Evaluation of Stool Based Markers for the Early Detection of Colorectal Cancers and Adenomas

University of Michigan Rogel Cancer Center

Status

Enrolling

Conditions

Colonic Neoplasms

Study type

Observational

Funder types

Other

NETWORK

Other U.S. Federal agency

Industry

NIH

Identifiers

NCT00843375

UMCC 2018.126 GLNE 007

UMCC 2018.126 (Other Identifier)

HUM00161344 (Other Identifier)

HUM00029506 (Other Identifier)

HUM00149961 (Other Identifier)

UMCC 2005.008 (Other Identifier)

U01CA086400 (U.S. NIH Grant/Contract)

Details and patient eligibility

About

Colon cancer is the second most common cancer in men and women. It is a disease that can be prevented if it is found early. Colonoscopy is still the best screening tool for colon cancer and the polyps that turn into colon cancer. However, due to a variety of factors, including affordability, time, and age, not all patients are able to be screened. Researchers are working on other options for early detection that are as accurate as colonoscopy.

The purpose of this study if to determine if stool or blood can be used to detect colon cancers as early or earlier than colonoscopy. The researchers plan to use these samples to learn about specific proteins (also known as biomarkers) that may indicate colon polyps, colon cancer or an increased risk of developing colon cancer. In order to learn more about preventing and detecting colon and rectal cancer, we are collecting samples from subjects with cancer, adenomas, and colonoscopies who may be at risk for polyps.

Full description

In recognition of the fact that novel potential biomarkers are continually being identified and will need to be validated in a rapid, efficient and scientifically rigorous manner, the NCI has made an enormous commitment to the development of a network that will facilitate biomarker development and validation in multiple organ sites. As part of the National Cancer Institute-funded Early Detection Research Network (EDRN), the Great Lakes-New England Clinical Epidemiological Center (GLNE CEC) proposes a research study that validates potential molecular markers ("biomarkers") for the detection of precancerous and cancerous conditions and cancer risk assessment. Although examples of such biomarkers are currently in clinical use (i.e. CEA, CA-125), there are limitations to all of them. Our consortium focuses on gastrointestinal neoplasia. The goals of this phase of the proposed research are:

Assessment of the utility of individual stool-based, serum-based and urine-based biomarkers for discriminating between patients with adenocarcinomas, patients with adenomas, patients without adenomas and normal subjects both at normal and high risk for developing colon cancer.
Construction of a panel of markers from those considered in Objective 1 to discriminate, under a number of assumptions concerning prevalence and cost of misclassification, between:
1. Subjects with normal colons versus patients without adenomas, patients with adenomas and patients with cancers;
2. Subjects with normal colons, patients without adenomas and patients with adenomas, versus subjects with cancers;
3. Subjects with normal colons versus patients without and patients with adenomas versus patients with cancers.
Comparison of the characteristics of individual markers and panels as discriminators to those of the established current standard, fecal immunochemical test (FIT).
Continued support of a renewal of a bank of stool samples linked to serum, tissue, and clinical data from patients with colorectal cancer, adenomas and normal controls for validation of stool-based markers that may be developed in the future.

To build our collection, we propose to collect stool, FIT, serum, plasma, and tissue samples from 1200 new subjects. Each biomarker will be analyzed individually and considered as a potential panel marker to be used for future largescale screening longitudinal trials. (This protocol previously recruited an additional 682 subjects from January 2006 to June 2010.)

Enrollment

1,200 estimated patients

Sex

All

Ages

18+ years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Willing to sign informed consent
Able to physically tolerate removal of up to 60 ml of blood
Adults at least 18 years old
Willing to collect 1-2 stool samples and prepare a Fecal Immunochemical Test (FIT)
Pregnant or nursing women who otherwise meet the eligibility criteria may participate
Subjects with one of the following:
- Colorectal adenocarcinoma-not treated and in colon at time of stool collection (CRC bin)
- Adenoma-pathologically confirmed adenoma present in colon at time of stool collection (Adenoma Bin)
- Higher Risk Non-neoplastic Bin
  - Subjects with a personal history of adenomas (confirmed by pathology) with none present on qualifying colonoscopy
  - Subjects with a personal history of CRC (longer than 3 years ago because of exclusion criteria of cancer within last 3 years) with none present at time of qualifying colonoscopy
  - Any family history of CRC (1st degree relative)
  - Current positive screening stool test for blood, for DNA or for both within 12 months with no follow-up intervention.
- Average Risk, Non-neoplastic Bin
  - No history or current finding of any colorectal neoplasia including CRC, adenomas, sessile serrated adenomas and no family history of CRC.
  - Subjects who had CRC that was successfully treated at least three years ago may be considered eligible for the adenoma bin if their polyps are adenomas and there is no evidence of CRC, or for the higher risk non-neoplastic bin as noted above.
  - Subjects whose screening colonoscopy shows any of these types of polyps may be included in the non-neoplastic or the higher risk non-neoplastic bin if they meet the other criteria noted above.
    - Hyperplastic polyps
    - Benign mucosal polyps
    - Polypoid granulation tissue
    - Prolapsed mucosal polyps
    - Inflammatory polyp
    - Transitional mucosal polyp
    - Lipoma
    - Gangleoneuroma
    - Neuroma
    - Hamartomatous polyp

Exclusion criteria

Cancer patients who have had any surgery, radiation, or chemotherapy for their current colorectal cancer prior to collecting the baseline samples
History of or clinically active Inflammatory Bowel Disease
Known HNPCC or FAP
Inability to provide informed consent.
Other active malignancy within 3 years of enrollment except any of the following:
- Squamous cell carcinoma of the skin
- Basal cell carcinoma of the skin
- Carcinoma in situ of the cervix, Stages Ia or Ib invasive squamous cell carcinoma of the cervix treated by surgery only. (Excluded if had pelvic radiation)
- Stage Ia Grade 1 adenocarcinoma of the endometrium treated with surgery
Patients on active chemotherapy or radiation treatment for any purpose
Known HIV or chronic active viral hepatitis
Women who are pregnant
CT colonography (virtual colonoscopy) patients

Trial design

1,200 participants in 4 patient groups

Higher risk, no neoplasia

Description:

Negative study colonoscopy and one or more of the following: * Subjects with a personal history of adenomas (confirmed by pathology) with none present on qualifying colonoscopy * Subjects with a personal history of colorectal cancer (CRC) (longer than 3 years ago because of exclusion criteria of cancer within last 3 years) with none present at time of qualifying colonoscopy * Any family history of CRC (1st degree relative) * Current positive screening stool test for blood, for DNA or for both within 12 months with no follow up intervention

Adenoma

Description:

Pathologically confirmed adenomas, both non-advanced adenoma and advanced. Advanced adenoma includes any of the following: * Sessile serrated adenoma * Tubulovillous adenoma * Villous adenoma * Sessile serrated polyp/adenoma * Traditional serrated adenoma * Any adenoma ≥1 cm

Colorectal adenocarcinoma

Description:

Pathologically confirmed colorectal cancer either present at time of stool collection or discovered during colonoscopy

Average risk, no neoplasia

Description:

No neoplasia found at colonoscopy and: * No prior history of adenomas or sessile serrated adenomas * No prior history of CRC * No first degree family history of CRC * Negative colorectal cancer screening test (if performed) for blood, for DNA or for both within 12 months.

Trial contacts and locations

Central trial contact

Cancer AnswerLine

Data sourced from clinicaltrials.gov

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