Your search keyword '"Advanced adenomas"' showing total 5 results

1. Evaluation of Blood Soluble CD26 as a Complementary Biomarker for Colorectal Cancer Screening Programs.

Author

De Chiara, Loretta, Barcia-Castro, Leticia, Gallardo-Gómez, María, Páez de la Cadena, María, Martínez-Zorzano, Vicenta S., Rodríguez-Berrocal, Francisco J., Bujanda, Luis, Etxart, Ane, Castells, Antoni, Balaguer, Francesc, Jover, Rodrigo, Cubiella, Joaquín, and Cordero, Oscar J.

Subjects

*COLONOSCOPY, *EARLY detection of cancer, *PROTEOLYTIC enzymes, *COLORECTAL cancer, *GLYCOPROTEINS, *DESCRIPTIVE statistics, *TUMOR markers, *BLOOD testing

Abstract

Simple Summary: Many countries have implemented, or are implementing, general age-based screening programs to reduce mortality due to colorectal cancer. Fecal hemoglobin immunodetection (FIT) in combination with endoscopy has already been relatively successful in achieving this goal. However, there are issues that can be improved in relation to participation rates and reduction in false positives. We studied whether the blood biomarker soluble-CD26 (sCD26), a glycoprotein with dipeptidyl peptidase enzyme activity (DPP4), could help in the early diagnosis of colorectal cancer and advanced adenomas in combination with FIT, also reducing false positives. We propose a sequential testing strategy for FIT positive individuals, offering an alternative blood test with our biomarker for a confirmation prior to colonoscopy in the short term. Fecal hemoglobin immunodetection (FIT) in combination with endoscopy has been implemented to reduce mortality from colorectal cancer (CRC), although there are issues that can be improved in relation to participation rates. We studied whether the blood biomarker soluble-CD26 (sCD26), related at least in part to the immune system and inflammation, and/or its dipeptidyl peptidase enzyme activity (DPP4), could help reduce false positives. In a cohort of 1703 individuals who underwent colonoscopy and had a serum sample, sCD26 and DPP4 activity showed statistically significant differences regarding sex and age. According to the colonoscopy findings, sCD26 and DPP4 activity progressively decreased in advanced adenomas and CRC, with statistically significant differences, even between both groups; 918 of them had a FIT result (n = 596 positive cases) with approximately 70% of these (n = 412) false positives. With cut-offs of 440 ng/mL for sCD26, 42 mU/mL for DPP4, and 11 ng/mU for their ratio, the combined information of the three biomarkers (at least positive for one biomarker) identified almost all advanced adenomas and CRC cases in the FIT cohort with approximately half of the false positives compared to FIT. A sequential testing strategy with FIT and our blood biomarker test is proposed. [ABSTRACT FROM AUTHOR]

Published

2022

2. Evaluation of Blood Soluble CD26 as a Complementary Biomarker for Colorectal Cancer Screening Programs

Author

Loretta De Chiara, Leticia Barcia-Castro, María Gallardo-Gómez, María Páez de la Cadena, Vicenta S. Martínez-Zorzano, Francisco J. Rodríguez-Berrocal, Luis Bujanda, Ane Etxart, Antoni Castells, Francesc Balaguer, Rodrigo Jover, Joaquín Cubiella, and Oscar J. Cordero

Subjects

Cancer Research, Oncology, colorectal cancer, advanced adenomas, FIT, endoscopy, blood test, soluble CD26, DPP4

Abstract

Fecal hemoglobin immunodetection (FIT) in combination with endoscopy has been implemented to reduce mortality from colorectal cancer (CRC), although there are issues that can be improved in relation to participation rates. We studied whether the blood biomarker soluble-CD26 (sCD26), related at least in part to the immune system and inflammation, and/or its dipeptidyl peptidase enzyme activity (DPP4), could help reduce false positives. In a cohort of 1703 individuals who underwent colonoscopy and had a serum sample, sCD26 and DPP4 activity showed statistically significant differences regarding sex and age. According to the colonoscopy findings, sCD26 and DPP4 activity progressively decreased in advanced adenomas and CRC, with statistically significant differences, even between both groups; 918 of them had a FIT result (n = 596 positive cases) with approximately 70% of these (n = 412) false positives. With cut-offs of 440 ng/mL for sCD26, 42 mU/mL for DPP4, and 11 ng/mU for their ratio, the combined information of the three biomarkers (at least positive for one biomarker) identified almost all advanced adenomas and CRC cases in the FIT cohort with approximately half of the false positives compared to FIT. A sequential testing strategy with FIT and our blood biomarker test is proposed.

Published

2022

3. Multitarget Stool mRNA Test for Detecting Colorectal Cancer Lesions Including Advanced Adenomas

Author

Jean-François Beaulieu, Shigeru Kanaoka, Elizabeth Herring, Nathalie McFadden, and Eric Tremblay

Subjects

Cancer Research, medicine.medical_specialty, Colorectal cancer, mRNA, Stool testing, colorectal cancer, Gastroenterology, lcsh:RC254-282, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Screening method, medicine, Stage (cooking), stool, Messenger RNA, Receiver operating characteristic, Advanced adenomas, business.industry, screening, Curve analysis, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, digestive system diseases, 3. Good health, Oncology, 030220 oncology & carcinogenesis, advanced adenoma, 030211 gastroenterology & hepatology, business

