Kramer I R, Lucas R B, el-Labban N, Lister L
Br J Cancer. 1970 Dec;24(4):673-83. doi: 10.1038/bjc.1970.80.
In a retrospective survey of 235 cases in which the diagnosis on biopsy was lichen planus, keratosis or leukoplakia, the histological features were re-assessed as objectively as possible and without reference to the original diagnosis.The tissue changes were recorded under 39 headings, and many were assessed on a roughly quantitative basis. In addition, two clinical features were included; whether the biopsy was from the buccal mucosa (as opposed to some other intraoral site) and whether the lesions involved multiple intraoral sites. For each possible pair of diagnostic categories (keratosis and leukoplakia, lichen planus and keratosis, lichen planus and leukoplakia) the recorded findings were subjected to discriminant analysis in order to provide a quantitative assessment of the value of each individual feature for discriminating between the two diagnostic groups. The computer programme also provided for the application of these calculated values to yield a "score" for each case, and for an assessment of the significance of the separation of the diagnostic groups thus achieved. In general, the values calculated by the computer for the discriminatory value of each tissue change accorded with our subjective impressions, but a number of features that were given a relatively high value had not previously been recognized as important in differential diagnosisA discriminant analysis was also performed on those cases of leukoplakia known to have later developed a carcinoma, in comparison with the leukoplakia cases that did not develop carcinoma. High values were accorded mainly to the well-known features of epithelial atypia, but a similar high value was indicated for the presence of Russell bodies. we had not previously realized that the presence of Russell bodies was of prognostic significance in this context.When the total scores for the groups of cases were analysed, it was found that the separation of each pair of diagnostic groups was significant at the 1% level. The separation of leukoplakia cases that subsequently developed carcinoma, from those that did not develop carcinoma, was significant at the 5% level. In this latter analysis, a better separation might be achieved with larger numbers of cases, but there will always be the complicating factor that an unknown number of leukoplakia cases would develop carcinoma if the patient had received no treatment.
在一项对235例活检诊断为扁平苔藓、角化病或白斑的病例的回顾性调查中,尽可能客观地重新评估了组织学特征,且不参考原始诊断。组织变化按照39个项目进行记录,许多项目进行了大致的定量评估。此外,还纳入了两个临床特征:活检是否取自颊黏膜(相对于其他口腔内部位)以及病变是否累及多个口腔内部位。对于每一对可能的诊断类别(角化病和白斑、扁平苔藓和角化病、扁平苔藓和白斑),对记录的结果进行判别分析,以便对每个个体特征在区分两个诊断组方面的价值进行定量评估。计算机程序还用于应用这些计算值为每个病例得出一个“分数”,并评估由此实现的诊断组分离的显著性。总体而言,计算机计算出的每个组织变化的鉴别值与我们的主观印象相符,但一些被赋予相对较高值的特征此前未被认为在鉴别诊断中很重要。还对已知后来发展为癌的白斑病例与未发展为癌的白斑病例进行了判别分析。高值主要赋予了上皮异型性这一众所周知的特征,但Russell小体的存在也显示出类似的高值。我们此前没有意识到Russell小体的存在在此背景下具有预后意义。当分析病例组的总分时,发现每对诊断组的分离在1%水平上具有显著性。后来发展为癌的白斑病例与未发展为癌的白斑病例的分离在5%水平上具有显著性。在后者的分析中,增加病例数量可能会实现更好的分离,但总会存在一个复杂因素,即如果患者未接受治疗,未知数量的白斑病例会发展为癌。
