Wei Jianshe, Fujita Masayo, Nakai Masaaki, Waragai Masaaki, Watabe Kazuhiko, Akatsu Hiroyasu, Rockenstein Edward, Masliah Eliezer, Hashimoto Makoto
Laboratory for Chemistry and Metabolism, Tokyo Metropolitan Institute for Neuroscience, 2-6 Musashidai, Fuchu, Tokyo 183-8526, Japan.
Laboratory for Molecular Neuropathology, Tokyo Metropolitan Institute for Neuroscience, 2-6 Musashidai, Fuchu, Tokyo 183-8526, Japan.
J Biol Chem. 2007 Sep 28;282(39):28904-28914. doi: 10.1074/jbc.M703711200. Epub 2007 Jul 24.
Two missense mutations (P123H and V70M) of beta-synuclein (beta-syn), the homologue of alpha-syn, have been recently identified in dementia with Lewy bodies. However, the mechanism through which these mutations influence the pathogenesis of dementia with Lewy bodies is unclear. To investigate the role of the beta-syn mutations in neurodegeneration, each mutant was stably transfected into B103 neuroblastoma cells. Cells overexpressing mutated beta-syn had eosinophilic cytoplasmic inclusion bodies immunopositive for mutant beta-syn, and electron microscopy revealed that these cells were abundant in various cytoplasmic membranous inclusions resembling the histopathology of lysosomal storage disease. Consistent with these findings, the inclusion bodies were immunopositive for lysosomal markers, including cathepsin B, LAMP-2, GM2 ganglioside, and ATP13A2, which has recently been linked to PARK9. Notably, formation of these lysosomal inclusions was greatly stimulated by co-expression of alpha-syn, was dependent on the phosphorylation of alpha-syn at Ser-129, and was more efficient with the A53T familial mutant of alpha-syn compared with wild type. Furthermore, the inclusion formation in cells overexpressing mutant beta-syn and transfected with alpha-syn was significantly suppressed by treatment with autophagy-lysosomal inhibitors, which were associated with impaired clearance of syn proteins and enhanced apoptosis, indicating that formation of lysosomal inclusions might be protective. Collectively, the results demonstrated unambiguously that overexpression of beta-syn mutants (P123H and V70M) in neuroblastoma cells results in an enhanced lysosomal pathology. We suggest that these missense mutations of beta-syn might play a causative role in stimulating neurodegeneration.
α-突触核蛋白的同源物β-突触核蛋白(β-syn)的两个错义突变(P123H和V70M)最近在路易体痴呆中被发现。然而,这些突变影响路易体痴呆发病机制的具体机制尚不清楚。为了研究β-突触核蛋白突变在神经退行性变中的作用,将每个突变体稳定转染到B103神经母细胞瘤细胞中。过表达突变型β-突触核蛋白的细胞含有对突变型β-突触核蛋白呈免疫阳性的嗜酸性细胞质包涵体,电子显微镜显示这些细胞富含各种细胞质膜性包涵体,类似于溶酶体贮积病的组织病理学表现。与这些发现一致,这些包涵体对溶酶体标记物呈免疫阳性,包括组织蛋白酶B、溶酶体相关膜蛋白2(LAMP-2)、GM2神经节苷脂和最近与帕金森病9型(PARK9)相关的ATP13A2。值得注意的是,α-突触核蛋白的共表达极大地刺激了这些溶酶体包涵体的形成,其依赖于α-突触核蛋白在丝氨酸129位点的磷酸化,并且与野生型相比,α-突触核蛋白的A53T家族突变体更有效。此外,用自噬-溶酶体抑制剂处理可显著抑制过表达突变型β-突触核蛋白并转染α-突触核蛋白的细胞中的包涵体形成,这与突触蛋白清除受损和细胞凋亡增强有关,表明溶酶体包涵体的形成可能具有保护作用。总的来说,结果明确表明神经母细胞瘤细胞中β-突触核蛋白突变体(P123H和V70M)的过表达导致溶酶体病理学增强。我们认为β-突触核蛋白的这些错义突变可能在刺激神经退行性变中起致病作用。
