Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT00212043 |
| Other study ID # |
CTRG L08/99 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
Phase 2
|
| First received |
September 13, 2005 |
| Last updated |
October 7, 2009 |
| Start date |
July 2000 |
| Est. completion date |
February 2004 |
Study information
| Verified date |
May 2008 |
| Source |
National University Hospital, Singapore |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
Singapore: Health Sciences Authority |
| Study type |
Interventional
|
Clinical Trial Summary
Hypothesis - Infusional gemcitabine may give better intracellular pharmacologic activation
and be more effective clinically in non-small cell lung cancer
Description:
Objectives of study:
1. to compare the response rate of carboplatin and constant rate infusion gemcitabine to
the response rate of gemcitabine given in the standard 30-minute infusion
2. to compare the toxicity experience in both arms
3. To compare the time to progression in both study arms, and overall survival
4. To compare the quality of life on both study arms using the EORTC QLQ-C30 and QLQ-LC13.
Inclusion criteria
- Histologically or cytologically confirmed NSCLC.
- Stage IIIB unsuitable for radical radiation (eg. with cytologically proven
malignant effusion) or stage IV disease as defined by the AJCC criteria (see
appendix 1).
- Karnofsky performance status 70% or higher (see appendix 2).
- Presence of at least one bidimensionally or unidimensionally measurable, non-CNS,
indicator lesion defined by radiologic study or physical examination.
- No previous chemotherapy for advanced disease. Prior neoadjuvant or adjuvant
chemotherapy, or chemotherapy given concurrently with radiotherapy for
non-metastatic disease, is allowed if the last dose was given 6 months or more
before study entry.
- Patients with recurrent disease after primary surgery and/or radiotherapy will be
eligible.
- For patients with previous radiotherapy, the indicator lesion(s) must not be
within previous radiation field. The last dose of radiotherapy should be at least
3 weeks prior to study entry. The total radiotherapy received should not be more
than 30% of the bone marrow.
- Screening laboratory criteria:
WBC count > 3500/microl Neutrophils > 2000/microl Platelet count > 100,000/microl
Hemoglobin > 9 g/dl (transfusion allowed)
Serum creatinine < 133 micromol/l, or Creatinine clearance > 30 ml/min, based on the
Cockcroft formula (see section 5.1.1)
Bilirubin < 1.5 x upper limit of normal ALT/AST < 2 x upper limit of normal if liver
metastases are absent < 5 x upper limit of normal if liver metastases are present
- Aged 18 years and above.
- Life expectancy > 3 months.
- Written informed consent.
4.2 Exclusion criteria
The following conditions will render patients ineligible to participate in this study:
- Patients with only evaluable disease.
- Active uncontrolled infection.
- Pregnant or lactating women.
- Females of childbearing potential who are unwilling to avoid pregnancy, for the
duration of the study.
- Presence of any underlying medical conditions which in the investigators opinion
would make the patient unsuitable for treatment.
- Concomitant malignancies or previous malignancies other than NSCLC within the last
5 years, with the exception of adequately treated basal or squamous cell carcinoma
of the skin, carcinoma-in-situ of the cervix, or stage A low grade prostate
cancer.
- Patients with CNS and/or leptomeningeal metastases; unless asymptomatic and not
receiving corticosteriod therapy.
4.3 Inclusion and exclusion criteria for phase I patients
The exclusion criteria are the same as above.
The inclusion criteria are the same as above except for the following groups of
patients, which are allowed in the phase I study:
- Patients with evaluable disease only (with no measurable lesions).
- Patients with one (and only one) line of chemotherapy for advanced NSCLC,
excluding patients who had received prior platinium and/or gemcitabine.
- Patients with indicator lesions in previous radiation field.
Measurability of indicator lesions
- Measurable: The lesion can be measured accurately in at least one dimension
(longest diameter to be recorded) as > 20 mm with conventional techniques or as >
10mm with spiral CT scan.
- Non-measurable: All other lesions including small lesions (longest diameter <20 mm
with conventional techniques or < 10 mm with spiral CT scan) and truly
non-measurable lesions. Lesions considered to be truly non-measurable include the
following: bone lesions, leptomeningeal disease, ascites, pleural/cutis/pulmonis,
abdominal masses that are not confirmed and followed by imaging techniques, and
cystic lesions.
