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突触素在人脊髓中的表达。一项免疫组织化学研究的诊断意义。

Synaptophysin expression in the human spinal cord. Diagnostic implications of an immunohistochemical study.

作者信息

Zhang P J, Rosenblum M K

机构信息

Department of Pathology, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA.

出版信息

Am J Surg Pathol. 1996 Mar;20(3):273-6. doi: 10.1097/00000478-199603000-00002.

Abstract

Surface perikaryal labeling on immunohistochemical assay for synaptophysin (SYN)--a glycoprotein component of synaptic vesicle membranes--has been posited to distinguish the neoplastic neuronal elements of gangliogliomas from native central nervous system neurons overrun by gliomas invasive of gray matter. To assess the validity of this criterion in the evaluation of intramedullary neoplasms, we screened formalin-fixed, paraffin-embedded sections from 35 histologically unremarkable spinal cords (removed at autopsy) using commercially available monoclonal antibodies to SYN. All specimens exhibited anti-SYN reactivity, which was confined to gray matter, and all evidenced the concentrated deposition of reaction product along the perikarya of large neurons in the anterior horns, Clarke's columns, and intermediolateral cell columns. A majority (23 specimens) contained neurons completely outlined by reaction product rings comparable to those depicted as being pathognomonic of neuronal neoplasia. This phenomenon presumably reflects the rich complement of axosomatic synapses documented in fine structural studies of the normal spinal cord. Surface perikaryal labeling for SYN is not restricted to the neoplastic neurons of ganglion cell tumors and should be cautiously interpreted, particularly when neurosurgical material derives from the spinal cord.

摘要

免疫组织化学检测突触素(SYN,突触小泡膜的一种糖蛋白成分)时的表面核周标记,被认为可将神经节胶质瘤的肿瘤性神经元成分与被侵犯灰质的胶质瘤所累及的中枢神经系统天然神经元区分开来。为评估该标准在评估髓内肿瘤中的有效性,我们使用市售抗SYN单克隆抗体,对35例组织学无异常的脊髓(尸检时取出)的福尔马林固定、石蜡包埋切片进行了筛查。所有标本均显示抗SYN反应性,且局限于灰质,所有标本均显示反应产物在前角大神经元、克拉克柱和中间外侧细胞柱的核周集中沉积。大多数(23例标本)含有被反应产物环完全勾勒出轮廓的神经元,这些环与被描述为神经元肿瘤特征性的环相似。这种现象可能反映了正常脊髓超微结构研究中记录的丰富的轴体突触。SYN的表面核周标记并不局限于神经节细胞瘤的肿瘤性神经元,应谨慎解释,尤其是当神经外科材料来自脊髓时。

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