LRRK2/ dlrrk介导的溶酶体途径参与胶质细胞死亡和DA神经元存活。

IF 3.6 3区 生物学 Q3 CELL BIOLOGY Traffic Pub Date : 2022-10-01 Epub Date: 2022-09-11 DOI:10.1111/tra.12866
Linfang Wang, Honglei Wang, Shuanglong Yi, Shiping Zhang, Margaret S Ho
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引用次数: 2

摘要

富亮氨酸重复激酶2 (LRRK2)突变是家族性和散发性帕金森病的最常见原因。大量证据表明,LRRK2在神经元内溶酶体运输中发挥作用,而LRRK2在胶质细胞中的功能,虽然高表达,但仍不清楚。在这里,我们提出证据表明LRRK2/dLRRK介导溶酶体途径,有助于胶质细胞死亡和多巴胺能(DA)神经元的存活。LRRK2/dLRRK在永生化小胶质细胞或果蝇中的敲低导致溶酶体数量增加和肿胀。这些溶酶体流动性较差,被错误酸化,表现出膜通透性缺陷和溶酶体水解酶组织蛋白酶b活性降低。此外,LRRK2/dLRRK耗损导致胶质细胞凋亡、DA神经退行性变和运动障碍,并以年龄依赖的方式发生。综上所述,这些发现证明了LRRK2/dLRRK在调节胶质溶酶体途径中的功能作用;与神经胶质细胞凋亡相关的溶酶体生物发生和功能缺陷可能是DA神经退行性变的机制基础,为正常和病理大脑中的LRRK2/dLRRK功能提供了新的见解。
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A LRRK2/dLRRK-mediated lysosomal pathway that contributes to glial cell death and DA neuron survival.

Mutations in leucine-rich repeat kinase 2 (LRRK2) are the most common cause of familial and sporadic Parkinson's disease. A plethora of evidence has indicated a role for LRRK2 in endolysosomal trafficking in neurons, while LRRK2 function in glia, although highly expressed, remains largely unknown. Here, we present evidence that LRRK2/dLRRK mediates a lysosomal pathway that contributes to glial cell death and the survival of dopaminergic (DA) neurons. LRRK2/dLRRK knockdown in the immortalized microglia or flies results in enlarged and swelling lysosomes fewer in number. These lysosomes are less mobile, wrongly acidified, exhibit defective membrane permeability and reduced activity of the lysosome hydrolase cathepsin B. In addition, LRRK2/dLRRK depletion causes glial apoptosis, DA neurodegeneration, and locomotor deficits in an age-dependent manner. Taken together, these findings demonstrate a functional role of LRRK2/dLRRK in regulating the glial lysosomal pathway; deficits in lysosomal biogenesis and function linking to glial apoptosis potentially underlie the mechanism of DA neurodegeneration, providing insights on LRRK2/dLRRK function in normal and pathological brains.

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来源期刊
Traffic
Traffic 生物-细胞生物学
CiteScore
8.10
自引率
2.20%
发文量
50
审稿时长
2 months
期刊介绍: Traffic encourages and facilitates the publication of papers in any field relating to intracellular transport in health and disease. Traffic papers span disciplines such as developmental biology, neuroscience, innate and adaptive immunity, epithelial cell biology, intracellular pathogens and host-pathogen interactions, among others using any eukaryotic model system. Areas of particular interest include protein, nucleic acid and lipid traffic, molecular motors, intracellular pathogens, intracellular proteolysis, nuclear import and export, cytokinesis and the cell cycle, the interface between signaling and trafficking or localization, protein translocation, the cell biology of adaptive an innate immunity, organelle biogenesis, metabolism, cell polarity and organization, and organelle movement. All aspects of the structural, molecular biology, biochemistry, genetics, morphology, intracellular signaling and relationship to hereditary or infectious diseases will be covered. Manuscripts must provide a clear conceptual or mechanistic advance. The editors will reject papers that require major changes, including addition of significant experimental data or other significant revision. Traffic will consider manuscripts of any length, but encourages authors to limit their papers to 16 typeset pages or less.
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