帕金森病相关突变体DNAJC13（N855S）导致其加速降解并对巨噬和逆转录复合物介导的动力学产生负面影响

IF 4 2区生物学 Q2 CELL BIOLOGY

Journal of Cellular Physiology Pub Date : 2025-07-27 DOI:10.1002/jcp.70074

Anna Stein, Stella Vo, Christian Freese, Joram Kluge, Joanna Maus, Ingrid Koziollek-Drechsler, Beate Silva, Christian Behl, Albrecht M. Clement

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引用次数: 0

摘要

虽然帕金森病具有多因素病因，但5%-10%的病例存在可识别的致病基因突变。进一步研究这些突变是确定潜在病理机制的一种方法。其中一种罕见的帕金森相关基因是DNAJC13，编码一种内核体相关蛋白。一些证据表明，紊乱的内体通路在帕金森病的发展中起着重要作用。最近，我们已经证明DNAJC13/RME-8是自噬的积极调节剂，自噬是溶酶体相关的降解过程。在这里，我们进一步表征了疾病相关的DNAJC13（N855S）突变体的作用，并通过使用DNAJC13表达降低的新建立的细胞系和瞬时表达DNAJC13（N855S）突变体进行生化、细胞生物学、共定位和表达分析。我们观察到，DNAJC13（N855S）变体比野生型蛋白更不稳定，因此可能影响蛋白质静止。此外，该蛋白具有功能缺陷，因为它不能补偿长期降低DNAJC13水平的细胞中受损的自噬活性。此外，DNAJC13（N855S）对阳离子非依赖性甘露糖-6-磷酸受体的分布表现出明显的负向影响，但不影响组织蛋白酶D的总体水平或活性。最后，我们观察到在稳定的DNAJC13敲低细胞中，一些与自噬诱导和生物发生相关的基因表达降低。我们的数据指向DNAJC13（N855S）变异的功能丧失机制，并且长期降低DNAJC13蛋白水平导致主要参与内体运输和自噬体生物发生的基因表达减少。因此，DNAJC13（N855S）突变体可能部分由于其不稳定性和部分由于对自噬途径的主要负面影响而引起疾病。这些数据支持了内体通路损伤在帕金森病发病机制中的关键作用。

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The Parkinson Disease-Associated Mutant DNAJC13(N855S) Leads to Its Accelerated Degradation and Negatively Affects Macroautophagy and Retromer Complex-Mediated Dynamics

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The Parkinson Disease-Associated Mutant DNAJC13(N855S) Leads to Its Accelerated Degradation and Negatively Affects Macroautophagy and Retromer Complex-Mediated Dynamics

While Parkinson′s disease has a multifactorial etiology, 5%–10% of cases present with identifiable disease-causing gene mutations. Further investigation into these mutations is a way to identify underlying pathologic mechanism. One of the rare Parkinson-associated genes is DNAJC13, coding for an endosome-associated protein. Several lines of evidence suggest that disturbed endosomal pathways are instrumental in the development of Parkinson pathology. Recently, we have shown that DNAJC13/RME-8 is a positive modulator of autophagy, a lysosome-associated degradative process. Here, we further characterize the role of the disease-linked DNAJC13(N855S) mutant and perform biochemical, cell biological, co-localization, and expression analysis by employing a newly established cell line with reduced DNAJC13 expression and by transiently expressing the DNAJC13(N855S) mutant variant. We observed that the DNAJC13(N855S) variant is less stable than the wild-type protein and might thus impact proteostasis. Furthermore, the protein has functional deficits as it cannot compensate for the impaired autophagic activity in cells with chronically reduced DNAJC13 levels. In addition, the DNAJC13(N855S) showed a dominant negative effect on the distribution of the cation-independent mannose-6-phosphate receptor without affecting overall cathepsin D levels or activity. Lastly, we observed a decreased expression of several genes related to autophagy induction and biogenesis in stable DNAJC13 knockdown cells. Our data point toward a loss-of-function mechanism of the DNAJC13(N855S) variant and that chronically reduced DNAJC13 protein levels result in a reduced expression of genes largely involved in endosomal traffic and autophagosome biogenesis. The DNAJC13(N855S) mutant might thus cause disease in part by its instability and in part by a dominant negative effect on the autophagic pathway. These data support a pivotal role of endosomal pathway impairment in Parkinson′s disease pathogenesis.

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来源期刊

Journal of Cellular Physiology 生物-生理学

CiteScore

14.70

自引率

0.00%

发文量

256

审稿时长

1 months

期刊介绍： The Journal of Cellular Physiology publishes reports of high biological significance in areas of eukaryotic cell biology and physiology, focusing on those articles that adopt a molecular mechanistic approach to investigate cell structure and function. There is appreciation for the application of cellular, biochemical, molecular and in vivo genetic approaches, as well as the power of genomics, proteomics, bioinformatics and systems biology. In particular, the Journal encourages submission of high-interest papers investigating the genetic and epigenetic regulation of proliferation and phenotype as well as cell fate and lineage commitment by growth factors, cytokines and their cognate receptors and signal transduction pathways that influence the expression, integration and activities of these physiological mediators. Similarly, the Journal encourages submission of manuscripts exploring the regulation of growth and differentiation by cell adhesion molecules in addition to the interplay between these processes and those induced by growth factors and cytokines. Studies on the genes and processes that regulate cell cycle progression and phase transition in eukaryotic cells, and the mechanisms that determine whether cells enter quiescence, proliferate or undergo apoptosis are also welcomed. Submission of papers that address contributions of the extracellular matrix to cellular phenotypes and physiological control as well as regulatory mechanisms governing fertilization, embryogenesis, gametogenesis, cell fate, lineage commitment, differentiation, development and dynamic parameters of cell motility are encouraged. Finally, the investigation of stem cells and changes that differentiate cancer cells from normal cells including studies on the properties and functions of oncogenes and tumor suppressor genes will remain as one of the major interests of the Journal.