Colorectal Cancer Clinical Trial
Official title:
Screening of Colorectal Cancer Using Improved SEPT9 (Septin 9) Gene Methylation Assay in Chinese Population
The purpose of this study is to evaluate the performance of the SEPT9 gene methylation assay in Colorectal cancer (CRC) high-risk population in Chinese hospitals using the opportunistic screening method. The trial plans to evaluate a Chinese domestic SEPT9 assay kit produced by BioChain (Beijing) Science and Technology Corporation, who is a close partner of Epigenomics AG, the producer for Epi proColon 2.0 CE.
1. Background
Colorectal cancer (CRC) is the third most common malignancy of the gastrointestinal
system. Regular screening, early detection and early treatment of colorectal cancer can
achieve better prevention and even cure. Currently, 60%-70% of CRC patients are not
diagnosed until late stages and only 11.8% of cases are detected at early stage. It is
therefore urgent to reduce the CRC mortality by improving the early screening rate. In
China,fecal occult blood test (FOBT) and colonoscopy are available presently for early
CRC screening. FOBT is widely used due to its low cost and non-invasiveness, however,
its false positive rate is relatively high due to many interfering factors. The more
advance FOBT, fecal immunochemical test (FIT), has greatly improved the test
specificity compared with the traditional chemical method and its compliance is high,
but is still subject to the influence of other intestinal diseases, leading to low
positive predictive value. In contrast, the compliance for colonoscopy is low due to
its invasiveness, cost and risk of complications.
In recent years, the plasma-based SEPT9 gene methylation assay has proved to be a
promising method for the early detection of CRC. Many clinical studies have
demonstrated that the methylated SEPT9 gene is a useful biomarker for early CRC
detection.At present, Epigenomics' Epi proColon 2.0 CE is the only commercialized assay
of SEPT9 gene methylation globally. This product has obtained the approval from the
European Union CE certification, the Chinese FDA and the Argentina FDA. It has
completed key clinical data submission to the US FDA, with reasonable expectation of
the US FDA approval soon. Services based on the SEPT9 gene methylation assay are also
provided in clinical laboratories such as quest, Arup, companion to DX and gamma
dynacare with the common medical procedure code (CPT code) 81401. In China, BioChain
(Beijing) Science and Technology, Inc, a strong partner of Epigenomics AG, has
developed its own SEPT9 gene methylation assay with the agreement of Epigenomics AG.
2. Estimation of sample size
Based on the equation N=Z2* (P (1-p))/E2 for known positivity detection rate, the
investigators calculated the number of samples needed for the trial, in which N
represents the sample size, Z is a statistical parameter (Z=1.96 for 95% confidence
interval); E represents the error (5% was chosen in this study), and P represents the
probability (putative positive detection rate). The investigators choose 0.75 for P
value based on existing literatures on SEPT9 sensitivity. The number of CRC cases is
calculated as 288 based on the equation above. The investigators aim to collect
complete information for 300 cases due to information incompleteness and tracking loss.
etc. Based on the estimation that CRC account for 30% of high-risk outpatients and
inpatients in Chinese hospitals, the total number of patients in the trial should be no
less than 1000 cases. The investigators aim at recruiting 1200 cases in this trial
taking account of 20% loss of follow-up rate.
The final actual number of cases for this trial was 1031, due to loss of tracking,
incomplete test or clinical data, or samples that did not meet the test criteria.
3. Subject grouping
All patients will not be grouped before blood draw for SEPT9 assay, and blood samples
will be obtained for all subjects who met the selection criteria. All the technicians
are blinded to the clinical information of subjects. In order to investigate the
feasibility of joint detection with SEPT9 assay and other screening tests,
carcino-embryonic antigen (CEA) and FIT tests will be performed at the will of
participating patients and the judgment of physicians. This part of data will be used
in a retrospective analysis after the completion of the trial.
When all planned tests are finished, all subjects will be divided into three groups
based on colonoscopy diagnosis and pathology, the CRC group, the precancerous disease
group and other disease group, in which the CRC group consists of patients with stage
0-IV CRC, the precancerous disease group includes patients of adenoma and polyps, and
other disease group includes patients of other bowel disease, other cancers, and
subjects with no evidence of disease.
