment
Initially
but only
included
90 41 5 5 5
7 0
Diarrhea
half of the patients
Percentage of total patients
Number of patients with grade 3-4 toxicities
Number of patients
Type
toxicities
creatinine
we did not demonstrate
impairment. 6 weeks
after
The only fatal renal the
to be drug-related.
treatment
and
No antitumor
activity was detected in this trial concerning patients pretreated with cisplatin. We conclude that iproplatin given at a dose of 180-240 mg/m’ is not active in this patient population.
M. Clavel et al.
1348
REFERENCES 1. Bradner WT, Rose WC, Huftalen JB. Antitumor activity of platinum analogs. In: Prestayko
2. 3.
4.
5.
AW, Crooke ST, Carter SK, eds. Cisplatin, Current Status and New Developments. New York, Academic Press, 1980, 17 l-l 82. Creaven PJ, Madajewicz S, Pendyala L et al. Phase I clinical trial of cis-dichloro-transdihydroxy-bis-isopropylamine platinum (IV) (CHIP). Cancer Treat Rep 1983, 67, 795-800. Ginsberg S, Lee F, Issell B et al. A phase I study of cis-dichloro-trans-dihydroxy-bisisopropylamine platinum (IV) (CHIP) a d ministered by intravenous bolus daily for 5 days. Proc MC0 1983, 2, 35. Yap BS, Tenney DM, Yap HY et al. Phase I clinical evaluation of cis-dichloro-transdihydroxy-bis-isopropylamine platinum IV (CHIP-JMS). Proc Am Assoc Cancer Res 1983, 24, 166. Bramwell VHC, Crowther D, O’Malley S et al. Activity ofJM 9 in advanced ovarian cancer: a phase I-II trial. Cancer Treat Rep 1985, 69, 409-416.
II Study of Iproplatin
Advanced
Tes titular
(CHIP,
Cancers
JM-9)
Progressing
in After
Prior Chemotherapy MICHEL CLAVEL,* SILVIO MONFARDINI,? SIEGENTHALER,II JOSETTE RENARD,l
‘Centre Lebn Be’rard, F-69373 Hospital,
Montebello,
hleuchatel,
patients
General Hospital,
CH 2000 Neuchatel, Switzerland,
with advanced
The most severe toxicip
cycle of 240 and 180 mg/m2
dei Tumori, I-20133
was thrombocytopenia
No antitumor activig
pylamine
with two toxic deaths after a
occurred 6 weeks after the Jirst cycle while the tumor was was observed in this heavily pretreated population
(IV), CHIP, of cisplatin,
platinum
derivative
search
for a better
to the parent activity
of
although
I studies
and in Europe ranging
from
with
index
consisting
and doses
In all the studies,
in cumulative
other
myelosuppres-
skin rashes
dose
schedule,
repeated
rate was reported
carcinoma
including
to entry
in the study.
All ofthe
tumors
which
criteria
included cells
Patients
to or recurrent
therapy
containing
cisplatin. therapy
of a member
of the
4 weeks
preceding
Trials
Group,
program
with
treated
and resistant
pmol/l.
or radiation
disease-oriented
in previously
4
S25
paper
we decided phase reports
disseminated
to
that
had primary
the
testis.
status
23.5
of
provided
patients
creatininc
therapy
on
This
(WBC)
presence
the 4 weeks prior
from
serum
1
evi-
the
within
a performance
(in
the only
such as AFP and/
for the study
rising
2 130 X log/l,
in patients
was
markers
originated
proven with
or evaluable in whom
disease
were eligible
pati-
Early Clinical iproplatin.
Patients
pretreated
EORTC
large
every
2 diameters)
histologically teratocarcinoma
the level was clearly
blood
and rarely
(in
levels of serum
bilirubin
embark
icular
[2-41
had
lesions.
of progressive
elevated or PHCG,
schedules
cnts [5]. Based on this experience
conclusions
dence
with
in the U.S.A.
toxicity,
a single
a
significant,
was thrombocytopenia,
a high response ovarian
is
patients malignant
measurable diameter)
[ 11.
[5] used various toxicity
antitumor
selection
All eligible progressive
as compared The
animals
conducted
sion, gastrointestinal renal toxicity. Using
JM-91 is a quadrideveloped in the
20 to 380 mg/m’.
dose limiting toxicities
Patient
to be cross-resistant
in L 1210 leukemia
Phase
weeks,
in
found
of patients.
MATERIALS AND METHODS
compound.
iproplatin
it was
cisplatin
therapeutic
cisplatin
at a dose
or recurred after chemotherapy
[cis-dichloro-trans-hydroxy-bis-isopro-
valent
:Det Norske Radium
IEORTC Data Center, B-1000 Bruxelles. Be&urn and **Free University Hospital, NL-1081 HVAmsterdam, The Netherlands
INTRODUCTION IPROPLATIN
Milano, Itab,
respectively. Nausea and vomiting were almost universal but
mild in intensity. One renal failure progressing.
