Colorectal Cancer Clinical Trial
Official title:
Sorafenib Plus Capecitabine Efficacy Assessment in Patients With Advanced Pre-treated Colorectal Cancer
Prospective non-randomized phase II study assessing the activity of the Capecitabine-Sorafenib combination by estimating overall survival of the study population at a fixed time point (6 months) and, as an exploratory analysis the overall survival of metabolic responders versus non-responders.
Treatment doses :
Sorafenib 200mg in the morning,400mg in the evening; escalation to 400mg twice daily after 1
cycle Capecitabine 850mg/m2 twice daily Oral Days 1-14, weeks 1-2
Fluoro-Deoxy Glucose Positron Emitting Tomography (FDG-PET)imaging at baseline and after
17-21 days while on therapy.
Sample size justification/statistical analysis
Sample size has been estimated in order to be able to test the null hypothesis that the
overall survival rate at 6 months is less than 30%. This hypothesis will be tested using a
binomial distribution. The study should be able to reject the null hypothesis, using a
1-sided test with α = 0.025, with a power of 90% in case of a true overall survival ≥ 50%
(rate at 6 months). The sample size required is 66 eligible patients (to be followed for 6
months minimum). Analysis will be done on all registered patients using an ITT approach on
all eligible patients.
A co-primary endpoint is to compare the overall survival of patients assessed as early PET
responders and of patients assessed as early PET non responders (the clinicians will remain
blinded for PET response assessment). For this primary analysis, patients who will undergo
the second PET assessment will be eligible and time zero for measuring survival will be the
date of this second PET examination. It is anticipated that 95% of the patients will be
eligible for the analysis with a 50% expected rate of early PET non-responders (result
obtained from an unpublished study conducted at Jules-Bordet Institute). With 66 patients
registered, we anticipate then that 63 patients will be available for the co-primary
endpoint. With 63 patients and our assumption that the HR for the comparison between the
survival distributions will be around 0.385 (based on the previously mentioned unpublished
study), we will need using a two-sided logrank test at the 2.5% level (2.5% chosen because
of the existence of 2 co-primary endpoints), 54 events (power of 90%). With 63 patients and
a follow-up after accrual of 1 year, we should reach this number of 54 events. However, to
account for another possible 5% drop-out (patient's refusal for undergoing the second PET
examination for instance), sample size should be increased to 70 eligible patients.
However, our estimation of 50% expected rate of early PET responders is coming from a
prospective unicentric cohort of 38 patients undergoing chemotherapy for 1st line or 2nd
line treatment of advanced colorectal cancer with a few of them having received biological
agents together with chemotherapy. Our estimation may then not be reliable due to small
sample size and different patients population. If this rate of early PET responders proves
to be higher, we should be prepared to increase our sample size for targeting the same power
of 90%. For instance, if the rate is 67% instead of 50%, the required number of events would
be 62 in-stead of 54. If the rate is 75%, the number of events should be increased to 73.
The number of patients would have then to be adapted according to the rate of evaluable
patients for this PET objective and the rate of patients lost to follow-up. For reassessing
the required numbers of events, we did not change our hypothesis of detecting, if true, a
hazard ratio of 0.385 in favor of early PET responders.
We plan, during the course of accrual, to assess the rate of patients evaluable for the PET
objective, of early PET responders and, if possible the rate of patients lost to follow-up
in order to check whether we need to review our planned sample size. However, no interim
analysis will be done on the primary endpoints.
Secondary endpoints are to estimate progression-free survival and objective response rate,
and to describe the adverse reactions associated with the study regimen in the study
population. Also, to determine the correlation of early metabolic response, as assessed by
FDG-PET/CT immediately before the first and the second cycles of treatment with the study
regimen, with overall survival, progression-free survival, and response rate, and to
determine the correlation of growth modulation index (GMI), defined as the time to
progression under the study regimen over the time to progression under the latest regimen
administered to the patient, with overall survival and progression-free survival.
The study is designed as a single-arm phase II study, with all patients accrued in one
stage. No early stopping rules will be used.
;
Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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