Abstract

Simple Summary Colorectal cancer is still one of the deadliest cancers, even though its detection at early stages has been shown to be a key factor for reducing mortality. Screening methods are available, but their efficacy for detecting early-stage lesions is limited. In the present discovery stage study, we used a targeted mRNA assay in the stools to optimize the identification of patients bearing precancerous lesions as well as colorectal cancers at curable stages with only five targets, thus compatible with standard multiplex PCR. Although further validation is required, this assay has high potential for improving colorectal cancer screening efficacy. Abstract Current approved non-invasive screening methods for colorectal cancer (CRC) include FIT and DNA-FIT testing, but their efficacy for detecting precancerous lesions that are susceptible to progressing to CRC such as advanced adenomas (AA) remains limited, thus requiring further options to improve the detection of CRC lesions at earlier stages. One of these is host mRNA stool testing. The aims of the present study were to identify specific stool mRNA targets that can predict AA and to investigate their stability under a clinical-like setting. A panel of mRNA targets was tested on stool samples obtained from 102 patients including 78 CRC stage I-III and 24 AA as well as 32 healthy controls. Area under the receiver operating characteristic (ROC) curves were calculated to establish sensitivities and specificities for individual and combined targets. Stability experiments were performed on freshly obtained specimens. Six of the tested targets were found to be specifically increased in the stools of patients with CRC and three in the stools of both AA and CRC patients. After optimization for the choice of the 5 best markers for AA and CRC, ROC curve analysis revealed overall sensitivities of 75% and 89% for AA and CRC, respectively, for a ≥95% specificity, and up to 75% and 95% for AA and CRC, respectively, when combined with the FIT score. Targets were found to be stable in the stools up to 3 days at room temperature. In conclusion, these studies show that the detection of host mRNA in the stools is a valid approach for the screening of colorectal cancerous lesions at all stages and is applicable to a clinical-like setup.

Published

2021

4. Fecal Immunochemical Tests Detect Screening Participants with Multiple Advanced Adenomas Better than T1 Colorectal Cancers

Author

Anton Gies, Thomas Heisser, Hermann Brenner, Laura Fiona Gruner, Tobias Niedermaier, and Petra Schrotz-King

Subjects

Cancer Research, medicine.medical_specialty, Adenoma, Colorectal cancer, fecal occult blood test, Gastroenterology, lcsh:RC254-282, Article, 03 medical and health sciences, 0302 clinical medicine, prevention, Internal medicine, Tumor stage, medicine, Stage (cooking), early detection, neoplasms, Feces, Advanced adenomas, business.industry, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, digestive system diseases, Oncology, colon cancer, 030220 oncology & carcinogenesis, advanced neoplasia, 030211 gastroenterology & hepatology, business, Body mass index

Abstract

Background: Fecal immunochemical tests (FITs) are widely used for colorectal cancer (CRC) screening. The detection of early-stage cancer and advanced adenoma (AA), the most important premalignant lesion, is highly relevant to reducing CRC-related deaths. We aimed to assess sensitivity for the detection of CRC and AA stratified by tumor stage, number, size, histology of AA, and by location, age, sex, and body mass index (BMI). Methods: Participants of screening colonoscopy (n = 2043) and newly diagnosed CRC patients (n = 184) provided a stool sample before bowel preparation or CRC surgery. Fecal hemoglobin concentration was determined in parallel by nine different quantitative FITs among 94 CRC patients, 200 AA cases, and 300 participants free of advanced neoplasm. Sensitivities were calculated at original cutoffs and at adjusted cutoffs, yielding 93% specificity among all FITs. Results: At adjusted cutoffs, UICC stage I cancers yielded consistently lower sensitivities (range: 62–68%) compared to stage II–IV cancers (range: 73–89%). An even stronger gradient was observed according to T status, with substantially lower sensitivities for T1 (range: 39–57%) than for T2–T4 cancers (range: 71–100%). Sensitivities for the detection of participants with multiple AAs ranged from 55% to 64% and were by up to 25% points higher than sensitivities for T1 cancers. Conclusions: FITs detect stage I cancers and especially T1 cancers at substantially lower sensitivities than more advanced cancer stages. Participants with multiple AAs were detected with slightly lower sensitivities than stage I cancers and with even higher sensitivities than T1 cancers. Further research should focus on improving the detection of early-stage cancers.

Published

2021

5. BAGE Hypomethylation Is an Early Event in Colon Transformation and Is Frequent in Histologically Advanced Adenomas

Author

Andriy P Lutsyk, V. V. Gordiyuk, Erica Lana, Isabelle Rivals, Alla Rynditch, Albertina De Sario, Frédéric Bibeau, Sylvain Kirzin, Marie-Elisabeth Brun, and Janick Selves

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Colorectal cancer, Advanced adenomas, business.industry, Normal tissue, adenomas, colorectal cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Article, Transformation (genetics), BAGE, DNA hypomethylation, biomarker, COBRA, B MELANOMA ANTIGEN, Oncology, medicine, Biomarker (medicine), business

Abstract

We showed earlier that BAGE (B melanoma antigen) loci are hypermethylated in normal tissues and hypomethylated in 98% of human cancers. More recently, we provided evidence that hypomethylation of BAGE loci represents an informative marker for colon cancer detection. In this study, we show that hypomethylation of BAGE loci was an early event that occurred in 43% of colorectal adenomas. Interestingly, hypomethylation of BAGE loci was frequent (50%) in tubulo-villous and villous adenomas, these adenomas having a high probability of being transformed into colorectal cancers.

Published

2009