首页> 外文期刊>Neuropathology: official journal of the Japanese Society of Neuropathology >Colocalization of Bunina bodies and TDP‐43 inclusions in a case of sporadic amyotrophic lateral sclerosis with Lewy body‐like hyaline inclusions
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Colocalization of Bunina bodies and TDP‐43 inclusions in a case of sporadic amyotrophic lateral sclerosis with Lewy body‐like hyaline inclusions

机译:Bunina体和TDP-43夹杂物中的孢子肌萎缩侧面硬化和Lewy Body透明夹杂物的情况下夹杂物

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Sporadic amyotrophic lateral sclerosis (sALS) is characterized pathologically by loss of upper and lower motor neurons with occurrence of transactivation response DNA‐binding protein 43 kDa (TDP‐43)‐immunoreactive skein‐like and round hyaline inclusions. Lewy body‐like hyaline inclusions (LBHIs) are also found in a small proportion of sALS cases as well as in individuals with familial ALS with mutations in the Cu/Zu superoxide dismutase (SOD1) gene. LBHIs in sALS are immunopositive for TDP‐43, but not for SOD1. The occurrence of Bunina bodies (BBs) is another key pathological feature of sALS. BBs are immunonegative for TDP‐43 but immunopositive for cystatin C, transferrin, peripherin and sortilin‐related receptor CNS expressed 2 (SorCS2). Despite differences between BBs and TDP‐43 inclusions in terms of protein constituents and ultrastructure, the two inclusions are known to be linked. We recently encountered a case of sALS of 10?months duration in which many round hyaline inclusions, LBHIs and BBs were found in the anterior horn cells of the spinal cord. Our immunohistochemical and ultrastructural examinations revealed the presence of BBs within the skein‐like and round hyaline inclusions, and in the LBHIs. Colocalization of BB‐related proteins (cystatin C, transferrin and SorCS2) and TDP‐43 was also confirmed in the halo of LBHIs as well as in the marginal portion of the skein‐like and round hyaline inclusions. These findings suggest that there is some relationship between BBs and TDP‐43‐immunoreactive inclusions in terms of their formation processes.
机译:散发性肌萎缩的外侧硬化症(SAL)的特征在于,通过丧失上下电动机神经元的损失,随着转移反应DNA结合蛋白43kDA(TDP-43) - 免疫反应性伴侣和圆形透明夹杂物的出现病理。石油脂等透明夹杂物(LBHIS)也以小比例的唾液病例以及具有Cu / zu超氧化物歧化酶(SOD1)基因的突变的个体。 Sals中的LBHIS是TDP-43的免疫阳性,但不适用于SOD1。 Bunina身体(BBS)的发生是含硅的另一个关键病理特征。 BBS对于TDP-43的免疫基因,但胱抑素C,转铁蛋白,外周和分层相关受体CNS的免疫倍数表达2(Sorcs2)。尽管BBS和TDP-43在蛋白质成分和超微结构方面存在差异,但已知两个夹杂物被连接。我们最近遇到了10个月的含量为10?几个月的持续时间,其中在脊髓的前喇叭细胞中发现了许多圆形透明夹杂物,LBHI和BBS。我们的免疫组织化学和超微结构检查揭示了粉状样和圆形透明夹杂物和LBHIS内的BBS存在。在LBHI的卤素中也证实了BB相关蛋白质(胱抑素C,转铁蛋白和Sorcs2)和TDP-43的分致化,以及粉状样和圆形透明夹杂物的边缘部分。这些发现表明,BBS和TDP-43-IMM-IMM含有在其形成过程方面存在一些关系。

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