Neoplasm Metastases Clinical Trial
Official title:
Prospective Multi-center, Single Blinded, Randomized, Controlled Trial of EUS-FNB(Endoscopic Ultrasonography-Fine Needle Biopsy ) and EUS-FNA(Endoscopic Ultrasonography-Fine Needle Aspiration ) on Solid Occupying Lesion
The purpose of this study is to compare the diagnosis accuracy of FNA and FNB biopsy on pancreatic, retroperitoneal, mediastinum and pelvic cavity solid occupying lesions.
The study subjects are divided into two groups: the EUS-FNA(22G EchoTip Ultra needles) Group
and EUS-FNB group(22G EchoTip ProCore needles).Take the malignant occupying lesion diagnosis
accuracy as the research major indicator to compare the EUS-FNB group and EUS-FNA group as
optimal efficiency test. Take the class I error a=0.05, class II error β=0.15, power=0.85.
Suppose the malignancy diagnosis accuracy is 80%, while that of FNB is 93%. The two trial
groups be randomly allocated in 1:1, suppose the malignancy cases take 70% of the whole
case, and considering the shedding factors , extra 20% cases should be included. So the
estimated cases numbers is 204 cases for EUS-FNB group and 204 cases for EUS-FNA group,
totally 408 cases in this trial.
Done by professional statistical people with randomized block grouping method and SAS 9.2
statistical software to generate randomized serial number(001—408)for the two groups in 1:1
manner. The serial numbers are the randomized grouping numbers for the trial patients, block
capacity is 8, totally 51 randomized block. The randomized grouping will be generated in
duplicate copies and sealed. One copy send to trial centers for patient allocating, and the
another copy be saved by the trial applicant unit. Every trail centers will be responsible
for the screening of qualified patients, rank them in visit time to get the randomized
grouping number so as to determine them goes to the EUS-FNA or EUS-FNB.The research people
and patients in all trial centers should not know the the randomized grouping number and
relevant groups. The group name will be sealed under scratch card. Every trial patients will
get a unique randomized number, and it will not change through out the whole trial.
Use the inclusion and exclusion criteria to observe the patients and do relative
inspections, and confirm if the patients qualified or not to the trial. Record the result of
last time test before the treatment. Although it is better to get the informed consent
before doing all kinds of observation and tests, if for some reason, the medical imaging
examination has completed, as long as the imaging examination was done within 3 weeks before
the needle biopsy, it can still be collect as baseline data (imaging examination can be done
at other hospitals, but the trial center should issue a new evaluation report 1 week before
the patient join the trial group); other lab test items done at 2 weeks before the needle
biopsy can still be collect as baseline data for pre-research use, but these tests should be
done at the trail center hospital so as to guarantee the data trace ability.
The investigators will do the needle passes for 4 times for all of them:the 1-2 needle
passes with Slow-Pull and the 3-4 needle passes with Vacuum suction.If no core tissues
obtained or the operator/onsite pathologist determine insufficient specimen after the
operations above, then remedy procedures will be done, the operator use proper puncture
method to continue the remedy biopsy.After the first round of needle biopsy, if the trial
patient cannot be diagnosed, by getting the agreement of the patient, the patient will be
cross-over to another trial group and do needle biopsy again on the same lesion 1 week later
with the method mentioned above.Without knowing the needle biopsy type, the cytologist and
pathologist evaluate the specimen quality and make diagnosis. Every specimen will be
independently evaluated and diagnosed by 2 experts. If the 2 experts have different
judgments, then these two experts discuss together and make the final diagnose discussion.
If the same sample has 2 or more cytology smear slides, than take the highest score slide as
the result.Follow up (outpatient follow up or telephone follow up) the patients at 1 week,
12 weeks and 36 weeks after the needle biopsy and collect the patients clinical data and
confirm their final diagnosis.
During the trial, if severe adverse event occurs, the trialed center must take immediate
actions necessary to guarantee the trialed patients' safety. Once severe adverse event
occurs, the researchers should inform the trial applicant and the trail center's ethics
committee within 24 hours after the researchers gets to know the adverse event. And the
researchers should also fax the report to State Food and Drug Administration of China and
the local provincial food and drug administration. After receiving the report, the applicant
should inform other clinical trial centers within 24 hours. All the severe adverse events
should be filed at group leader medical center and other trial centers.
CRF(Case Report Form ) will be filled by the researchers, every involved patient must have
the CRF(Case Report Form ) filled. This will be audited by clinical monitor and handed over
to data administrator to input and manage data, the first copy will be kept by the
applicant, the second copy will go to the trial center, and the third copy will be kept by
the trail researchers.The data input and management will be taken care by specially assigned
person. In order to guarantee the data accuracy, data input will be done twice by two
independent data administrators, by computerized and manual verifying, hand over the data to
statistical experts to do blind check and statistic analyzing.For the questions and doubts
within the case report form, the data administrator make DRQ and via the clinical monitor
asking the researchers. The researchers will answer and feed back as soon as possible.
According to the researchers answer, data administrator will do the data modifying,
confirming or inputting, and when necessary send out DRQ again.After blind audition and
confirming that the established data base is correct, major researchers, applicant and the
statistic analyzing people lock the data. The locked data will not be changed, and the data
base will be handed over to statistical analyzer to do the statistic analyze according to
the statistic analyzing plan. Problems found after data locking can be modified during the
statistic analyzing procedure.This will be done by specialized statistic analyzing people
according to the predetermined statistic analyzing plan. The statistic analyze will be
carried out according to intention principle confirmed full analysis set and per-protocol
set principle. After completing the statistic analyzing, the statistic analyzer issue the
statistic analysis report and send this to major researchers to write the study report.
Statistic analyzing plan:⑴ General principle:① all the statistic tests are use the
two-tailed-test method, P<0.05 will be thought as the tested difference is statistical
significance. ② the quantitative indicator description will calculate the Mean and Standard
deviation. The classification indicator description will describe the cases and percentage
of all types of cases. ⑵ Statistic analyzing method:① for the measurement data, compare it
with the baseline value at selection period, use paired t-test or symbol rank sum test to
compare with the before-after-difference within the group.② for the counting data, use x2
test to compare the groups. ⑶ Shedding analysis:Comparison of groups'total shedding rates
and the shedding rates caused by adverse events will use x2 test or Fisher's exact test
method. ⑷ The baseline value's equilibrium analysis: Use group t test or x2 test to compare
the demography info and vital signs, disease history, and basic treatment and other
indicators of baseline value, so as to measure the balance of the groups. The baseline
evaluation will be done on FAS(full analysis set) and PPs(per-protocol set). ⑸ Effectiveness
analysis:The major indicator of effectiveness analysis is the diagnostic accuracy on
malignant disease, and the indicators of second effectiveness include the percentage of
Grade A specimen and complications rate etc. while the two groups rate and the Youden index
comparison will use approximate normal Z test or use central effect x2 test.(6) Safety
analysis:Use x2 test or Fisher's exact test to compare the adverse event/adverse reaction
(include biopsy complications) rates between the groups. And use table to describe the
adverse events during this trial project; the lab test results before and after the trial,
the normal/abnormal changing condition and the relationship with this trial research when
abnormal changes happened.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Diagnostic
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