活动诱导的钙离子内流与突触自噬之间受内收蛋白 A 依赖性偶联作用被帕金森病风险突变所破坏。
EndophilinA-dependent coupling between activity-induced calcium influx and synaptic autophagy is disrupted by a Parkinson-risk mutation.
机构信息
VIB-KU Leuven Center for Brain & Disease Research, Leuven 3000, Belgium; KU Leuven, Department of Neurosciences, Leuven Brain Institute, Mission Lucidity, Leuven 3000, Belgium; Clem Jones Centre for Ageing Dementia Research, Queensland Brain Institute, The University of Queensland, St Lucia Campus, Brisbane, QLD 4072, Australia.
VIB-KU Leuven Center for Brain & Disease Research, Leuven 3000, Belgium; KU Leuven, Department of Neurosciences, Leuven Brain Institute, Mission Lucidity, Leuven 3000, Belgium.
出版信息
Neuron. 2023 May 3;111(9):1402-1422.e13. doi: 10.1016/j.neuron.2023.02.001. Epub 2023 Feb 23.
Neuronal activity causes use-dependent decline in protein function. However, it is unclear how this is coupled to local quality control mechanisms. We show in Drosophila that the endocytic protein Endophilin-A (EndoA) connects activity-induced calcium influx to synaptic autophagy and neuronal survival in a Parkinson disease-relevant fashion. Mutations in the disordered loop, including a Parkinson disease-risk mutation, render EndoA insensitive to neuronal stimulation and affect protein dynamics: when EndoA is more flexible, its mobility in membrane nanodomains increases, making it available for autophagosome formation. Conversely, when EndoA is more rigid, its mobility reduces, blocking stimulation-induced autophagy. Balanced stimulation-induced autophagy is required for dopagminergic neuron survival, and a variant in the human ENDOA1 disordered loop conferring risk to Parkinson disease also blocks nanodomain protein mobility and autophagy both in vivo and in human-induced dopaminergic neurons. Thus, we reveal a mechanism that neurons use to connect neuronal activity to local autophagy and that is critical for neuronal survival.
神经元活动导致蛋白功能的使用依赖性下降。然而,目前尚不清楚这是如何与局部质量控制机制相联系的。我们在果蝇中表明,内吞蛋白 Endophilin-A(EndoA)以帕金森病相关的方式将活性诱导的钙内流与突触自噬和神经元存活联系起来。包括帕金森病风险突变在内的无序环中的突变使 EndoA 对神经元刺激不敏感,并影响蛋白动力学:当 EndoA 更灵活时,其在膜纳米域中的迁移性增加,使其可用于自噬体形成。相反,当 EndoA 更僵硬时,其迁移性降低,从而阻止刺激诱导的自噬。平衡的刺激诱导自噬对于多巴胺能神经元的存活是必需的,而人类 ENDOA1 无序环中的一个变体赋予帕金森病风险,也会阻止体内和人类诱导的多巴胺能神经元中的纳米域蛋白迁移和自噬。因此,我们揭示了一种神经元用来将神经元活动与局部自噬联系起来的机制,这对于神经元存活至关重要。
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