- Target Lesions: All measurable lesions up to a maximum of 5 lesions per organ and
10 lesions in total representative of all involved organs should be identified as
target lesions and be recorded and measured at baseline. Target lesions should be
selected on the basis of their size (lesion with the longest diameter) and their
suitability for accurate measurements (either by imaging techniques or
clinically). A sum of the longest diameter (LD) for all target lesions will be
calculated and reported as the baseline sum LD. The baseline sum LD is used as the
reference by which to characterize the objective tumor response. If there are > 10
measurable lesions, those not selected as target lesions will be considered
together with non-measurable disease as non-target lesions.
- Non-target Lesions: All non-measurable lesions (or sites of disease) plus any
measurable lesions over and above the 10 listed as target lesions. Measurements
are not required but these lesions should be noted at baseline and should be
followed as "present" or "absent".
- Any tumour measurement relying solely on physical examination should be verified
by a second physician.
- The same diagnostic imaging method must be used throughout the study to evaluate
the lesions.
5. TREATMENT PLAN
5.1 Phase I study
5.1.1 Carboplatin
The starting dose of carboplatin is given at a fixed dose at a target AUC of 5 over 1
hour on day 1 in both arms of the study. Carboplatin will be given before gemcitabine
in all patients. The dose is repeated every 21 days and will be calculated using the
Calvert formula:
Dose of carboplatin (mg) = [calculated glomerular filtration rate (GFR) + 25] x 5
The GFR will be calculated according to the Cockroft-Gault formula:
GFR (ml/min) = (140 - age) x body weight (in kg) / 0.81 x serum creatinine (micromol/l)
For female, the correction factor is 0.85 (x calculated GFR)
5.1.2 Infusional gemcitabine
Infusional gemcitabine is given at a constant rate of 10 mg/m2 per minute in all
patients on days 1 and 8, the cycle is repeated every 21 days. Dose escalation is
achieved by increasing the duration of infusion. The total dose of gemcitabine is
re-constituted in 500 ml of normal saline and infused through a peripheral or central
venous line.
5.2.1 Treatment courses
Prior to initiating treatment, eligible patients will be randomised to receive
gemcitabine given either in the standard short 30 minutes infusion, or constant rate
prolonged infusion over the duration determined in the phase I study. All patients in
both arms will receive carboplatin at a dose of AUC of 5 over 1 hour.
Standard arm
Carboplatin AUC of 5 over 1 hour, day 1, followed by Gemcitabine 1000 mg/m2 over 30
min, day 1 and 8 Cycle is repeated every 21 days
Study arm
Carboplatin AUC of 5 over 1 hour, day 1, followed by Gemcitabine 10 mg/m2/min at MTD,
day 1 and 8 Cycle is repeated every 21 days
Supportive treatment
- All patients should receive pre-medications to prevent nausea and vomiting
according to local policy.
- No prophylactic growth factors are allowed.
- Growth factor is allowed only in the rescue setting, eg. prolonged grade 4
neutropenia for more than 7 days, or for febrile neutropenia.
5.2.2 Dosing in cycle 2 and subsequent cycles
The next treatment cycle will begin on schedule providing
• There is no evidence of tumour progression
- Neutrophils ~ 2 x 109/L
- Platelets ~ 100,000 x 109/l
- Absence of grade 2 or above non-haematological toxicity
5.2.3 Dose modifications
5.2.3.1 General rules
- No intra-patient dose escalation is allowed.
- Any patient who requires a dose reduction will not be eligible for any dose
escalation for the remainder of the study.
- Treatment may be delayed up to day 35 to allow a patient sufficient time for
recovery from treatment related toxicity. Any patient who cannot proceed to the
next cycle by day 35 will be discontinued from the study.
5.2.3.2 Dose modifications based on haematologic toxicity
Adjustment based on day 8 count Platelets (x 109/l) ANC (x 109/l) Action > 75 and > 1.0
Proceed with day 8 dose > 75 and 0.5 - 1.0 Proceed with reduced dose 50 - 75 and ~ 0.5
Proceed with reduced dose < 50 and/or < 0.5 Omit dose When day 8 dose is reduced, the
same reduced dose will be used for the following cycle.
When day 8 dose is omitted, the cycle is completed, and the next cycle will be
scheduled on day 22, with dose reduction.
