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溃疡性结肠炎发育异常评估中的观察者差异。

Observer variation in the assessment of dysplasia in ulcerative colitis.

作者信息

Dixon M F, Brown L J, Gilmour H M, Price A B, Smeeton N C, Talbot I C, Williams G T

机构信息

Department of Pathology, University of Leeds, UK.

出版信息

Histopathology. 1988 Oct;13(4):385-97. doi: 10.1111/j.1365-2559.1988.tb02055.x.

Abstract

Six histopathologists allocated 100 sections from patients with long-standing ulcerative colitis into four diagnostic categories, regular hyperplasia, reactive atypia, low-grade and high-grade dysplasia. Their allocations were analysed using kappa statistics, including Fleiss's multiple kappa for groups of observers, and agreement on specific diagnoses was explored by constructing a conditional probability matrix. The nature of their disagreements was investigated using coefficients for systematic and haphazard errors. Over the four diagnostic categories there was a wide range of pairwise agreement from a low of 49% up to 72% and kappa values were only 'fair' or 'moderate'. As expected, agreement over the two categories 'dysplasia' vs 'no dysplasia' was better, ranging from 68% to 84%, and for 'atypia present' (reactive atypia, low- and high-grade dysplasia) vs "no atypia' two pairings achieved over 90% and 11 pairings over 80% agreement. In view of its clinical importance, conditional agreement on high-grade dysplasia, pairwise agreement on this diagnosis ranged from 100% down to as low as 33%. However, most of these disagreements fell into the low-grade dysplasia category so that closer follow-up and further biopsies would still have been indicated. It is a truism that the basis for safe management is careful co-operation between clinicians and pathologists who have all the relevant facts and who know and trust one another's judgement. Thus, several aspects of the ideal diagnostic process cannot be evaluated in inter-observer studies and the element of artificiality should be borne in mind when applying the findings to diagnostic practice. Nevertheless, the low level of agreement on the diagnosis of high-grade dysplasia achieved by certain pairings of specialist pathologists is a disturbing outcome of this study. Inaccuracies should be minimized by a concensus approach and we therefore recommend referral of putative cases of dysplasia to interested pathologists for further opinions. We would also advocate that pathologists faced with appearances which are indefinite between reactive atypia and dysplasia, would do better to describe them in terms of "atypia, significance uncertain', so that closer surveillance is undertaken, rather than force them into more precise diagnostic categories which may be incorrect.

摘要

六位组织病理学家将100份来自长期溃疡性结肠炎患者的切片分为四个诊断类别:普通增生、反应性异型增生、低级别和高级别发育异常。使用kappa统计分析他们的分类结果,包括用于观察组的Fleiss多重kappa,并通过构建条件概率矩阵来探讨特定诊断的一致性。使用系统误差和随机误差系数研究他们分歧的性质。在这四个诊断类别中,两两之间的一致性范围很广,从低至49%到高达72%,kappa值仅为“一般”或“中等”。正如预期的那样,“发育异常”与“无发育异常”这两个类别之间的一致性更好,范围从68%到84%,对于“存在异型增生”(反应性异型增生、低级别和高级别发育异常)与“无异型增生”,两组配对的一致性超过90%,11组配对的一致性超过80%。鉴于其临床重要性,高级别发育异常的条件一致性,该诊断的两两之间的一致性范围从100%到低至33%。然而,这些分歧大多属于低级别发育异常类别,因此仍需要更密切的随访和进一步活检。不言而喻,安全管理的基础是临床医生和病理学家之间的密切合作,他们掌握所有相关事实,并且相互了解和信任彼此的判断。因此,理想诊断过程的几个方面无法在观察者间研究中进行评估,在将研究结果应用于诊断实践时应牢记人为因素。尽管如此,某些专业病理学家配对在高级别发育异常诊断上的低一致性是本研究令人不安的结果。应通过共识方法将不准确程度降至最低,因此我们建议将疑似发育异常病例转诊给感兴趣的病理学家以获取进一步意见。我们还主张,当病理学家面对反应性异型增生和发育异常之间不确定的表现时,最好将其描述为“异型增生,意义不确定”,以便进行更密切的监测,而不是强行将它们归入可能不正确的更精确诊断类别。

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