2016
DOI: 10.1523/jneurosci.3627-15.2016
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α-Synuclein Mutation Inhibits Endocytosis at Mammalian Central Nerve Terminals

Abstract: ␣-Synuclein (␣-syn) missense and multiplication mutations have been suggested to cause neurodegenerative diseases, including Parkinson's disease (PD) and dementia with Lewy bodies. Before causing the progressive neuronal loss, ␣-syn mutations impair exocytosis, which may contribute to eventual neurodegeneration. To understand how ␣-syn mutations impair exocytosis, we developed a mouse model that selectively expressed PD-related human ␣-syn A53T (h-␣-syn A53T ) mutation at the calyx of Held terminals, where rel… Show more

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Cited by 64 publications
(70 citation statements)
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“…Indeed, using a combination of FM1-43 dye loading and unloading experiments together with electrophysiology, we find that OE of TDP-43 WT or TDP-43 G298S in motor neurons leads to defects in SV endocytosis but not exocytosis. Although loss of endogenous fly TDP-43 (TBPH) has been shown to cause reduced expression of the synaptic proteins Syntaxin (Romano et al, 2014) and Cacophony (Chang et al, 2014) at the NMJ, and defects in SVC have been previously described in Parkinson’s disease (Xu et al, 2016), here we provide mechanistic insights into reduced SV endocytosis at the NMJ, in the context of TDP-43 toxicity.…”
Section: Discussionmentioning
confidence: 89%
“…Indeed, using a combination of FM1-43 dye loading and unloading experiments together with electrophysiology, we find that OE of TDP-43 WT or TDP-43 G298S in motor neurons leads to defects in SV endocytosis but not exocytosis. Although loss of endogenous fly TDP-43 (TBPH) has been shown to cause reduced expression of the synaptic proteins Syntaxin (Romano et al, 2014) and Cacophony (Chang et al, 2014) at the NMJ, and defects in SVC have been previously described in Parkinson’s disease (Xu et al, 2016), here we provide mechanistic insights into reduced SV endocytosis at the NMJ, in the context of TDP-43 toxicity.…”
Section: Discussionmentioning
confidence: 89%
“…When fast mechanisms fail, CME will probably still be capable of maintaining presynaptic homeostasis to a certain level, and this is what one might see as a slowing down of endocytosis/membrane retrieval [48,49], or bulk endocytosis may take over, as seen in lamprey synapses upon intense stimulation [50]. Although these studies clearly show a disruption of endocytosis, they do not point to any specific 'pathway' that a-synuclein is potentially involved in.…”
Section: Discussionmentioning
confidence: 93%
“…However, membrane retrieval was delayed in A53T a-synuclein-expressing calyces. Furthermore, acute short-term whole-cell dialysis of A53T as well as wild-type a-synuclein delayed membrane retrieval, indicating a direct interaction with, and influence on, membrane properties by a-synuclein [49].…”
Section: A-synuclein In Synaptic Vesicle Endocytosis [ 4 4 9 _ T D $ mentioning
confidence: 89%
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