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首页> 外文期刊>Chinese Journal of Clinical Oncology >NATURAL HISTORY OBSERVATION FOR ESOPHAGEAL AND CARDIA PRECURSORS BY REPETITIVE ENDOSCOPIC SCREENING OF 301 SUBJECTS IN SHEXIAN
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NATURAL HISTORY OBSERVATION FOR ESOPHAGEAL AND CARDIA PRECURSORS BY REPETITIVE ENDOSCOPIC SCREENING OF 301 SUBJECTS IN SHEXIAN

机译:食管301例重复内镜筛查食管和CAR门前体的自然历史观察。

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OBJECTIVE To investigate the natural history of fast developing esophageal and cardia precursors. METHODS Repetitive endoscopic screenings were performed among 40-69-year-olds in the high-incidence areas for esophageal cancer in Shexian. RESULTS The initial diagnosis and the lag-time for 7 subsequently identified severe dysplasia (SD) subjects were as follows: in one subject 13 months after a baseline diagnosis of normal epithelium, in another subject 7 months after a baseline diagnosis of base cell hyperplasia (BCH), in four subjects 3, 4, 4, and 10.5 months after baseline diagnosis of mild dysplasia (mD), and in one subject 12.5 months after a baseline diagnosis of moderate dysplasia (MD). The initial diagnosis and the lag-time for 6 subsequently identified carcinomas in situ or intramucosal carcinoma cases were: in one case 48 months after a baseline diagnosis of mD, in 2 cases 4 and 13 months after baseline diagnoses of MD, and in the other 3 cases 3.5, 9, and 17.5 months after baseline diagnoses of SD. The initial diagnosis and lag- time for 3 subsequently identified invasive cancer cases were: in one case 50 months after a baseline diagnosis of MD, in 2 cases 14 and 19 months after baseline diagnoses of SD. In addition, during a 4-year-follow-up of 18 subjects after endoscopic mucosa resection, 9 of them were found to have developed precursors again at other sites, and also additional findings were obtained for 11 of the 16 dysplasia cases by repetitive biopsy in less than 2 months after the initial endoscopy. CONCLUSION A 5-year screening interval for BCH and mD, and a 3-year interval for MD may be too long for the fast developing precursors. Periodic screenings with shorter intervals should be considered to control the number of interval cases due to fast development, multifocal carcinogenesis, and false negative results inherent in one-time endoscopic biopsy sampling.
机译:目的探讨快速发展的食道和card门前体的自然史。方法对She县食管癌高发地区的40-69岁人群进行反复内镜检查。结果7名随后被识别出的严重发育异常(SD)受试者的初步诊断和时滞如下:在基线诊断为正常上皮的13个月后的一个受试者中,在基线诊断为基础细胞增生的7个月后的另一个受试者中( BCH),在基线诊断为轻度发育不良(mD)的3、4、4和10.5个月后的四个受试者中,以及在基线诊断为中度发育异常(MD)的12.5个月后的一个受试者中。 6例随后发现的原位或粘膜内癌病例的初步诊断和滞后时间是:一个病例在基线诊断为mD后48个月,2例在基线诊断为MD后4和13个月,另一例基线诊断为SD后3.5、9和17.5个月3例。 3例随后确定的浸润性癌症病例的初步诊断和滞后时间为:1例在基线诊断为MD后50个月,2例在基线诊断为SD之后14和19个月。此外,在对内镜黏膜切除术后18位受试者进行了为期4年的随访中,发现其中9位在其他部位再次形成了前体,并且通过重复活检对16例不典型增生病例中的11例也获得了其他发现。在初次内镜检查后不到2个月内。结论对于快速发展的前体,BCH和mD的5年筛查间隔以及MD的3年筛查间隔可能太长。应考虑以较短的间隔进行定期筛查,以控制由于快速发展,多灶致癌和一次性内镜活检样本固有的假阴性结果而导致的间隔病例数。

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