Jesse C M, Bushuven E, Tripathi P, Chandrasekar A, Simon C M, Drepper C, Yamoah A, Dreser A, Katona I, Johann S, Beyer C, Wagner S, Grond M, Nikolin S, Anink J, Troost D, Sendtner M, Goswami A, Weis J
Institute of Neuropathology, RWTH Aachen University Medical School, Pauwelsstr. 30, 52074 Aachen, Germany.
Department of Neurosurgery, RWTH Aachen University Medical School, Pauwelsstr. 30, 52074 Aachen, Germany.
Brain Pathol. 2017 Nov;27(6):781-794. doi: 10.1111/bpa.12453. Epub 2017 Feb 15.
Alpha-motoneurons and muscle fibres are structurally and functionally interdependent. Both cell types particularly rely on endoplasmic reticulum (ER/SR) functions. Mutations of the ER proteins VAPB, SigR1 and HSP27 lead to hereditary motor neuron diseases (MNDs). Here, we determined the expression profile and localization of these ER proteins/chaperons by immunohistochemistry and immunoblotting in biopsy and autopsy muscle tissue of patients with amyotrophic lateral sclerosis (ALS) and other neurogenic muscular atrophies (NMAs) and compared these patterns to mouse models of neurogenic muscular atrophy. Postsynaptic neuromuscular junction staining for VAPB was intense in normal human and mouse muscle and decreased in denervated Nmd mouse muscle fibres. In contrast, VAPB levels together with other chaperones and autophagy markers were increased in extrasynaptic regions of denervated muscle fibres of patients with MNDs and other NMAs, especially at sites of focal myofibrillar disintegration (targets). These findings did not differ between NMAs due to ALS and other causes. G93A-SOD1 mouse muscle fibres showed a similar pattern of protein level increases in denervated muscle fibres. In addition, they showed globular VAPB-immunoreactive structures together with misfolded SOD1 protein accumulations, suggesting a primary myopathic change. Our findings indicate that altered expression and localization of these ER proteins and autophagy markers are part of the dynamic response of muscle fibres to denervation. The ER is particularly prominent and vulnerable in both muscle fibres and alpha-motoneurons. Thus, ER pathology could contribute to the selective build-up of degenerative changes in the neuromuscular axis in MNDs.
α运动神经元和肌纤维在结构和功能上相互依存。这两种细胞类型都特别依赖内质网(ER/SR)的功能。内质网蛋白VAPB、SigR1和HSP27的突变会导致遗传性运动神经元疾病(MNDs)。在这里,我们通过免疫组织化学和免疫印迹法,确定了这些内质网蛋白/伴侣蛋白在肌萎缩侧索硬化症(ALS)和其他神经源性肌肉萎缩症(NMA)患者的活检和尸检肌肉组织中的表达谱和定位,并将这些模式与神经源性肌肉萎缩的小鼠模型进行了比较。在正常人和小鼠肌肉中,VAPB的突触后神经肌肉接头染色强烈,而在去神经支配的Nmd小鼠肌纤维中则减弱。相反,在患有MNDs和其他NMA的患者的去神经支配肌纤维的突触外区域,VAPB水平与其他伴侣蛋白和自噬标记物一起升高,尤其是在局灶性肌原纤维解体部位(靶点)。由ALS和其他原因引起的NMA之间的这些发现没有差异。G93A-SOD1小鼠肌纤维在去神经支配的肌纤维中显示出类似的蛋白质水平升高模式。此外,它们还显示出球状VAPB免疫反应性结构以及错误折叠的SOD1蛋白积累,提示原发性肌病改变。我们的研究结果表明,这些内质网蛋白和自噬标记物表达和定位的改变是肌纤维对去神经支配动态反应的一部分。内质网在肌纤维和α运动神经元中都特别突出且易受影响。因此,内质网病理学可能导致MNDs中神经肌肉轴上退行性变化的选择性积累。