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多发性硬化症病灶中髓鞘相关糖蛋白和髓鞘碱性蛋白分布的免疫细胞化学观察

Immunocytochemical observations on the distribution of myelin-associated glycoprotein and myelin basic protein in multiple sclerosis lesions.

作者信息

Itoyama Y, Sternberger N H, Webster H D, Quarles R H, Cohen S R, Richardson E P

出版信息

Ann Neurol. 1980 Feb;7(2):167-77. doi: 10.1002/ana.410070212.

DOI:10.1002/ana.410070212
PMID:6154440
Abstract

To study the distribution of myelin-associated glycoprotein (MAG) in human nervous tissue and in multiple sclerosis (MS) lesions, we used paraffin sections and our modification of the peroxidase-antiperoxidase technique. Sections of MS lesions also were treated with antiserum to basic protein (BP) and with histological stains for axons and myelin sheaths. In tissue from normal developing central nervous system, oligodendroglia, their processes, and wwly formed myelin sheaths were intensely stained by MAG antiserum. In adults, MAG was found in periaxonal regions of myelinated fibers of the central and peripheral nervous system. The most striking finding in MS lesions was the extension of decreased MAG immunostaining into white matter that appeared normal when treated with BP antiserum or luxol fast blue. In acute early MS lesions the decrease in MAG immunostaining extended far beyond the margin of acute demyelination, where the BP staining of degenerating sheaths often was increased. In chronic inactive plaques, this decrease in periaxonal MAG immunostaining was limited to relatively few fibers in a thin rim around each lesion. These observations suggest that in MS, immunoreactivity of periaxonal MAG is altered before myelin breakdown begins. Early in degeneration, myelin sheaths and their fragments often were more intensely stained by BP antiserum than normal sheaths; later the staining intensity decreased. In shadow plaques, BP antiserum stained some oligodendroglia. Their appearance and location among thinly myelinated axons suggested that these oligondendroglia were forming new sheaths around previously demyelinated axons.

摘要

为研究髓鞘相关糖蛋白(MAG)在人类神经组织及多发性硬化(MS)病灶中的分布,我们采用石蜡切片及改良的过氧化物酶-抗过氧化物酶技术。MS病灶切片还用碱性蛋白(BP)抗血清及轴突和髓鞘的组织学染色剂进行处理。在正常发育的中枢神经系统组织中,少突胶质细胞、其突起及新形成的髓鞘被MAG抗血清强烈染色。在成年人中,MAG见于中枢和周围神经系统有髓纤维的轴周区域。MS病灶中最显著的发现是,在用BP抗血清或变色酸2R染色时看似正常的白质中,MAG免疫染色减少的区域扩大。在急性早期MS病灶中,MAG免疫染色减少的区域远远超出急性脱髓鞘边缘,在该边缘处,退化髓鞘的BP染色常常增加。在慢性静止斑块中,轴周MAG免疫染色的减少仅限于每个病灶周围薄边缘内相对较少的纤维。这些观察结果提示,在MS中,轴周MAG的免疫反应性在髓鞘破坏开始之前就已改变。在退变早期,髓鞘及其碎片常常比正常髓鞘被BP抗血清染色更强;之后染色强度降低。在影斑中,BP抗血清可染一些少突胶质细胞。它们在薄髓鞘轴突中的外观和位置提示,这些少突胶质细胞正在先前脱髓鞘的轴突周围形成新的髓鞘。

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