Dose adjustment based on nadir count Platelets (x 109/l) ANC (x 109/l) Action ~ 25 with
no bleeding and ~ 0.5 or < 0.5 for < 7 days No change < 25 or < 50 with bleeding and/or
< 0.5 for > 7 days Dose reduction (see below) Any and < 0.5 and fever Dose reduction
Recurrence of any of the above after 2 dose reductions Off study
Adjustment based on day 22 count Platelets (x 109/l) ANC (x 109/l) Action
~ 100 and > 2.0 Proceed with next cycle < 100 and/or < 2.0 Delay 1 week Maximum delay
of 2 weeks (next cycle must start by day 35 to remain on study)
Dose reduction schema First Reduction Second reduction Third reduction Carboplatin AUC
4.5 AUC 4.0 Off study Gemcitabine (standard arm) 750 mg/m2 (1000 mg/m2 x 75%) 500 mg/m2
(1000 mg/m2 x 50%) Off study Infusional Gemcitabine 75% of Phase II duration 50% of
previous infusion duration Off study
5.2.3.3 Dose modifications for non-haematologic toxicity
Any grade 3 or 4 non-haematologic toxicity, except for nausea and vomiting and fatigue
and reversible transaminitis, will render patient off study.
Non-haematologic toxicity must be less than grade 2 before proceeding to the next
cycle. If they are higher than grade 2, treatment is delayed for 1 week. Treatment may
be delayed for a maximum of 2 weeks.
5.2.4 Treatment duration
Responding patients will receive up to six cycles of chemotherapy.
After treatment completion or withdrawal, patients may continue to receive further
treatment at the discretion of their physician.
Screening evaluations
The following screening investigations must be performed within 28 days of day 1 of
cycle 1:
- Complete staging and documentation of tumour status - baseline chest x-ray, CT
thorax, abdomen, brain and bone scan if clinically indicated.
The following screening evaluations and investigations must be performed within 14 days
of the first dose of therapy and includes the following:
• Consent
• Complete medical history, include details of symptoms, prior treatments, any residual
toxicity, concomitant medical conditions and medications
• Physical examinations, including documentation of all palpable lesions, vital signs,
body weight and height, and KPS.
• Documentation of indicator lesion(s) to include date of assessment, description of
lesion site, dimensions, and type of diagnostic study to follow lesion. The same
diagnostic method must be used throughout the study to evaluate a lesion.
The following tests must be performed within 7 days of the first dose of therapy and
includes the following:
- Full blood count
- Serum electrolytes and liver enzymes, total calcium and magnesium
- Serum pregnancy test, if applicable
- Dipstick urinalysis - if dipstick is positive for protein or blood, a complete
microscopic examination is required
8.3 Evaluation during treatment
Prior to day 1 of each cycle
• History and physical examination
• Assess and record toxicities from prior course. Assign appropriate toxicity grades
(see Appendix 4).
• Record all medications taken since the last cycle.
• Weight measurement for re-calculation of body surface area and creatinine clearance
• Assessment of symptoms of disease (QoL questionnaire should be given and filled by
patient before assessment by investigator).
- Assessment of performance status
- Full blood count, electrolytes and liver enzymes (if day15 levels are abnormal).
- Urine dipstick analysis, if the baseline result is abnormal
- Clinical tumour measurements should be obtained prior to every cycle of treatment
- Radiographic tumour measurements should be obtained after every 2 cycles of
treatment.
- Modify dose of the next cycle if necessary (see section 5.2.3).
Day 8 assessment
• Full blood count
Day 15 assessment
• Full blood count, electrolytes and liver enzymes
8.4 Evaluation of response
Patients will be evaluable for response after 2 cycles of therapy. Clinical tumour
measurements should be performed prior to every cycle of treatment. Radiographic tumour
measurements should be obtained after every 2 cycles of treatment.
If a patient meets the response criteria (see section 7) for CR, PR or SD for the first
time, another clinical and radiographic tumour assessment will be performed 4 or more
weeks later to document that the response has lasted at least 4 weeks.
Clinical tumour assessment after every cycle and radiographic tumour response after
every 2 cycles will continue until completion of treatment or patient withdrawal.
8.5 Post-treatment follow-up
Responding patients will be reviewed every 2 monthly after completion of chemotherapy.
Clinical tumour assessment will be carried out 2 monthly. Radiographic tumour
assessment will be done every 4 monthly. These will continue until disease progression
is documented.
Patients who never had a response, and patients with disease progression after a
previously documented response will be followed every 3 monthly for survival data.
9. TREATMENT COMPLETION AND WITHDRAWAL
A patient will be considered as completing the treatment if:
- Patient has completed 6 cycles of therapy.
