| Literature DB >> 28560510 |
Christos Kontovounisios1,2, Shengyang Qiu3, Shahnawaz Rasheed1,2, Ara Darzi1,2, Paris Tekkis1,2.
Abstract
Colorectal cancer screening programs aim at early detection of cancer to reduce incidence rates and mortality. The objective of this study is to identify the role of neurotensin in the endoscopic screening of high-risk population for developing colorectal neoplasia. Blood samples from patients referred for urgent colonoscopy to investigate symptoms suspicious of colorectal cancer were collected. Blood neurotensin levels were measured using enzyme-linked immunosorbent assay. Colonoscopy findings were used as reference for determining the diagnostic accuracy of blood neurotensin. The study comprised 26 patients in total: 12 healthy and 14 with colon pathology (13 high-grade dysplasia adenomatous polyps, 1 adenocarcinoma). There were no statistically significant differences in the clinical and biochemical parameters between colon pathology and healthy group except neurotensin levels. Pathology in colon was associated with 3.7-fold increase in NT levels. In multivariate analysis, patients with pathology in colon have increased serum neurotensin levels compared to controls adjusted for age, gender, BMI and co-morbidities. The value of 12.93 pg/ml is associated with 87.5% sensitivity and 91.7% specificity for discriminating the colon pathology from normal colonic epithelium (p = 0.001). Neurotensin plasma values differentiate healthy people from patients suffering from colonic pathologies such as adenomatous polyps and cancer. The use of neurotensin as a potential endoscopic screening tool for identifying high-risk population for developing colorectal cancer is promising, but much has to be done before it is validated in larger scale prospective studies.Entities:
Keywords: Colorectal cancer; Diagnostic biomarker; Neurotensin
Mesh:
Substances:
Year: 2017 PMID: 28560510 PMCID: PMC5591352 DOI: 10.1007/s13304-017-0464-6
Source DB: PubMed Journal: Updates Surg ISSN: 2038-131X
Characteristics and average blood neurotensin levels of patients who had normal colonoscopy vs. patients with colon pathologies (polyps and cancer)
| Group |
| ||||
|---|---|---|---|---|---|
| Normal | Colon pathology | ||||
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| Gender | |||||
| Female | 9 | 75.0 | 7 | 50.0 | n.s+ |
| Male | 3 | 25.0 | 7 | 50.0 | |
| Co-morbidities | |||||
| No | 9 | 75.0 | 9 | 64.3 | n.s+ |
| Yes | 3 | 25.0 | 5 | 35.7 | |
| Smoker | |||||
| No | 11 | 91.7 | 12 | 85.7 | |
| Yes | 1 | 8.3 | 2 | 14.3 | n.s+ |
| Alcohol consumption | |||||
| No | 12 | 100.0 | 11 | 78.6 | |
| Yes | 0 | 0.0 | 3 | 21.4 | n.s+ |
BMI body mass index, SEM standard error of mean, pg/ml picograms per millilitre
+Chi-square/Fisher’s exact test, * Mann–Whitney U test
Multivariate regression analysis of effect of the presence of colorectal pathology and other patient factors on increased serum NT levels
| OR | 95% CI |
| |
|---|---|---|---|
| Group | |||
| Colorectal pathology vs. normal | 26.17 | 12.47 to 39.271 | 0.001 |
| Age (years) | 0.341 | −0.108 to 0.79 | n.s |
| Gender | |||
| Female vs. male | 5.742 | −8.8 to 20.28 | n.s |
| BMI (kg/m2) | −0.454 | −2.2 to 1.2 | n.s |
| Co-morbidities | |||
| Yes vs. no | 6.128 | −9.27 to 21.53 | n.s |
OR odds ratio, 95% CI 95% confidence intervals, BMI body mass index
Fig. 1Received operator characteristics (ROC) curve for the sensitivity and specificity of plasma neurotensin level in identifying colorectal polyps and cancer