STANLEY KAYE,$ PIERRE
Glasgow G12 OYN, United Kingdom, [[Hipitaux de la Ville de
testicular cancer received iprojdatin
mg/m’ every 4 weeks. All the patients progressed
including cisplatin. jrst
Lyon, Cedex 08, France, tlstituto Narionale
Oslo 3, Norway, SGartnavel
Cadolles Pourtales,
Abstract-Twenty-two of 180-240
STEIN GUNDERSEN,:
MARTINE VAN GLABBEKEI and HERBERT M. PINEDO** on behalf of the EORTC Early Clinical Trials Group77
Entry
of O-2, white
X lO”/l,
platelets
S 150 pmol/l
and
had to be pretreated
after a previous
chemo-
No previous
chemo-
was allowed
the administration
within
the
of iproplatin.
Drug and treatment
II
Vials
our test-
cancer.
Accepted 5 April 1988.
containing
50 mg of iproplatin
to1 were solution
reconstituted with and then further
isotonic 60 min.
saline for intravenous No further hydration
and manni-
50 ml of isotonic saline diluted in 1000 ml of administration was administered.
over
At the start of the study, the dose of iproplatin given was 240 mg/m2 but this was subsequently
ttOthcr participants (in orderofparticipation): Win’l‘en Bokkel Huinink, Amsterdam, ‘I‘he Netherlands; Rem Abeie, Geneva, Switzerland; Franc0 Cavalli, Bellinzona, Switzerland; Eduard Holdcner, St Gallen. Switzerland; Olhjorn Klepp, Trondheim, Norway.
reduced suppression 1345
to
180 mg/m’
because
in the first
14 patients
of severe
myelo-
treated.
Treat-
M. Clavel et al.
1346 ment
courses
case
of myelosuppression
were
rescheduled
repeated
treatment
maximum
(WHO)
occurred.
when
unless
of new lesions
gressive
disease),
iproplatin
stopped.
Otherwise,
qualify
and partial
standard
criteria.
eligible
the study
from
Table
1 shows
patients. progressive
were
entered
ofall the eligible patient
prior
Seven
received
majority
nantly
embryonal
carcinoma
five a raised
received two The
and
three first
starting
the
eight
considered
a definite
tumor,
three a raised
alone.
Fourteen
AFP
patients
three
received severe
of
the
not
patients,
a clear
definite
progression
cycle was completed.
2 shows
the lowest
blood
patients
penia;
suffered
toxicity
was observed, a first
dose
four evaluable
patients
were
for
tumor
2 (2-2.9)
degree
WBC
count
and
1 (1-1.9).
was much
more
severe.
count
higher
100 X lo”/1 after the first course
than
while four had the lowest 99 X log/l, two below patient
of
value:
four between
had a platelet
between
50 X 10’1
20 and
49 X log/1
20 X log/l. died.
men containing
He was a 29-year-old treated
240 mg/m2,
After
he
toxicity
with a nadir
pneumonia.
Leucopenia
developed and
platelet
0: 10 1: 7 2: 5
*All patients were previously treated by chemotherapy cisplatin [median number of drugs: 6 (4-g)].
regi-
the first iproplatin a
grade
delayed count
3
thrombo-
of 9 X log/l,3 he started broncho-
was not observed
amongst
the eight patients who receiued a starting dose of 180 mg/
another
(20-5;
Prior surgery curative palliative
patient,
by a chemotherapy
six drugs.
nausea-vomiting
year-old index
Among
only four patients
however,
was
still
a sig-
problem.
a life threatening
Performance
3 and
However,
A nadir platelet count between 50 and 99 was observed in two patients after the first cycle, while
22
Number
of leuco-
between
14 patients,
nificant
Table 1. Characteristics of eligible patient?
for white
with the day
these
dose of
a modest
five had a lowest
One
as a
values
together
In 14 patients receiving 240 mg/m’ as a starting dose, six patients had no evidence of leucopenia while
m2. Thrombocytopenia,
Median age in years Range
4
of nadir.
and
patients
240 mg/m2
received
being
second
in progression.
showed
Antitumor response as
as
and were
cytopenia
22 eligible
during
the treatment
weeks after the treatment. At that stage, gastro-intestinal bleeding and fatal
Among
a
tumor
out of the study.
180 mg/m’.
considered
after
were considered during
stopped
as being
patient
Table
1 and
five received
remaining
patients
4
was
received
progression
and dropped
PS = 1, previously
dose; because
next
then
evidence
of treatment
thrombocytopenia
cycles. 14 patients
any
progressed
interval,
3.9 X log/l,
predomi-
of the primary
+ AFP,
HCG
patients
?? one
eight 15
intention.
