Biliary Cancer Clinical Trial
Official title:
Covered Versus Uncovered Self-conformable Metal Stent for Palliation of Primary Malignant Extra-hepatic Biliary Strictures: a Randomized Multicenter Study
The purpose of this study is to compare the duration of stent patency of a covered vs. an uncovered biliary self-expandable metal stents (SEMS) placed to relieve biliary obstruction in patients with inoperable extrahepatic malignant biliary obstruction.
Cancer of the pancreas, gallbladder, or bile ducts is the most common cause of malignant
obstruction of the biliary tree. Patients who have unresectable tumors have a dismal
prognosis in terms of survival and quality of life. In these cases 5-year survival is less
than 2% and palliation, such as the establishment of a biliary drainage, is the only
treatment available. Two types of stents are routinely used: plastic stents (PS) and
self-expandable metal stents (SEMS). The first generation SEMS are uncovered and recurrent
obstruction, most frequently caused by tumor ingrowth through the metal mesh, is seen in
16-46%. Recently, covered SEMS have been introduced to prevent tumor ingrowth. Covered SEMS
are associated with stent occlusion in 14% of patients. As can be expected, the most
frequent cause of stent obstruction in these patients is sludge formation. Stent migration,
and cholecystitis and pancreatitis caused by obstruction of the cystic duct and pancreatic
duct, respectively, have been suggested to occur more frequently with covered SEMS. To date,
however, one randomized trial and three comparative studies compared covered with uncovered
SEMS, have found only a non statistically significant trend towards more frequent occurrence
of these complications.
From these initial studies comparing uncovered to covered SEMS, it suggested that stent
patency may be longer with covered SEMS. However, supporting evidence for the superior
efficacy of covered SEMS is lacking. In addition, the issue of safety of covered SEMS, as
well as the real world effectiveness of the self conformable SEMS, warrant further
investigation.
In this study, the Investigators will include patients with symptoms (jaundice, cholangitis)
due to malignant extrahepatic biliary tree obstruction (pancreatic cancer,
cholangiocarcinoma, gallbladder cancer, or metastatic lymphadenopathy) who are not
candidates for surgical cure either because the tumor is inoperable or because of the
patient's poor medical condition due to comorbidities and/or advanced age.
Patients with extrahepatic malignancy in whom a diagnostic work up is still ongoing to
establish the possibility of performing a curative approach will not be immediately
enrolled. Patients who have been previously treated with a plastic stent will be eligible if
the plastic stent was placed within the 4 weeks prior to enrolment in this study.
The purpose of this study is to compare the duration of stent patency of a covered vs. an
uncovered biliary self-expandable metal stents (SEMS) placed to relieve biliary obstruction
in patients with inoperable extrahepatic malignant biliary obstruction.
1. Primary Aim: To compare the duration of stent patency of a covered vs. an uncovered
biliary SEMS placed to relieve biliary obstruction in patients with inoperable extrahepatic
malignant biliary obstruction.
Secondary Aims:
In patients with inoperable extrahepatic malignant biliary obstruction managed with SEMS:
1. To evaluate complication rates of covered vs. uncovered biliary SEMS
2. To evaluate the quality of life before and after intervention with covered vs.
uncovered biliary SEMS
3. To evaluate the survival of patients treated with covered vs. uncovered biliary SEMS
4. To evaluate the cost-effectiveness of covered and uncovered biliary SEMS
5. To determine the predictors of survival in patients in patients with inoperable
extrahepatic malignant biliary obstruction managed with SEMS.
1.1 Primary endpoints
- Normalization of the bilirubin level and other cholestasis parameters
- Absence of clinically significant stent occlusion or migration prior to death of
patients (minimum follow-up: 4 months) as defined below Clinically Significant
Occlusion
It will be defined as an occurrence of the following items:
- The development of clinical symptoms of biliary obstruction such as cholangitis,
accompanied by jaundice and fever requiring antibiotic treatment, and pruritis
- Laboratory evidence of cholestasis, including elevation of conjugated bilirubin (≥ 30%
increase in bilirubin), alkaline phosphatase (ALP), aspartate aminotransferase (AST)
and alanine transaminase (ALT) following stent placement
- Imaging findings consistent with biliary obstruction Initial stent failure: if
normalization of bilirubin level and other cholestatic parameters does not occur
immediately after SEMS placement.
1.2 Secondary endpoints
- Health-related quality of life (HRQL) (evaluated monthly)
- Complications (perforation, haemorrhage, pancreatitis, cholecystitis, cholangitis,
stent migration [into the duodenal lumen by ≥ 1 cm], sludge occlusion, severe pain,
tumor in- and over-growth, infection, haemorrhage, stent fracture and shearing, stent
cover disruption) major and minor.
- Overall survival post stent placement
- Quality adjusted life years (QALYs)
- Costs of treatment strategies
- Occurrence of biliary re-intervention, defined as any endoscopic, percutaneous or
surgical procedure to improve biliary drainage after the stent placement
- Procedure time (stent deployment)
- Technical complications of the tested endoscopic devices. Population: The study
population will include patients with symptoms (jaundice, cholangitis) due to malignant
extrahepatic biliary tree obstruction (pancreatic cancer, cholangiocarcinoma,
gallbladder cancer, or metastatic lymphadenopathy) who are not candidates for surgical
cure either because the tumor is inoperable or because of the patient's poor medical
condition due to comorbidities and/or advanced age.
