Esophageal Cancer Clinical Trial
Official title:
Non-endoscopic Esophageal Cancer Screening Program in Northern Iran
The aim of this study is to assess the effects of implementation of a non-endoscopic esophageal cancer-screening program on outcomes of interest in an asymptomatic high-risk population in Golestan Province, Iran. Study population will be recruited in two arms. In the intervention arm, cytological examination of the esophagus will be performed using a capsule sponge device. Subjects in the control arm will receive no intervention. All participants will be followed for 5 years. The outcomes of interest, including the incidence of esophageal cancer as well as mortality rates, will be compared between the two groups.
Background:
Esophageal cancer (EC) is the 8th most common cancer and the 6th most common cause of death
from cancer worldwide. Golestan province located in Northern Iran has been known as a
high-risk area for esophageal squamous cell carcinoma (ESCC). Recent reports suggest an
increasing rate of esophageal adenocarcinoma (EAC) in this region as well. Designing and
implementing of screening programs may be effective for controlling these cancers. The
investigators aim to develop a screening program for esophageal cancer in this region. The
pilot phase of this project, the Golestan EC Screening Program (GESP), was conducted during
2011 and 2012 among 300 asymptomatic participants of Golestan Cohort Study (GCS), which is a
prospective population-based cohort of 50,045 individuals, aged 40-75 years at baseline, in
the eastern half of Golestan Province, Iran. The initial results of the GESP project showed a
low participation rate for endoscopic screening. In other words, endoscopic ESCC screening
was not feasible in our population, suggesting the need for a non-endoscopic screening
method. Further results of the GESP project suggested that capsule sponge cytology is a
feasible and valid primary method for ESCC screening in this region. Because of the promising
findings of the GESP project, it has been decided to start the main phase of the EC screening
program, called the "Non-endoscopic EC Screening Program in Northern Iran (NESP)". The aim of
this study is to assess the effects of implementation of a non-endoscopic EC screening
program on outcomes of interest in an asymptomatic high-risk population in Golestan Province,
Iran.
Methods:
For sample size calculations, the investigators considered different scenarios based on the
published literature and unpublished data. The prevalence of high grade dysplasia in the
general population of Golestan has been estimated to be 1.4-3.6%. The sensitivity of
cytological detection of esophageal squamous dysplasia (ESD) was predicted to be about 46%
based on studies from China, and 60-100% based on studies from Iran, and according to
previous studies, 27-65% of ESD lesions progress to invasive ESCC without treatment. The
investigators used a rather conservative assumption to calculate sample size: a dysplasia
prevalence of 1.5%, a 60% sensitivity for the sponge cytology, and a 2% progression to
invasive ESCC in the screened (and treated) group vs. 40% in the untreated group. The
investigators also assumed a power of 90%, a mean cluster size of 28 based on the PolyIran
study (CV=0.84%), and an intra-class correlation (ICC) of 0.01. Based on these assumptions
the investigators will need 4980 people in each arm. So, the investigators need to enroll
9,960 GCS participants > 50 years old. Estimating a 20% lack of consent, the final invitation
lists of NESP project will consist of 12000 GCS participants including 6000 subjects in the
intervention (capsule sponge) arm and 6000 subjects in the control arm.
A list of 12000 subjects from GCS participants will be prepared. Sampling will be done using
a cluster randomization method. Each village will be considered as a cluster. Clusters will
randomly be allocated into two groups, the intervention group (group 1) and the control group
(group 2). Capsule sponge examination will be performed for all subjects in intervention
clusters. But, participants in control clusters will be enrolled without capsule sponge
examination. Both intervention and control subjects will be offered endoscopy if they develop
upper GI symptoms according to current clinical practice.
The process of data collection and sampling will be performed at the community level. The
NESP enrollment team will go to healthcare houses located in each village and data collection
and sampling will be done there.
After obtaining informed consent, a structured questionnaire including data on demographic,
socioeconomic status and medical history will be completed for each subject. Subjects will
also be asked to fill in a quality of life (QOL) questionnaire. The investigators will use
the validated Persian version of the WHOQOL-BREF questionnaire which was basically developed
by the WHO.
Then the capsule sponge examination will be performed for each subject in the community
clinic after an overnight fast. The cytological specimen will be placed in preservative fluid
and transferred to the histopathology lab.
Cytological specimens will be processed into paraffin blocks, and slides will be prepared
from each paraffin block and will be stained using the hematoxylin and eosin (H&E) method.
Cytological examination of the capsule sponge H&E slides will be done by expert pathologists.
The result will be reported according to the Bethesda system. All subjects with cytological
diagnosis of atypia will be referred to Atrak clinic (a central clinic for upper
gastrointestinal disease in Gonbad, Iran) for endoscopic examination. Endoscopic examination
with Lugol's iodine staining will be performed by previously described methods and biopsies
will be taken from abnormal lesions. Histological examination of endoscopic biopsy samples
will be done by expert pathologists. If the results of the endoscopic examination show
high-grade dysplasia or cancer, the subject will be referred for treatment. These subjects
will be treated with endoscopic mucosal resection (EMR) and/or radiofrequency ablation (RFA).
Participants will be followed annually according to the protocol of the GCS follow-up. Each
subject will annually be contacted by a telephone call, and questions about the subject's
vital status and cancer incidence will be asked from the subject or a first-degree relative.
In addition, official data on subject's vital status will be obtained from the death registry
unit in the Department of Health of Golestan University of Medical Sciences. Data on cancer
incidence in the study subjects will also be obtained from the Golestan population-based
cancer registry.
Both groups will be followed for 5 years. At the end of the study, the QOL questionnaire will
be completed again for all available subjects.
The risk of developing outcomes will be compared between the intervention and control groups.
Odds ratios and 95% confidence intervals (CI) will be calculated. Survival analysis will be
done to assess survival rates in the sponge and control groups. The log rank test will be
used to compare the survival rates between the two groups. Hazard ratios and 95% CI will be
calculated for different variables using Cox regression analysis. Changes in QOL scores
during the 5 year follow-up period will be compared between the sponge and control groups.
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