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艾滋病及艾滋病前期的进行性多灶性白质脑病(PML)。使用免疫细胞化学和原位DNA杂交进行病毒检测的神经病理学比较。

Progressive multifocal leukoencephalopathy (PML) in AIDS and in the pre-AIDS era. A neuropathological comparison using immunocytochemistry and in situ DNA hybridization for virus detection.

作者信息

Schmidbauer M, Budka H, Shah K V

机构信息

Neurologisches Institut, Universität Wien, Austria.

出版信息

Acta Neuropathol. 1990;80(4):375-80. doi: 10.1007/BF00307690.

DOI:10.1007/BF00307690
PMID:2173328
Abstract

Twenty-five brains with definite, and three brains with possible, progressive multifocal leukoencephalopathy (PML), including six brains of AIDS patients, were studied with special regard to the detection of papovaviruses. Formalin-fixed serial paraffin sections were immunostained with monospecific anti-JC virus (JCV) and genus-specific anti-simian virus (SV) 40 antisera, and hybridized in situ with DNA probes for JCV and SV 40, respectively. Immunocytochemistry (ICC) and in situ hybridization (ISH) were similarly sensitive in detecting virus in classical PML lesions. In all but one definite PML cases at least one method detected virus (96%). Possible PML tissue was never labeled. Labeling patterns were generally similar in ICC and ISH: mainly oligodendroglia and, less frequently, astroglia harbored virus, whereas labeling of neurons and endothelia was absent. Bizarre giant astrocytes were occasionally labeled by ICC and ISH. Burnt-out lesions harbored JCV DNA but not virus antigens. SV 40 DNA was never detectable. PML morphology in AIDS cases did not usually differ from the disease process seen in the pre-AIDS era. However, two AIDS brains presented extremely extended and, in one case, unusually necrotizing PML damage; in the latter case, PML lesions contained large amounts not only of JCV, but also of human immunodeficiency virus (HIV) antigens. We conclude that ICC and ISH are methods of comparable sensitivity for detection of papovavirus in fluorishing PML lesions. In burnt-out PML lesions only ISH may detect virus. The possibility of an exceptional non-JCV (e.g., SV 40) etiology of PML could be neither confirmed nor disproved. In AIDS, massive coinfection by HIV of PML lesions may increase damage to tissue, resulting in unusually extended and necrotizing PML.

摘要

对25例确诊为进行性多灶性白质脑病(PML)以及3例可能患有PML的大脑进行了研究,特别关注乳头多瘤空泡病毒的检测,其中包括6例艾滋病患者的大脑。用单特异性抗JC病毒(JCV)和属特异性抗猴病毒(SV)40抗血清对福尔马林固定的连续石蜡切片进行免疫染色,并分别用JCV和SV 40的DNA探针进行原位杂交。免疫细胞化学(ICC)和原位杂交(ISH)在检测典型PML病变中的病毒时敏感性相似。在除1例确诊PML病例外的所有病例中,至少有一种方法检测到了病毒(96%)。可能患有PML的组织从未被标记。ICC和ISH中的标记模式通常相似:主要是少突胶质细胞携带病毒,星形胶质细胞携带病毒的情况较少,而神经元和内皮细胞无标记。奇异的巨大星形胶质细胞偶尔被ICC和ISH标记。陈旧性病变含有JCV DNA但无病毒抗原。从未检测到SV 40 DNA。艾滋病病例中的PML形态通常与艾滋病前期所见的疾病过程无差异。然而,2例艾滋病患者的大脑呈现出极其广泛的病变,其中1例出现异常坏死性PML损害;在后一种情况下,PML病变不仅含有大量JCV,还含有大量人类免疫缺陷病毒(HIV)抗原。我们得出结论,ICC和ISH是检测活跃PML病变中乳头多瘤空泡病毒的敏感性相当的方法。在陈旧性PML病变中,只有ISH可能检测到病毒。PML由非JCV(如SV 40)引起的特殊病因的可能性既无法证实也无法排除。在艾滋病中,PML病变被HIV大量合并感染可能会增加对组织的损害,导致异常广泛和坏死性的PML。

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Progressive multifocal leukoencephalopathy.进行性多灶性白质脑病
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