Literature DB >> 22104755

Colon cancer screening: which non-invasive filter tests?

Christian Pox1.   

Abstract

The following non-invasive stool tests for colorectal cancer (CRC) screening exist: guaiac or immunochemical fecal occult blood testing (FOBT), genetic stool tests and the M2-PK. Currently the most widely used tests are guaiac-based (gFOBT). Several randomized controlled trials have shown that gFOBT are able to achieve a reduction in CRC-related mortality. This reduction is achieved by detecting asymptomatic cancers at an early stage with a better prognosis. However, gFOBT have a low sensitivity for colorectal adenomas and are thus unlikely to be able to reduce the incidence of CRC. Furthermore, gFOBT are not specific for human blood and can be influenced by external factors. Immunochemical tests (iFOBT) only detect human blood in the stool. In two recent randomized studies from the Netherlands comparing guaiac and immunochemical tests in the asymptomatic population, iFOBT were found to detect more cancers than gFOBT. Furthermore, iFOBT were able to detect more advanced adenomas thus having the potential to be able to reduce the incidence of CRC as well as CRC-related mortality. In the recently released European CRC screening guidelines, iFOBT are considered the screening test of choice. Several questions remain however. It is currently unknown what the optimal cut-off value for an iFOBT to be considered positive should be and what the number of stool samples is that are required. Genetic stool tests detect mutations in stool that can be found in CRC. The original test testing for 21 genetic changes was found to be superior to gFOBT for the detection of cancers. However, the sensitivity was moderate (51.6%) and the sensitivity for advanced adenomas was low. In the meantime the test has been modified improving DNA extraction and reducing the number of mutations tested for as well as including a methylation marker. The efficacy of the modified test in the screening population is unknown. M2-PK is an isomer of the enzyme pyruvate kinase that is involved in glycolysis. Studies have found a good sensitivity for cancers, a low sensitivity for advanced adenomas with a specificity of around 80%. Further studies in the screening population are required.
Copyright © 2011 S. Karger AG, Basel.

Entities:  

Mesh:

Year:  2011        PMID: 22104755     DOI: 10.1159/000331127

Source DB:  PubMed          Journal:  Dig Dis        ISSN: 0257-2753            Impact factor:   2.404


  10 in total

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2.  Discovery of genes from feces correlated with colorectal cancer progression.

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3.  Application of quantitative estimates of fecal hemoglobin concentration for risk prediction of colorectal neoplasia.

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Review 4.  Colorectal cancer screening: 20 years of development and recent progress.

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Review 5.  Gastrointestinal endoscopy in the pregnant woman.

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Review 6.  Tumor markers in colorectal cancer, gastric cancer and gastrointestinal stromal cancers: European group on tumor markers 2014 guidelines update.

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7.  KCNQ5 and C9orf50 Methylation in Stool DNA for Early Detection of Colorectal Cancer.

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Authors:  Hui Cai; Elena G Chiorean; Michael V Chiorean; Douglas K Rex; Bruce W Robb; Noah M Hahn; Ziyue Liu; Patrick J Loehrer; Marietta L Harrison; Yan Xu
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10.  The Use of M2-Pyruvate Kinase as a Stool Biomarker for Detection of Colorectal Cancer in Tertiary Teaching Hospital: A Comparative Study.

Authors:  Shahidah Che Alhadi; Wan Zainira Wan Zain; Zalina Zahari; Mohd Nizam Md Hashim; Syed Hassan Syed Abd Aziz; Zaidi Zakaria; Michael Pak-Kai Wong; Andee Dzulkarnaen Zakaria
Journal:  Ann Coloproctol       Date:  2020-09-18
  10 in total

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