巴雷特食管低度发育异常的诊断及其对疾病进展的影响。
The diagnosis of low-grade dysplasia in Barrett's esophagus and its implications for disease progression.
作者信息
Skacel M, Petras R E, Gramlich T L, Sigel J E, Richter J E, Goldblum J R
机构信息
Department of Anatomic Pathology, The Cleveland Clinic Foundation, Ohio 44195, USA.
出版信息
Am J Gastroenterol. 2000 Dec;95(12):3383-7. doi: 10.1111/j.1572-0241.2000.03348.x.
OBJECTIVE
The reported risk of progression from low-grade dysplasia (LGD) to high-grade dysplasia (HGD) or carcinoma (CA) in Barrett's esophagus varies. However, the validity of a diagnosis of LGD may be questioned because of interobserver variability.
METHODS
A search of the Cleveland Clinic Foundation surgical pathology files between 1986 and 1997 yielded biopsy specimens from 43 patients with Barrett's esophagus diagnosed and coded as LGD. Patients with concurrent or prior diagnoses of HGD or carcinoma were excluded. The LGD cases were randomized and blindly reviewed by three gastrointestinal (GI) pathologists along with cases originally diagnosed as Barrett's esophagus without dysplasia (ND; n = 28), indefinite for dysplasia (IND; n = 14), or HGD (n = 15). Each pathologist classified every biopsy specimen as ND, IND, LGD, or HGD, and interobserver agreements were determined by kappa statistics (K). Follow-up data were available on 25 patients originally diagnosed with LGD. Progression was defined as a subsequent diagnosis of HGD or CA on esophageal biopsy or resection specimens.
RESULTS
Agreement between two GI pathologists for a diagnosis of LGD was fair (K = 0.28) and poor (K = 0.21 and -0.04). Individual GI pathologists agreed with the original diagnosis of LGD in 70%, 56%, and 16% of cases. The 25 patients with follow-up included 21 men and four women (mean age, 67 yr) with a mean follow-up of 26 months (range: 2-84 months). Seven patients (28%) with follow-up developed HGD (five patients) or CA (two patients), 2-43 months (median: 11 months) after a diagnosis of LGD. The individual GI pathologists' diagnosis did not correlate with progression. However, when at least two GI pathologists agreed on LGD, there was a significant association with progression (seven of 17 patients, 41%, p = 0.04). When all three GI pathologists agreed on a diagnosis of LGD, four of five patients progressed (p = 0.012). In contrast, of the eight patients with follow-up and no agreement among GI pathologists for a diagnosis of LGD, none progressed.
CONCLUSIONS
A high degree of interobserver variability is seen in the histological diagnosis of Barrett's esophagus-related LGD. Although the number of observations is low, a consensus diagnosis of LGD among GI pathologists suggests an increased risk of progression from LGD to HGD or carcinoma.
目的
据报道,巴雷特食管中低度异型增生(LGD)进展为高度异型增生(HGD)或癌(CA)的风险各不相同。然而,由于观察者间的差异,LGD诊断的有效性可能受到质疑。
方法
检索克利夫兰诊所基金会1986年至1997年的外科病理档案,获得43例诊断为LGD并编码的巴雷特食管活检标本。排除同时或先前诊断为HGD或癌的患者。将LGD病例随机分组,并由三名胃肠(GI)病理学家进行盲法复查,同时复查最初诊断为无异型增生的巴雷特食管(ND;n = 28)、异型增生不确定(IND;n = 14)或HGD(n = 15)的病例。每位病理学家将每个活检标本分类为ND、IND、LGD或HGD,并通过kappa统计量(K)确定观察者间的一致性。有25例最初诊断为LGD的患者的随访数据。进展定义为食管活检或切除标本随后诊断为HGD或CA。
结果
两位GI病理学家对LGD诊断的一致性一般(K = 0.28),较差(K = 0.21和 -0.04)。个别GI病理学家在70%、56%和16%的病例中同意最初的LGD诊断。25例接受随访的患者包括21名男性和4名女性(平均年龄67岁),平均随访26个月(范围:2 - 84个月)。7例(28%)接受随访的患者在诊断为LGD后2 - 43个月(中位数:11个月)出现HGD(5例)或CA(2例)。个别GI病理学家的诊断与进展无关。然而,当至少两名GI病理学家对LGD达成一致时,与进展有显著关联(17例患者中的7例,41%,p = 0.04)。当所有三名GI病理学家对LGD诊断达成一致时,五名患者中有四名进展(p = 0.012)。相比之下,在8例接受随访且GI病理学家对LGD诊断未达成一致的患者中,无人进展。
结论
在巴雷特食管相关LGD的组织学诊断中存在高度的观察者间差异。尽管观察数量较少,但GI病理学家之间对LGD的共识诊断表明从LGD进展为HGD或癌的风险增加。
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