- Patient has a confirmed CR or confirmed PR and received at least 4 cycles of therapy
and the investigator does not feel further therapy is indicated.
- Patient maintained a status SD for at least 8 weeks on treatment and received at least
2 cycles of treatment.
- Patient has PD after completing at least one full course of treatment.
- A patient is removed from the study due to unacceptable toxicity.
Patients may be withdrawn from the treatment for the following reasons:
- Adverse experience, including intercurrent illness or unacceptable toxicity.
- If attending physician thinks a change of therapy would be in the best interest of the
patient.
- Protocol violation (including non-compliance).
- Patient withdrawal at his/her request, for reasons other than those above.
- Lost to follow-up.
All patients will be followed for status of disease and survival until death. 10. QUALITY OF
LIFE (QoL) ASSESSMENT
It is essential to explain to the patient that the QoL assessment is an important part of
the trial, and that all sections should be answered even if the patient feels them to be
irrelevant. It should be emphasized that the completion of these forms helps doctors find
out more about the effects of treatment on patients' well-being.
A named contact person other than the responsible clinician managing the patient in the
context of the trial, must be appointed to take responsibility for the administration,
collection and checking of the completed EORTC QLQ-C30 and QLQ-LC13 questionnaire. The
questionnaire must be taken before consultation with the clinician, according to the EORTC
guidelines for QoL assessment. They should be checked to ensure that all questions have been
answered; if necessary go back to the patient immediately and ask him or her to fill in any
missing items. If an assessment is missed because of administrative failure, the patient
should be contacted by telephone or letter and an arrangement should be made for the
questionnaire to be taken within a week of the scheduled assessment.
The questionnaire may be filled in by the patient if he/she is able to read and understand
the language of the questionnaire. Otherwise, the named person for administering the QoL
should read out the questions as written, in the language the patient understands, and
record the response to each question without prejudicing his/her answer. The mode of
delivery should be noted in the questionnaire.
11. RANDOMISATION PROCEDURE
Study participants will be randomly assigned to receive either gemcitabine given in the
conventional 30 minutes infusion, or protracted infusion, both in combination with
carboplatin.
11.1 Stratification
Stratified randomization will be carried out using the minimization method based on the
following factors:
(i) Centre (National University Hospital, Sydney Cancer Centre, Johns Hopkins-NUH
International Medical Centre) (ii) Karnofsky performance status (90 - 100% vs 70 - 80%)
(iii) Stage of disease (IIIB vs IV)
11.2 Registration
Patients will be entered into the trial by a telephone call to the National Medical Research
Council (NMRC) Clinical Trials & Epidemiology Research Unit (CTERU), Singapore (+65
220-1292) between 0830 to 1730 hours Monday to Friday, and 0830 to 1230 hours Saturday
(Singapore time), or by Fax (+65 220-1485), stating that the patient is to be entered into
the CTRG L08 or SQLU02 trial.
Informed written consent for entry into the study should be obtained prior to randomization.
All eligibility criteria and consent form will be checked, and the stratification factors
stated before treatment is allocated. The patient will be randomized to long infusional
gemcitabine (L) or 30- minute short infusion gemcitabine (S), and allocated a trial number.
The design will involve equal allocation of patients to the two treatments. Confirmation fax
will be sent to the investigator.
12. STATISTICAL CONSIDERATIONS
The sample size calculation is carried out based on the statistical selection theory
criterion as detailed in Simon et al (62) and Gibbons et al (63). Assuming a 90% probability
of correctly selecting the best treatment, and anticipating a baseline response rate of 40%,
then to detect a 15% superiority of the best treatment over the other, a trial size of 37
patients per treatment arm would be required. The total accrual target would thus be 74
patients.
13. STATISTICAL ANALYSES
Statistical analysis of all study endpoints will be carried out on an intention-to-treat
basis. In the event of lost to follow-up, patients will still be included in the analysis
for the duration that they are observed. The inherent comparability of results in this
randomized phase II design using the statistical selection theory assures that the two
treatments can be reliably ranked when large differences are obtained.
The best response will be used in the analysis of objective tumour response. In the case of
adverse event, where multiple events of the same kind has occurred in a patient, only the
maximum grade will be documented for the analysis. The tumour response rates and toxicities
between treatment groups will be compared descriptively using estimates of proportions.
