The Parkinson’s disease risk gene cathepsin B promotes fibrillar alpha-synuclein clearance, lysosomal function and glucocerebrosidase activity in dopaminergic neurons

IF 14.9 1区医学 Q1 NEUROSCIENCES

Molecular Neurodegeneration Pub Date : 2024-11-25 DOI:10.1186/s13024-024-00779-9

Jace Jones-Tabah, Kathy He, Nathan Karpilovsky, Konstantin Senkevich, Ghislaine Deyab, Isabella Pietrantonio, Thomas Goiran, Yuting Cousineau, Daria Nikanorova, Taylor Goldsmith, Esther del Cid Pellitero, Carol X.-Q. Chen, Wen Luo, Zhipeng You, Narges Abdian, Jamil Ahmad, Jennifer A. Ruskey, Farnaz Asayesh, Dan Spiegelman, Stanley Fahn, Cheryl Waters, Oury Monchi, Yves Dauvilliers, Nicolas Dupré, Irina Miliukhina, Alla Timofeeva, Anton Emelyanov, Sofya Pchelina, Lior Greenbaum, Sharon Hassin-Baer, Roy N. Alcalay, Austen Milnerwood, Thomas M. Durcan, Ziv Gan-Or, Edward A. Fon

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引用次数: 0

Abstract

Variants in the CTSB gene encoding the lysosomal hydrolase cathepsin B (catB) are associated with increased risk of Parkinson’s disease (PD). However, neither the specific CTSB variants driving these associations nor the functional pathways that link catB to PD pathogenesis have been characterized. CatB activity contributes to lysosomal protein degradation and regulates signaling processes involved in autophagy and lysosome biogenesis. Previous in vitro studies have found that catB can cleave monomeric and fibrillar alpha-synuclein, a key protein involved in the pathogenesis of PD that accumulates in the brains of PD patients. However, truncated synuclein isoforms generated by catB cleavage have an increased propensity to aggregate. Thus, catB activity could potentially contribute to lysosomal degradation and clearance of pathogenic alpha synuclein from the cell, but also has the potential of enhancing synuclein pathology by generating aggregation-prone truncations. Therefore, the mechanisms linking catB to PD pathophysiology remain to be clarified. Here, we conducted genetic analyses of the association between common and rare CTSB variants and risk of PD. We then used genetic and pharmacological approaches to manipulate catB expression and function in cell lines, induced pluripotent stem cell-derived dopaminergic neurons and midbrain organoids and assessed lysosomal activity and the handling of aggregated synuclein fibrils. We find that catB inhibition impairs autophagy, reduces glucocerebrosidase (encoded by GBA1) activity, and leads to an accumulation of lysosomal content. In cell lines, reduction of CTSB gene expression impairs the degradation of pre-formed alpha-synuclein fibrils, whereas CTSB gene activation enhances fibril clearance. In midbrain organoids and dopaminergic neurons treated with alpha-synuclein fibrils, catB inhibition potentiates the formation of inclusions which stain positively for phosphorylated alpha-synuclein. These results indicate that the reduction of catB function negatively impacts lysosomal pathways associated with PD pathogenesis, while conversely catB activation could promote the clearance of pathogenic alpha-synuclein.

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帕金森病风险基因 cathepsin B 可促进多巴胺能神经元中纤维状α-突触核蛋白的清除、溶酶体功能和葡萄糖脑苷脂酶的活性

编码溶酶体水解酶 cathepsin B（catB）的 CTSB 基因变异与帕金森病（PD）患病风险增加有关。然而，驱动这些关联的特定 CTSB 变体以及将 catB 与帕金森病发病机制联系起来的功能通路都尚未定性。CatB 的活性有助于溶酶体蛋白降解，并调节自噬和溶酶体生物生成的信号转导过程。先前的体外研究发现，catB 可以裂解单体和纤维状的α-突触核蛋白，这是一种参与脊髓灰质炎发病机制的关键蛋白，会在脊髓灰质炎患者的大脑中积聚。然而，由 catB 分解产生的截短突触核蛋白异构体具有更高的聚集倾向。因此，catB 的活性可能有助于溶酶体降解和清除细胞中的致病性α-突触核蛋白，但也有可能通过产生易聚集的截短突触核蛋白而增强突触核蛋白的病理学。因此，catB 与帕金森病病理生理学的关联机制仍有待明确。在此，我们对常见和罕见的CTSB变异与帕金森病风险之间的关联进行了遗传分析。然后，我们采用遗传学和药理学方法操纵了细胞系、诱导多能干细胞衍生的多巴胺能神经元和中脑器官组织中 catB 的表达和功能，并评估了溶酶体活性和对聚集的突触核蛋白纤维的处理。我们发现，抑制 catB 会损害自噬，降低葡萄糖脑苷脂酶（由 GBA1 编码）的活性，并导致溶酶体内容物的积累。在细胞系中，CTSB基因表达的减少会影响预先形成的α-突触核蛋白纤维的降解，而CTSB基因的激活则会增强纤维的清除。在用α-突触核蛋白纤维处理的中脑器官组织和多巴胺能神经元中，catB抑制可促进包涵体的形成，包涵体对磷酸化的α-突触核蛋白染色呈阳性。这些结果表明，catB功能的降低会对与帕金森病发病机制相关的溶酶体通路产生负面影响，反之，catB的激活则会促进致病性α-突触核蛋白的清除。

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来源期刊

Molecular Neurodegeneration 医学-神经科学

CiteScore

23.00

自引率

4.60%

发文量

审稿时长

6-12 weeks

期刊介绍： Molecular Neurodegeneration, an open-access, peer-reviewed journal, comprehensively covers neurodegeneration research at the molecular and cellular levels. Neurodegenerative diseases, such as Alzheimer's, Parkinson's, Huntington's, and prion diseases, fall under its purview. These disorders, often linked to advanced aging and characterized by varying degrees of dementia, pose a significant public health concern with the growing aging population. Recent strides in understanding the molecular and cellular mechanisms of these neurodegenerative disorders offer valuable insights into their pathogenesis.