4. Trial procedure
Training will be finished before the trial starts including the operation procedure of
the assay and the use of kits and instruments. This trial is a randomized, single-blind
study. All patients should sign the informed consent before blood draw of 10ml. Samples
will be processed and the SEPT9 assay will be performed based on the instructions for
users. All subjects will receive colonoscopy and/or pathological examination to confirm
the diagnosis, and the results for SEPT9 assay will be decided based on the
instructions for users. Statistical analysis will be performed based on the results
from both SEPT9 assay and colonoscopy and/or pathological examination.
5. Sample collection and storage
1) sample collection:
1. sample should be collected from outpatients or inpatients and the sample information
should be recorded in sample collection forms.
2. sample collection: 10 mL peripheral blood (K2EDTA decoagulant only).
3. in order to ensure the accuracy of the assay, sample collection should be performed
strictly based on the above requirements, otherwise it may affect the accuracy of the
assay.
2) sample storage and transportation method: Store and transfer the samples based on the
instructions for use of the kit
6, SEPT9 assay
SEPT9 gene methylation assay (PCR fluorescence probe method) is composed of two steps.
Firstly, the cell-free DNA in plasma is extracted using the plasma processing kit, followed
by bisulfite conversion, in which the unmethylated cytosine will be converted while the
methylated cytosine will not. Secondly, real-time PCR using bisulfite-converted DNA (bisDNA)
as the template will be performed to determine the amplification of template. PCR blocking
agent and methylation-specific probes can work together to distinguish between methylated
and unmethylated DNA. Beta-actin will be used as the internal control to evaluate the plasma
DNA quality and the validity of PCR amplification. Positive and negative controls will be
provided in the kit as quality controls and will be run parallel with samples each time.
7,Data analysis and statistics
The data for SEPT9 assay and the data of colonoscopy of all subject will be collected and
analyzed, the following parameters will be calculated:
Sensitivity Specificity Consistency positive predictive value (PPV) negative predictive
value (NPV)
8,Ethics
The budget plan for the clinical trial will be submitted to the ethic committee of
participating hospitals for review before the clinical trial starts. The study will not be
initiated unless the approval by the committees. All subjects will sign the informed consent
before blood collection, and will be informed the usage of plasma and the test results.
9, Research progress
2014.02-2014.04 Confirmation of clinical trial protocols and training of personnel for
sample collection and test
2014.04-2014.08 Submission of clinical trial application to ethics committee for approval in
four hospitals
2014.08-2015.04 Start patient recruitment and collection of general information of subjects
2014.10-2015.04 Sample collection and tests
2015.04-2015.07 Collect and track the colonoscopy and/or pathology information
2015.07-2015.09 Data processing, statistics and analysis
2015.10 Close of patient recruitment and finish of the trial
10,Budget
The costs include expenses for recruiting 1200 subjects, equipment rent charges, test
material costs, sample processing fee, labor costs, patient compensation costs, travel and
conference costs, publication and intellectual property (IP) fees. All expenses will be
covered by BioChain, as this trial is initiated and organized by BioChain.
11,Publication and intellectual properties
1. plan to publish 2-3 papers in science citation index (SCI)-indexed journals, 3-4 papers
in Chinese domestic core journals.
2. plan to submit one patent
12, Data management
Quality of clinical trial data is the basis for evaluation of results. To ensure the reality
and reliability of experiment results, the investigators set up a series of data management
principles. The investigators will explain data management principles in this study
thoroughly in the following from the composition and responsibility of Data Management
Committee and content of data management.
13.Research team and personnel
In order to avoid the possible errors caused by difference in disease incidence and ratio of
patients in different hospitals, four hospitals in Beijing will be chosen for patient
recruitment in this clinical trial. Since patients in these four hospitals are mainly from
northern China, the study population is representative for disease epidemiology in this part
of the country. Doctors and technicians from the department of gastrointestinal diseases,
endoscopy and general surgery from the four hospitals will participate the trial, they are:
Peking Union Medical College Hospital (Beijing) Beijing Military General Hospital (Beijing)
Cancer Hospital Chinese Academy of Medical Sciences (Beijing) Beijing Cancer Hospital
(Beijing)
;
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