The response duration and time to response for responding patients will be assessed using
appropriate descriptive statistics. The evaluation of progression-free and overall survival
will be carried out using the Kaplan-Meier technique at 1-year follow-up. In the case of
progression-free survival, patients whose disease has not progressed will be censored at the
date last known to be alive. Similarly, the analysis of overall survival censors patients
who are lost to follow-up or who remained alive at the date last known to be alive.
For each QoL dimension, changes in scores over time will be compared between treatment arms
by means of appropriate graphical representation or descriptive statistics.
No interim analysis is planned for this randomised phase II trial.
14. ETHICAL CONSIDERATIONS
14.1 IRB/Ethics committee
Before study initiation, the protocol will be submitted for review and approval by the
hospital and Ministry of Health research and ethics committee or equivalent group. Approval
of the protocol and informed consent must be obtained.
14.2 Patient information
The responsible physician will inform the patient about the background and current knowledge
of the treatment under study with special reference to known activity and toxicity. The
patient will be told about the investigative nature of this treatment and in particular, the
randomization process involved in this study. The patient will be told of his or her right
to withdraw from the study at any time without any penalty with regards to the continuation
of care at this institution and by the same physicians as he chooses. Before accrual, all
patients will sign a written, informed consent form.
14.3 Informed consent
Informed consent should meet the requirement of the latest revision of the Declaration of
Helsinki and any applicable regulations and guidelines such as the Good Clinical Practice
(Singapore).
The study will be completely explained to each prospective candidate and the subject must
give consent by signing and dating the consent form.
Consent must be obtained before any protocol-required procedures are performed, including
any procedures not part of normal patient care.
Plasma dFdC and dFdU levels
Ten millilitres of blood will be drawn at 0 hours (baseline), 10 minutes, 30 minutes, 10
minutes before the end of the infusion, and 30 minutes, 1 hour, 2 hours after the end of the
infusion. The blood will be drawn into 10 ml tubes (green topped) containing heparin and 5
micromol tetrahydrouridine. The tubes are then centrifuged at 3300 rpm for 15 minutes and
the supernatant plasma is then transferred to plain tubes (red topped) for immediate storage
at -80oC. Samples will be labeled with the patient's name, ID number, date, exact time of
sample and protocol number. A pharmacokinetic form will accompany the plasma samples to the
Pharmacology laboratory in the Department of Pharmacology, National University of Singapore,
c/o Prof Lee How Sung.
DFdC and dFdU levels in plasma will be measured using reverse phase HPLC, as described by
Grunewald (22). Briefly, 20 microl to 50 microl of plasma is injected onto a C18 mBondapak
analytical column (Waters Associates, Inc.). Components will be separated with a mobile
phase consisting of a 30 minute linear gradient starting with 100% solution A (0.5M ammonium
acetate, pH = 6.8) and ending with 60% solution B (50% methanol in deionised water). Flow
rate is at 1.5 ml/min. Detection wavelengths are 275 nm and 262 nm for dFdC and dFdU,
respectively.
16.2 Intracellular dFdCTP levels
Samples of blood will be collected to assay intracellular dFdCTP. Only 3 samples per
patient, obtained 10 minutes after the start and 10 minutes before the end of the infusion
of gemcitabine, and one in the middle of infusion, will be assayed for dFdCTP.
Plasma is first separated from the blood by centrifugation at 3300 rpm for 20 minutes.
Mononuclear cells are then isolated by Ficoll-Hypaque density gradient centrifugation and
deoxyribonucleoside triphosphates are extracted with 0.4 NHClO4, and the acid-insoluble
material is removed by centrifugation. The supernatant is then carefully neutralized to pH 7
with potassium hydroxide, and the precipitated KClO4 is then removed by centrifugation. An
ion-exchange high performance liquid chromatography method is then used to separate and
quantitate the dFdCTP.
17. STUDY ADMINISTRATION
17.1 Drug accountability
Stocks of gemcitabine will be supplied by Eli Lilly for trial purposes, and all these vials
will be accounted for at the site pharmacy.
17.2 Maintenance of patients records
CTRG clinical report forms will be used to record data for this study. All patient clinical
report forms will be faxed to the CTRG Office (+65 777-5545). A copy of each patients
eligibility report form, randomization report form (for phase II), study schedule, consent
forms, laboratory and radiological reports, and QoL assessment will be kept in the CTRG
Office. All records will be kept for a period of 6 years following the date of study closure
according to Singapore GCP guidelines
