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Magnified and enhanced computed virtual chromoendoscopy in gastric neoplasia: A feasibility study

机译:放大和增强型虚拟彩色内窥镜检查在胃肿瘤中的可行性研究

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摘要

AIM: To evaluate the feasibility of a new computed virtual chromoendoscopy (CVC) device (M i-scan) in the diagnosis of gastric neoplasia.METHODS: Patients with superficial lesions no larger than 1.0 cm found during high definition endoscopy were included. Those with advanced or obviously protruded or depressed lesions, lesions larger than 1.0 cm and/or lesions which were not amenable to observation by zoom function were excluded. The endoscopist was required to give the real-time descriptions of surface pit patterns of the lesions, based on surface pattern classification of enhanced magnification endoscopy. According to previous reports, types I-III represent non-neoplastic lesions, and types IV-V represent neoplastic lesions. Diagnosis with M i-scan and biopsy was performed before histopathological diagnosis. Magnified images of gastric lesions with and without enhancement were collected for further analysis. The diagnostic yield of real-time M i-scan and effects on magnification image quality by tone enhancement (TE), surface enhancement (SE) and color enhancement (CE) were calculated. The selected images were sent to another endoscopist. The endoscopist rated the image quality of each lesion at 3 levels. Ratings of image quality were based on visualization of pit pattern, vessel and demarcation line.RESULTS: One hundred and eighty-three patients were recruited. Five patients were excluded for advanced gastric lesions, 1 patient was excluded for poor preparation and 2 patients were excluded for superficial lesions larger than 1.0 cm; 132 patients were excluded for no lesions found by high definition endoscopy. In the end, 43 patients with 43 lesions were included. Histopathology revealed 10 inflammation, 14 atrophy, 10 metaplasia, 1 low grade dysplasia (LGD), 5 high grade dysplasia (HGD) and 3 cancers. For 7 lesions classified into type I, histopathology revealed 6 atrophy and 1 metaplasia; for 10 lesions classified into type II, histopathology revealed 2 inflammation, 7 atrophy and 1 metaplasia; for 10 lesions classified into type III, histopathology revealed 1 inflammation, 8 metaplasia and 1 LGD; for 9 lesions classified into type IV, histopathology revealed 4 inflammation, 1 atrophy and 4 HGD; for 7 lesions classified into type V, histopathology revealed 3 inflammation, 1 HGD and 3 cancers. A total of 172 still images, including 43 images by white light (MWL) and 129 images by M i-scan (43 with TE, 43 with SE and 43 with CE), were selected and sent to the endoscopist who did the analysis. General image quality of M i-scan with TE and SE was significantly better than that of MWL (TE, 4.55 ± 1.07; SE, 4.30 ± 1.02; MWL, 3.25 ± 0.99; P < 0.001). Visualization of pit pattern was significantly improved by M i-scan with SE (1.93 ± 0.25 vs 1.50 ± 0.50, P < 0.001). Microvessel visualization was significantly improved by M i-scan with TE (1.23 ± 0.78 vs 0.76 ± 0.73, P < 0.001). Demarcation line visualization was improved by M i-scan with both TE and SE (TE, 1.75 ± 0.52; SE, 1.56 ± 0.59; MWL, 0.98 ± 0.44; P < 0.001). M i-scan with CE did not show any significant improvements of image quality in general or in the 3 key parameters. Although M i-scan with TE and SE slightly increased the diagnostic yield of MWL, there was no significant difference (P > 0.1).CONCLUSION: Although digital enhancement improves the image quality of magnification endoscopy, its value in improving the diagnostic yield seems to be limited.
机译:目的:评估新型计算机虚拟彩色内窥镜(CVC)设备(M i-scan)在胃癌形成诊断中的可行性。方法:包括在高清内窥镜检查中发现浅表病变不大于1.0 cm的患者。那些具有晚期或明显突出或凹陷的病变,大于1.0cm的病变和/或不适合通过变焦功能观察的病变的患者被排除在外。根据增强型放大内窥镜的表面模式分类,要求内镜医师对病变的表面凹坑模式进行实时描述。根据先前的报道,I-III型代表非肿瘤性病变,IV-V型代表肿瘤性病变。在进行组织病理学诊断之前,先行Mi扫描和活检诊断。收集具有和不具有增强的胃部病变的放大图像用于进一步分析。计算了实时M i扫描的诊断结果以及通过色调增强(TE),表面增强(SE)和色彩增强(CE)对放大图像质量的影响。选定的图像被发送给另一位内镜医师。内镜医师将每个病变的图像质量分为3个等级。图像质量的评定基于凹坑图案,血管和分界线的可视化。结果:招募了183例患者。 5例因胃部晚期病变而被排除,1例因准备不良而被排除,2例因浅表病变大于1.0 cm而被排除。 132例患者因高清晰度内窥镜检查未发现病变而被排除在外。最后,纳入了43例病灶共43例。组织病理学显示有10个炎症,14个萎缩,10个化生,1个低度不典型增生(LGD),5个高度不典型增生(HGD)和3个癌症。对于分类为I型的7个病变,组织病理学显示有6个萎缩和1个化生。对于分类为II型的10个病变,组织病理学显示有2个炎症,7个萎缩和1个化生。对于分类为III型的10个病变,组织病理学显示1个炎症,8个化生和1个LGD。对于分类为IV型的9个病变,组织病理学显示有4个炎症,1个萎缩和4个HGD。对于分类为V型的7个病变,组织病理学显示3例炎症,1例HGD和3例癌症。总共选择了172张静态图像,包括白光(MWL)的43张图像和M i-scan的129张图像(TE分别为43,SE为43和CE为43),并发送给进行分析的内镜医师。带有TE和SE的M i-scan的一般图像质量明显优于MWL(TE,4.55±1.07; SE,4.30±1.02; MWL,3.25±0.99; P <0.001)。使用SE进行M i-scan显着改善了凹坑图案的可视化(1.93±0.25与1.50±0.50,P <0.001)。通过TE进行M i-scan显着改善了微血管的可视化(1.23±0.78 vs 0.76±0.73,P <0.001)。通过TE和SE的M i-scan改善了分界线的可视化效果(TE,1.75±0.52; SE,1.56±0.59; MWL,0.98±0.44; P <0.001)。带有CE的M i-scan总体上或3个关键参数均未显示图像质量有任何显着改善。尽管使用TE和SE进行M i-scan可以稍微提高MWL的诊断率,但差异无统计学意义(P> 0.1)。结论:尽管数字增强可以改善放大内窥镜的图像质量,但其在提高诊断率方面的价值似乎受到限制。

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