Mitochondrial localization of the Parkinson's disease related protein DJ-1: implications for pathogenesis

生物 亚细胞定位 线粒体 细胞分离 免疫金标记 分子生物学 蛋白质亚细胞定位预测 突变体 细胞生物学 膜间隙 热休克蛋白A9 基因 细胞质 生物化学 细菌外膜 遗传学 抗体 肽序列 大肠杆菌
作者
Li Zhang,Mika Shimoji,Bobby Thomas,Darren J. Moore,Seong-Woon Yu,Neena I. Marupudi,Reidun Torp,I A Torgner,Ole Petter Ottersen,Ted M. Dawson,Valina L. Dawson
出处
期刊:Human Molecular Genetics [Oxford University Press]
卷期号:14 (14): 2063-2073 被引量:413
标识
DOI:10.1093/hmg/ddi211
摘要

Both homozygous (L166P, M26I, deletion) and heterozygous mutations (D149A, A104T) in the DJ-1 gene have been identified in Parkinson's disease (PD) patients. The biochemical function and subcellular localization of DJ-1 protein have not been clarified. To date the localization of DJ-1 protein has largely been described in studies over-expressing tagged DJ-1 protein in vitro. It is not known whether the subcellular localization of over-expressed DJ-1 protein is identical to that of endogenously expressed DJ-1 protein both in vitro and in vivo. To clarify the subcellular localization and function of DJ-1, we generated three highly specific antibodies to DJ-1 protein and investigated the subcellular localization of endogenous DJ-1 protein in both mouse brain tissues and human neuroblastoma cells. We have found that DJ-1 is widely distributed and is highly expressed in the brain. By cell fractionation and immunogold electron microscopy, we have identified an endogenous pool of DJ-1 in mitochondrial matrix and inter-membrane space. To further investigate whether pathogenic mutations might prevent the distribution of DJ-1 to mitochondria, we generated human neuroblastoma cells stably transfected with wild-type (WT) or mutant (M26I, L166P, A104T, D149A) DJ-1 and performed mitochondrial fractionation and confocal co-localization imaging studies. When compared with WT and other mutants, L166P mutant exhibits largely reduced protein level. However, the pathogenic mutations do not alter the distribution of DJ-1 to mitochondria. Thus, DJ-1 is an integral mitochondrial protein that may have important functions in regulating mitochondrial physiology. Our findings of DJ-1's mitochondrial localization may have important implications for understanding the pathogenesis of PD.

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