(16) had
only one cycle of iproplatin,
cycles,
received
the
HCG
contain-
radiotherapy.
of the patients
seven had a raised alone,
previous
had
surgery,
aim, seven with palliative
patients
(WHO
a prior regimen
undergone
with a curative The
into
All of the patients
despite
and
blood cells and thrombocytes,
non-eligible
All had
with
after the third
the characteristics
disease
ing cisplatin.
first this
Toxicip
patients
iproplatin.
?? five
change
11 institutions.
PS 3) received
without
10 patients
weeks
response.
One additional
cycle
early progression
RESULTS Twenty-two
of iproplatin
as pro-
to
the
case,
reduction. ??
responses No
were considered
courses
the first 4 weeks
that was insufficient
within
In one
as no change
two
lesions was
death
treatment.
disease. ?? two patients
pati-
administration
shrinkage
for a 50% partial
(defined
to early
because of severe with progressive
third
In the
of the indicator
complete
with
a tumor
These
due following
considered to be a toxic death myelosuppresion in association
courses
progressions.
or the appearance
response weeks
of progressive
after one course. of 25%
defined
Organiz-
iproplatin
as early
a
myelosuppression
case of an increase
were
for
to 80% or
Health
4
clear evidence
considered
indicated
was
World
of two
was apparent
were
In the
postponed
3 or
A minimum
disease
4 weeks. retreatment
Dose adjustments
grade
were intended, ents
was
of 2 weeks.
60% were performed ation
every when
22 15 7 including
previously
patient
thrombocytopenia
occurred
receiving
180 mg/m*.
with
a PS of 1, who
patient treated
with
six different
in
He was a 48had
drugs.
been After
2
weeks of treatment with a dose of 180 mg/m* he developed thrombocytopenia with a nadir platelet count of 20, inducing a fatal upper gastro-intestinal bleeding despite intensive platelet transfusion. The non-hematological observed are listed in Table occurred almost universally
toxicities which were 3. Nausea and vomiting after iproplatin admin-
1347
Iproplatin in Advanced Testicular Cancers Table 2. Hematological
toxicity Nadir values
WBC x lo”/1 240 mg/m’ starting
X lo”/1
dose
1st course Median Range Day of nadir
4.2 (6.2-1.8) 20 (534)
Overall Median Range
3.1 (5.1-1.8)
180 mg/n?
Platelets
starting
(2K9, 20 (7-31)
dose
1st course Median Range Day of nadir
3.9 (2.4-9.5) 13 (G-21)
Overall Median Range
(2.4-9.5)
(31Y75, 13 (12-14)
54* (175-16)
3.9
*Two toxic deaths from thrombocytopenia. Table 3. Non-hematological
20 9 1 1 1
Nausea-vomiting Diarrhea Mucositis Drug fever Renal failure
istration,
of mild
or moderate
was observed
in almost
mildly.
grade
Other
intensity.
1 and 2 toxicities
1
prior m2
drug
patient,
renal
toxicity
previously
Bleomycin (240 mg/m’),
After
he
treatment. clear
At that
progression.
the fatal sidered
a fatal
cisplatin,
developed
toxicity;
VP 16,
During
after
from
grade
3 *weeks,
renal
failure
time tumor Although
indicators it is not clear
grade
4 renal
3 and
3
dose
the platebleeding. he
penia reported
the
of short
after showed
a
whether
and death.
in one case Thus
to 180 mg/m’.
by the vast majority duration
the
In spite
this
initial of this
of patients
and qualitatively
but were
less severe
than
with cisplatin. With
weekly
this case was contoxicity.
failure
occurred
was not proven
Phase II trials of new drugs in testicular cancer are difficult to accomplish because of the extent of
was
thrombocytopenia
a second toxic death due to thrombocytoNausea and vomiting were was noted.
any renal function
DISCUSSION
without
myelosuppression
developed
patient’s
reduced
dose was 240 mg/
intravenously
4, respectively,
to the
was
reduction
toxicity,
6 weeks
graded
given
Two patients
persisted
treatment
a
hematological
issue was drug-related, as a WHO
4 weeks
all of the patients. starting
Drug-induced
marked.
in a 30-year-old
was 2.7 X lo’/1 and he started
recovering
developed
with
Ifosfamide.
nausea-vomiting lets count
occurred
treated
and
every
in virtually
the iproplatin
hydration.
fever and mucositis. A severe
treatment
Initially
but only
included
90 41 5 5 5
7 0
Diarrhea
half of the patients
Percentage of total patients
Number of patients with grade 3-4 toxicities
Number of patients
Type
toxicities
creatinine
we did not demonstrate
impairment. 6 weeks
after
The only fatal renal the
to be drug-related.
treatment
and
No antitumor
activity was detected in this trial concerning patients pretreated with cisplatin. We conclude that iproplatin given at a dose of 180-240 mg/m’ is not active in this patient population.
M. Clavel et al.
1348
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