Magnification chromoendoscopy for the diagnosis of gastric intestinal metaplasia and dysplasia

彩色内窥镜 医学 肠化生 发育不良 胃肠病学 放大倍数 内科学 卡帕 粘膜切除术 病理 内窥镜检查 癌症 结肠镜检查 结直肠癌 哲学 语言学 计算机科学 计算机视觉
作者
Mário Dinis‐Ribeiro,Altamiro Costa‐Pereira,Carlos Lopes,Lúcio Lara Santos,Mateus Guilherme,Luís Moreira‐Dias,Helena Lomba-Viana,Armando Ribeiro,Mariane Santos De Tavares,José Maria Soares,Nuno Mesquita,Rui Silva,Rafael Lomba‐Viana
出处
期刊:Gastrointestinal Endoscopy [Elsevier BV]
卷期号:57 (4): 498-504 被引量:159
标识
DOI:10.1067/mge.2003.145
摘要

Background: The aim of this study was to define the reproducibility and accuracy of magnification chromoendoscopy for the diagnosis of lesions associated with gastric cancer (intestinal metaplasia and dysplasia). Methods: A total of 136 patients with previously diagnosed lesions and 5 gastrectomy specimens were studied. Endoscopic examination was performed with a magnification endoscope after methylene blue (1%) spraying. According to differences in color and mucosal pattern, groups and subgroups of endoscopic images were defined, and biopsies taken (n=462). Five endoscopists were asked to classify individually 2 endoscopic images per subgroup on 2 separate occasions. Results: Three groups of endoscopic images were defined: nonmetaplastic, nondysplastic mucosa (I); metaplastic mucosa (II); and dysplastic mucosa (III). Ten subgroups were defined according to pit pattern: round small (IA), round and tubular small (IB), coarse round (IC), and course round pits with a straight pit (ID); blue irregular marks (IIA), blue round and tubular pits (IIB), blue villi (IIC), and blue small pits (IID); and loss of clear pattern, with depression (IIIA) or with slight elevation (IIIB). The kappa statistic for intraobserver agreement on the classification of endoscopic images in groups was 0.86; for interobserver agreement, it was 0.74. For classification into subgroups, kappa values ranged from 0.48 to 0.78. For 85% of the areas classified endoscopically as Group I (n=146), no mucosal lesions or gastritis was described at histologic examination; for 83% of those in Group II (n=198), intestinal metaplasia was found. Subgroups IIA and IIB were more often associated with complete intestinal metaplasia (62%), and IIC and IID with incomplete metaplasia (67%); in Group III (n=118), dysplasia was diagnosed histopathologically in 33%. For the diagnosis of dysplasia, specificity was 81% (95% CI [77%, 85%]) and negative predictive value 99% (95% CI [99%, 100%]). Conclusions: Gastric endoscopic patterns with chromoendoscopy and magnification seem reproducible and valid for the diagnosis of lesions associated with gastric cancer. This procedure may improve the follow-up of individuals at high-risk of gastric cancer, at least for the exclusion of severe lesions.
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