Colorectal Neoplasms Clinical Trial
Official title:
Analysis of Intestinal Microflora Combined With DNA Methylation in Stool to Detect Colorectal Cancer: a Study Protocol for Colorectal Neoplasms Screening
Introduction: Colorectal cancer (CRC) has the third highest incidence rate and the fourth
mortality rate in the world. Traditional colonoscopy as an invasive examination method cannot
be widely used in screening for colorectal neoplasia. The fecal immunochemical test has some
limitations in sensitivity. Also, race and regional differences may affect results.
Abnormality in the composition of the gut microbiota has been implicated as a potentially
important etiologic factor in the initiation and progression of colorectal cancer. Analyzing
fecal flora and exfoliated cell genes may represent a new screening tool for colorectal
cancer.This research aims to use 16S rRNA to compare differences in fecal flora between
colorectal cancer patients and healthy controls. These data combined with DNA findings of
fecal exfoliated cells may further clarify this difference to build a model for screening
early colorectal cancer in Chinese people.
Methods and analysis: In total, 300 patients with positive colonoscopy results and 200 health
controls will be recruited. All participants will complete an information form and
questionnaires. Fecal samples will be examined by 16S rRNA analysis. Gene methylation levels
will be detected in fecal exfoliated cells. Models of related intestinal microbiota and
methylation genes will be built. Receiver operating characteristic (ROC) curve analysis will
be used to select some models with appropriate sensitivity and specificity.The models will be
further validated by multicenter studys.
Introduction: Colorectal cancer (CRC) has the third highest incidence rate and the fourth
mortality rate in the world. In China, CRC is the fifth leading cause of cancer deaths.
Age-standardized incidence rates in CRC have shown an upward trend.A Westernized lifestyle,
particularly physical inactivity, and an increase in the prevalence of obesity in recent
decades in China may explain the increase in CRC incidence .
The 5-year survival rate for people with CRC is 65%. Survival rates for CRC can vary
depending on various factors, particularly cancer stage. The 5-year survival rate with
localized-stage CRC is 90%. About 39% of patients are diagnosed at this early stage. Because
of the lack of typical clinical symptoms, early CRC is difficult to detect, and most patients
are already in the advanced stage when CRC is diagnosed, thus missing the best intervention
stage. Therefore, early detection and early treatment are effective means to reduce the
mortality with CRC. Screening has benefits, including diagnosis at an earlier stage, reduced
incidence of CRC and reduced mortality.
At present, the main screening methods for CRC are fecal occult blood test and colonoscopy.
Colonoscopy is the gold standard for screening for CRC. However, traditional colonoscopy, an
invasive examination method, cannot be widely used in screening for colorectal neoplasia.
Fecal samples are easily obtained.Using feces to screen CRC is the current research
consensus. According to the most updated Asia Pacific consensus recommendations for CRC
screening,FIT(fecal immunochemical test) is used to select high-risk patients for
colonoscopy. FIT has also been widely used in other world regions . The sensitivity of FIT is
limited (0.79; 95% CI, 0.69-0.86), and a recent systematic meta-analysis showed wide
variation in sensitivity among studies . In addition, race and regional differences may
affect test results. Therefore, the early screening methods which is non-invasive, highly
sensitive and suitable for Chinese people are needed.
Detection of molecular biomarkers in feces for non-invasive diagnosis of CRC may be a
promising alternative to detecting blood/plasma biomarkers in current clinical settings.
Abnormalities in the composition of the gut microbiota have been implicated as potentially
important causes of CRC. With the widespread use of metagenomic sequencing and pyrosequencing
in intestinal microbiota research, more bacteria have been found positively associated with
CRC incidence. In a recent study, 16S rRNA sequencing was used to classify microbial
communities in human intestinal mucosa at different stages of colorectal tumorigenesis, and
Fusobacterium was found enriched in colorectal tumors.
For CRC, the main process of benign polyps becoming malignant tumors is the accumulation of
genetic and epigenetic alterations that transform colonic epithelial cells into colon
adenocarcinoma cells. These cells are continuously shed into colonic lumen and mixed with the
stool. During tumor formation, epigenetic changes may occur earlier than mutations.
Deregulation of epigenetic mechanisms plays an important role in cancer. Most epigenetic
changes in cancer are triggered by genomic alterations in specific genes that are involved in
controlling one of the epigenetic mechanisms.Aberrant DNA methylation of tumor suppressor
genes induces abnormal expression of downstream genes, which is an important step in the
process of tumorigenesis.The methylation status of DNA changes during CRC progression. A
number of gene methylation abnormalities associated with CRC discovered in recent studies
include SFRP2, SEPT9, BMP3, NDRG4, and SPG20. In addition, some gene mutations are related to
CRC. For example, TP53 and KRAS mutations are common in CRC.
In previous research the investigators found that SEPT9, NDRG4, and SDC2 had higher frequency
and level of methylation in tumors than in normal or non-tumor adjacent CRC tissues,
indicating that these methylated genes may have diagnostic potential for CRC screening.
However, BMP3 had very limited contribution to detection accuracy in stool samples.
Furthermore, the combination of methylated SEPT9, NDRG4, and SDC2 showed high feasibility of
detection of CRC and adenoma and further study showed better performance in detecting CRC
than adenoma. Our research also demonstrates differences in fecal genes between different
ethnic groups.
This research aims to detect intestinal microbiota differences in stool by 16S rRNA analysis
between CRC patients and healthy controls. It will combine DNA analysis of fecal exfoliated
cells to further clarify this difference to build some models for screening early colorectal
cancer in Chinese people. At the same time, the research will also study the impact of
Chinese eating habits on Intestinal Microflora.
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