Patients with extrahepatic malignancy in whom a diagnostic work up is still ongoing to
establish the possibility of performing a curative approach will not be immediately
enrolled. Patients who have been previously treated with a plastic stent will be eligible if
the plastic stent was placed within the 4 weeks prior to enrolment in this study.
Materials Fully covered SEMS: Niti-S Biliary ComVi Stent; Uncovered SEMS: Niti-S (D type)
stent Sample size calculation: The primary end point of the study is stent occlusion. The
number of patients in each group required to demonstrate a statistically significant
difference in SEMS patency with an 80% power is 70 for a 22% difference,121 for a 17%
difference, and 248 for a 12% difference in the obstruction rate between the two groups.
Estimated sample size is 121 for a 17% difference, and 70 for a 22% difference.
With a lower (75%) power, 63 patients per treatment group are required to detect a
difference of 22%, 108 for a 17% difference and 222 for a 12% difference. This computation
is based on data on obstruction percentage reported in literature.
The target enrolment for this study will be 70 patients per study arm. Considering time to
occlusion analysis, a total of 140 patients will detect a treatment difference at a two
sided 0.05 significance level, with 80% power, if the true hazard ratio is at least 1.76.
Treatment of data Data storage, management, and analysis will be centralized. An electronic
database will be constructed to collect the data. The program will be distributed to all
participating centers and the data will be entered at the time of the encounters with the
subjects such as at the time of endoscopy for stent placement, follow-up visit, or follow-up
telephone call. Randomization assignment (stent type) will be coded. Standard operating
procedures for regularly backing up the data will be employed at each facility and
centrally.
Every 6 months the compact disk (CD) with the study site data will be sent to the
coordinating center where the data manger will download the data and merge it with the
previously collected study data.
Security measures will be adopted before the mailing of the CD in order to avoid any
possible disclosure of the privacy: the data will be encrypted and transformed in numbers.
The data manager will remove information regarding the type of SEMS used prior to sending
the data to the statistician. Therefore, data analysis will be performed by a statistician
who is blinded to the type of stent.
Data sheet
- Baseline and enrolment visit (Day 0)
- Follow-up visits (1 week, 1 month, 3 and 6 months after stent placement)
- Specific Exams/Tests required Stent placement procedure (Day 0) The patients who agree
to participate and who sign a Patient Consent will be enrolled in the study; prior to
enrolment, the investigator will provide thorough explanation of the study procedures.
Clinical data (Form A):
- patient demographics (gender, age)
- medical history related to diagnosis and history
- concomitant medications and treatments
- endoscopic and/or MRI and/or CT-scan exam for confirmation and location of stent
- stenosis (the endoscopic examination could be done immediately before the stent
placement procedure)
- liver function tests
1 week, 1 month, 3 and 6 months after placement (Form B):
- liver function tests
- concomitant medications and treatment
- confirmation of stent position via supine X-ray
- Complications 1. week, 1 month, 3 and 6 months after placement (Form E): HRQL
questionnaires Analysis Descriptive statistics, including graphical displays, will be
used to summarize all study variables. The unit of analysis will be the patient. For
continuous variables, means, medians, standard deviations, percentiles, ranges, box
plots and histograms will be generated. For categorical variables, frequencies and
proportions will be generated. The investigators will examine all variables to
determine if parametric distributional assumptions (e.g. normality for the continuous
variables) are valid.
Differences between continuous variables will be determined by parametric tests, or, when
appropriate by non-parametric tests. Differing frequencies of variables at different times
within each group (dysphagia score, body weight, etc) will be compared with tests for
related samples.
To address the primary aim, differences in duration of stent patency, the Kaplan-Meier
method will be used to estimate stent patency in each group and the log-rank test will be
used for an unadjusted comparison between groups. Then a Cox proportional hazard model will
be constructed to compare time to stent occlusion adjusted for important potential
confounders. Stent patency will be calculated in days and will represent the interval
between the time of stent insertion and the time of its replacement or the death of the
patient with concomitant cholangitis.
To address the secondary aims, relationships between complication rates and stent type will
be examined by the chi-square or the exact Fisher tests. Logistic regression will be used to
compare stent complication rates adjusted for important potential confounders.
Health-related quality of life (HRQL) will be evaluated by a paired t-test to determine the
impact of stent placement (i.e. compare baseline HRQL and month 3 HRQL) by Student's t -test
to compare the differences in HRQL at baseline and 3 months between study groups. Linear
regression models will be constructed to assess HQRL while adjusting for factors other than
stent type. Total direct costs for each study group will be compared and cost effectiveness
modelled.
For all analyses the Statistical Package for Social Sciences software (SPSS, Inc. for
Windows will be used.
Adverse events are defined as any undesirable experience occurring to a subject during a
clinical trial. All adverse events reported spontaneously by the subject or observed by the
investigator or his staff will be recorded.
A serious adverse event is any untoward medical occurrence or effect that at any level
results in death:
- is life threatening (at the time of the event)
- requires hospitalisation or prolongation of existing in patients' hospitalisation
- results in persistent or significant disability or incapacity
- is a new event of the trial likely to affect the safety of the subjects, such as an
unexpected outcome of an adverse reaction, lack of efficacy, major safety finding
Withdrawal of individual subjects Subjects can leave the study at any time for any
reason if they wish to do so without any consequences. The investigator can decide to
withdraw a subject from the study for urgent medical reasons.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Supportive Care
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