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免疫组织化学法对恶性间皮瘤组织学诊断的再评价。

Re-evaluation of histological diagnoses of malignant mesothelioma by immunohistochemistry.

机构信息

Department of Pathology and Medical Genetics, St, Olav University Hospital, Erling Skjalgssons gt, 1, N-7006 Trondheim, Norway.

出版信息

Diagn Pathol. 2010 Jul 6;5:47. doi: 10.1186/1746-1596-5-47.

Abstract

BACKGROUND

In order to provide reliable tissue material for malignant mesothelioma (MM) studies, we re-evaluated biopsies and autopsy material from 61 patients with a diagnosis of MM from the period of 1980-2002.

METHODS

Basic positive (Calretinin, EMA, Podoplanin, Mesothelin) and negative (CEA, Ber-Ep4) immunohistochemical (IHC) marker reactions were determined. If needed, more markers were used. Histological diagnoses were made by three pathologists. Survival data were calculated.

RESULTS

49 cases (80%) were considered being MM by a high degree of likelihood, five more cases possible MM. Of the remaining seven cases, three were diagnosed as adenocarcinoma, three as pleomorphic lung carcinoma, in one peritoneal case a clear entity diagnosis could not be given. One of the possible MM cases and two of the lung carcinoma cases had this already as primary diagnoses, but were registered as MM.With a sensitivity of 100%, Calretinin and CEA were the most reliable single markers. The amount of MM cells with positive immunoreactivity (IR) for Podoplanin and Mesothelin showed most reliable inverse relation to the degree of atypia.In the confirmed MM cases, there had been applied either no IHC or between one and 18 markers.The cases not confirmed by us had either lacked IHC (n = 1), non-specific markers were used (n = 4), IR was different (n = 1), or specific markers had not shown positive IR in the right part of the tumour cells (n = 3).46 of the 49 confirmed and three of the not confirmed cases had been diagnosed by us as most likely MM before IHC was carried out.

CONCLUSIONS

In order to use archival tissue material with an earlier MM diagnosis for studies, histopathological re-evaluation is important. In possible sarcomatous MM cases without any positive IR for positive MM markers, radiology and clinical picture are essential parts of diagnostics. IHC based on a panel of two positive and two negative MM markers has to be adapted to the differential diagnostic needs in each single case. New diagnostic tools and techniques are desirable for cases where IHC and other established methods cannot provide a clear entity diagnosis, and in order to improve MM treatment.

摘要

背景

为了给恶性间皮瘤(MM)的研究提供可靠的组织材料,我们重新评估了 1980 年至 2002 年间诊断为 MM 的 61 例患者的活检和尸检材料。

方法

确定基本的阳性(钙视网膜蛋白、EMA、Podoplanin、间皮素)和阴性(CEA、Ber-Ep4)免疫组织化学(IHC)标志物反应。如果需要,还会使用更多的标志物。组织学诊断由三位病理学家做出。计算生存数据。

结果

49 例(80%)被高度可能地诊断为 MM,另外 5 例可能为 MM。在其余 7 例中,3 例诊断为腺癌,3 例诊断为多形性肺癌,1 例腹膜病例无法明确实体诊断。1 例可能的 MM 病例和 2 例肺癌病例已被诊断为原发性疾病,但被登记为 MM。钙视网膜蛋白和 CEA 的敏感性为 100%,是最可靠的单一标志物。Podoplanin 和间皮素的阳性免疫反应(IR)的 MM 细胞数量与异型性程度呈最可靠的反比关系。在确诊的 MM 病例中,应用的免疫组化标记物数量为 1 至 18 种。未被我们确诊的病例要么缺乏免疫组化(n=1),要么使用了非特异性标志物(n=4),要么免疫反应不同(n=1),要么特异性标志物在肿瘤细胞的右部分未显示阳性 IR(n=3)。在我们进行免疫组化之前,49 例确诊病例中的 46 例和 3 例未确诊病例中的 3 例被我们诊断为最有可能的 MM。

结论

为了使用之前 MM 诊断的存档组织材料进行研究,组织病理学重新评估很重要。在没有任何阳性 MM 标志物阳性 IR 的可能肉瘤样 MM 病例中,放射学和临床表现是诊断的重要组成部分。基于两种阳性和两种阴性 MM 标志物的 IHC 必须适应每个病例的不同诊断需求。对于那些免疫组化和其他已建立的方法无法提供明确实体诊断的病例,以及为了改善 MM 治疗效果,需要新的诊断工具和技术。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0043/2915960/e828f66ca079/1746-1596-5-47-1.jpg

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