Ferrer I, Carmona M, Blanco R, Moreno D, Torrejón-Escribano B, Olivé M
Institut Neuropatologia, Servei Anatomia Patològica, IDIBELL-Hospital Universitari de Bellvitge, Spain.
Brain Pathol. 2005 Apr;15(2):101-8. doi: 10.1111/j.1750-3639.2005.tb00504.x.
Myofibrillar myopathies (MM) are characterized morphologically by the presence of non-hyaline structures corresponding to foci of dissolution of myofibrils, and hyaline lesions composed of aggregates of compacted and degraded myofibrillar elements. Inclusion body myositis (IBM) is characterized by the presence of rimmed vacuoles, eosinophilic inclusions in the cytoplasm, rare intranuclear inclusions, and by the accumulation of several abnormal proteins. Recent studies have demonstrated impaired proteasomal expression and activity in MM and IBM, thus accounting, in part, for the abnormal protein accumulation in these diseases. The present study examines other factors involved in protein aggregation in MM and IBM. Clusterin is a multiple-function protein which participates in Abeta-amyloid, PrP(res) and a-synuclein aggregation in Alzheimer disease, prionopathies and a-synucleinopathies, respectively. gamma-Tubulin is present in the centrosome and is an intracellular marker of the aggresome. Moderate or strong clusterin immunoreactivity has been found in association with abnormal protein deposits, as revealed by immunohistochemistry, single and double-labeling immunofluorescence and confocal microscopy, in MM and IBM, and in target structures in denervation atrophy. Gamma-Tubulin has also been observed in association with abnormal protein deposits in MM, IBM, and in target fibers in denervation atrophy. These morphological findings are accompanied by increased expression of clusterin and gamma-tubulin in muscle homogenates of MM and IBM cases, as revealed by gel electrophoresis and Western blots. Together, these observations demonstrate involvement of clusterin in protein aggregates, and increased expression of aggresome markers in association with abnormal protein inclusions in MM and IBM and in targets, as crucial events related to the pathogenesis of abnormal protein accumulation and degradation in these muscular diseases.
肌原纤维肌病(MM)的形态学特征是存在与肌原纤维溶解灶相对应的非透明结构,以及由紧密排列和降解的肌原纤维成分聚集体组成的透明性病变。包涵体肌炎(IBM)的特征是存在镶边空泡、细胞质中的嗜酸性包涵体、罕见的核内包涵体,以及几种异常蛋白质的积累。最近的研究表明,MM和IBM中蛋白酶体的表达和活性受损,这在一定程度上解释了这些疾病中异常蛋白质的积累。本研究探讨了MM和IBM中蛋白质聚集所涉及的其他因素。簇集蛋白是一种多功能蛋白,分别参与阿尔茨海默病、朊病毒病和α-突触核蛋白病中的β-淀粉样蛋白、PrP(res)和α-突触核蛋白聚集。γ-微管蛋白存在于中心体中,是聚集体的细胞内标志物。通过免疫组织化学、单标和双标免疫荧光以及共聚焦显微镜检查发现,在MM和IBM以及失神经萎缩的靶结构中,中等或强的簇集蛋白免疫反应性与异常蛋白质沉积有关。在MM、IBM以及失神经萎缩的靶纤维中也观察到γ-微管蛋白与异常蛋白质沉积有关。凝胶电泳和蛋白质免疫印迹显示,这些形态学发现伴随着MM和IBM病例肌肉匀浆中簇集蛋白和γ-微管蛋白表达的增加。这些观察结果共同表明,簇集蛋白参与蛋白质聚集体的形成,并且在MM和IBM以及靶结构中,聚集体标志物的表达增加与异常蛋白质包涵体有关,这是这些肌肉疾病中异常蛋白质积累和降解发病机制的关键事件。