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进行性多灶性白质脑病诊断中的可能陷阱。

Possible pitfalls in the diagnostic of progressive multifocal leukoencephalopathy.

作者信息

Zivanovic Milanka, Savšek Lina, Poljak Mario, Popovic Mara

出版信息

Clin Neuropathol. 2016 Mar-Apr;35(2):66-71. doi: 10.5414/NP300911.

Abstract

The most accurate diagnosis of clinically suspected progressive multifocal leukoencephalopathy (PML) is made by neuronavigated needle brain biopsy and microscopic examination of the specimen confirming typical morphological features of the disease and, additionally, using immunohistochemistry (IHC) for detection of early viral proteins of the etiologic agent - polyoma virus JC (JCV). Due to the small biopsy volume, this approach can sometimes fail to confirm the clinical diagnosis of PML, as demonstrated by the presented clinical case. To check the reliability of using only IHC, we additionally tested 6 archival cases from our institute using IHC, in-situ hybridization (ISH) and real-time polymerase chain reaction (PCR). In the presented case, both biopsy and autopsy material were tested, in three archival cases only biopsy material and in the remaining cases post-mortem brain tissue was available. IHC (Anti-SV40 T antigen, mAb Pab416) was negative in 3 samples, in another 3 fewer than 10 cells per one ×20 microscopic field were positive. In our study, ISH proved to be a more sensitive method for JCV detection than IHC, being positive in all cases. Out of 7 tested specimens, realtime PCR failed to confirm the presence of JCV in 1 specimen, which was the oldest brain autopsy of an AIDS patient. Our study demonstrated that, especially when confronted with borderline clinical suspicion of PML and when only a small biopsy specimen is available, a combination of at least two different methods for JCV detection should be considered, preferably IHC with one of the available molecular methods.

摘要

临床疑似进行性多灶性白质脑病(PML)的最准确诊断是通过神经导航针脑活检及对标本进行显微镜检查,确认疾病的典型形态特征,此外,还需使用免疫组织化学(IHC)检测病原体多瘤病毒JC(JCV)的早期病毒蛋白。由于活检样本量小,这种方法有时无法确诊PML,如本文所展示的临床病例。为检验仅使用免疫组织化学的可靠性,我们另外对本机构的6例存档病例进行了免疫组织化学、原位杂交(ISH)和实时聚合酶链反应(PCR)检测。在本文所述病例中,对活检和尸检材料均进行了检测,3例存档病例仅检测了活检材料,其余病例仅有死后脑组织可用。免疫组织化学(抗SV40 T抗原,单克隆抗体Pab416)检测中,3份样本呈阴性,另外3份样本在每20倍显微镜视野下阳性细胞少于10个。在我们的研究中,原位杂交被证明是一种比免疫组织化学更敏感的检测JCV的方法,所有病例均呈阳性。在7份检测标本中,实时PCR未能在1份标本中确认JCV的存在,该标本是一名艾滋病患者最陈旧的脑尸检样本。我们的研究表明,特别是当面对PML临床疑似程度处于临界状态且仅有少量活检标本可用时,应考虑至少结合两种不同的JCV检测方法,最好是免疫组织化学与一种可用的分子方法相结合。

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