Copyright
©The Author(s) 2019.
World J Gastroenterol. May 7, 2019; 25(17): 2045-2057
Published online May 7, 2019. doi: 10.3748/wjg.v25.i17.2045
Published online May 7, 2019. doi: 10.3748/wjg.v25.i17.2045
Table 1 Current guidelines for screening Barrett's esophagus from major gastroenterology societies[3]
| Society (year published) | Target populations |
| American College of Gastroenterology (2016) | Primary: Male patients with either > 5 years of GERD or with more than weekly GERD symptoms and at least two other risk factors including: (1) Age > 50; (2) central obesity; (3) smoking history; (4) Caucasian; (5) first degree relative with BE or EAC |
| American Society for Gastrointestinal Endoscopy (2012) | Patients with multiple risk factors including male sex, older than 50, Caucasian, family history of BE, increased duration of reflux symptoms, smoking and obesity |
| American Gastroenterological Association (2011) | Patients with multiple risk factors including male sex, older than 50, Caucasian, chronic GERD, hiatal hernia and obesity |
| British Society of Gastroenterology (2014) | Primary: Patients with GERD and at least three risk factors including male, older than 50, Caucasian, and obesity unless there is a family history of BE or EAC which would lower threshold |
Table 2 Univariate analyses for each risk factors progression to high grade dysplasia or esophageal adenocarcinoma[4]
| Variable | Adjusted P value and hazard ratios (95%CI) |
| Males | P = 0.0023, HR = 3.01 (1.48-6.11) |
| Smoking | P = 0.0029, HR = 1.83 (1.23-2.71) |
| Age + 10 yr | P = 0.3055, HR = 0.96 (0.89-1.04) |
| Caucasian | P = 0.8429, HR = 1.06 (0.61-1.82) |
| Hiatal hernia present | P = 0.5928, HR = 1.12 (0.73-1.72) |
| Visible lesion at baseline | P = 0.9254, HR = 1.04 (0.49-2.2) |
| Aspirin use | P = 0.2807, HR = 0.81 (0.56-1.18) |
| Non-steroidal anti-inflammatory drug | P = 0.5602, HR = 0.9 (0.64-1.28) |
| Proton pump inhibitor | P = 0.8197, HR = 0.9 (0.37-2.21) |
| Low grade dysplasia | P ≤ 0.0001, HR = 3.68 (2.56-5.31) |
| BE length + 1 cm increase in length | P ≤ 0.0001, HR = 1.12 (1.08-1.18) |
Table 3 Progression in Barrett's esophagus point system based on risk variables[4]
| Variable | Points |
| BE length in centimeters | |
| < 1 | 0 |
| 1 to < 2 | 1 |
| 2 to < 3 | 2 |
| 3 to < 4 | 3 |
| 4 to < 5 | 4 |
| 5 to < 6 | 5 |
| 6 to < 7 | 6 |
| 7 to < 8 | 7 |
| 8 to < 9 | 8 |
| 9 to < 10 | 9 |
| 10 + | 10 |
| Males | 9 |
| Smokers | 5 |
| Baseline confirmed LGD | 11 |
Table 4 Barrett's international narrow band imaging group classification for Barrett's esophagus with narrow band imaging[8]
| Mucosal pattern | |
| Circular, ridged/villous, or tubular | Regular |
| Absent or irregular | Irregular |
| Vascular pattern | |
| Blood vessels situated regularly along or between mucosal ridges and/or showing normal long branching patterns | Regular |
| Focally or diffusely distributed vessels not following normal architecture of the mucosa | Irregular |
Table 5 Miami criteria for classifying Barrett's esophagus using confocal laser endoscopy[12]
| Histology | Confocal characteristics |
| 1 Normal Squamous Epithelium | Flat Cells with bright intrapapillary capillary loops |
| 2 Non-dysplastic Barrett's Esophagus | Uniformed villiform architecture with dark goblet cells |
| 3 Barrett's esophagus with high-grade dysplasia | Villiform structures with dark, irregular and thick borders |
| 4 Adenocarcinoma | Disorganized villiform architecture and dilated irregular vessels |
Table 6 Screening techniques for Barrett's esophagus[7]
| Advantage | Disadvantage | |
| Standard definition white light endoscopy | Provides wide-field imaging and is widely available | Decreased sensitivity when compared to high definition |
| High definition white light endoscopy | Provides wide-field imaging and is widely available with improved image quality | Cost of procedure, sedation and in some cases updating entire endoscopy system. Some concerns over missed rates of dysplastic lesions |
| Dye-based chromoendoscopy | Provides wide-field imaging with benefit of mucosal enhancement | Additional steps in procedure are time consuming and some concerns over harm of contrast |
| Narrow band imaging | Provides wide-field imaging and is widely available with improved sensitivity and without need for contrast. Relatively cheap. | Still requires white light endoscopy as an adjunct with unclear evidence on its benefits when compared to white light endoscopy alone |
| Flexible intelligent chromoendoscopy and i-SCAN | Provides wide field imaging without the need for contrast | Not widely available and not enough research to determine benefits compared to standard of car |
| Blue light imaging | Helpful in defining subtle changes in elevation and depression of the mucosa | Beneficial as an adjunct to WLE only and hence requires similar costs. Not widely available. |
| Auto flourescence imaging | Provides wide field imaging with improved sensitivity and without the need for contrast | Poor specificity with high false positive rate. |
| Confocal laser endomicroscopy | Provides in vivo information, has a validated scoring classification, and can be used with any endoscope | Does not provide wide-field imaging, requires fluorescein prolonging procedure time, requires expert interpretation and expensive |
| Endocytoscopy | Increases ability to identify dysplastic and neoplastic lesions | Does not provide wide-field imaging and requires giving contrast agent |
| Optical coherence tomography | Provides in vivo information without need for contrast or fluorescein. Ability to evaluate subsurface | Does not provide wide-field imaging and research has varied and is ongoing |
| Volumetric laser endomicroscopy | Similar to OCT but provides high resolution, high speed images over wider surface area | Expensive and studies are still working to obtain interobserver agreement and correlating images with histology |
| Tethered capsule endomicroscopy | Utilizes same technology used for OCT and is safe, well tolerated by patients | Early in stages of research |
| Spectroscopy | Early studies have shown good success in real time detection of BE and neoplasia | Early in stages of research |
| wide area transepithelial sampling | Provides wide area sampling of tissue with high sensitivity and specificity and easy to use | Not yet widely available? Regarding cost and more research needed |
| Cytosponge | Generally safe and well tolerated with low cost | Still requires endoscopy for treatment if abnormality is identified |
| Transnasal Endoscopy | Generally safe and well tolerated with relatively lower cost than endoscopy without the need for general sedation. Can be used in clinic as well as hospital | While early studies have shown equivocal ability to diagnosis BE compared to conventional endoscopy, more research required |
| Biomarker panels | Early studies have shown ability to predict progression of BE from non-dysplastic to neoplasia | A single, ideal biomarker has not been delineated and more research is required. |
| Breath testing with an electronic nose device | Safe and well tolerated and easy to use with overall cost-effectiveness | Sensitivity and specificity are good but not great compared to some other methods and research at this point is limited |
- Citation: Steele D, Baig KKK, Peter S. Evolving screening and surveillance techniques for Barrett's esophagus. World J Gastroenterol 2019; 25(17): 2045-2057
- URL: https://www.wjgnet.com/1007-9327/full/v25/i17/2045.htm
- DOI: https://dx.doi.org/10.3748/wjg.v25.i17.2045