| Literature DB >> 29562188 |
Daehun Park1, Unghwi Lee1, Eunji Cho1, Haiyan Zhao2, Jung Ah Kim3, Byoung Ju Lee1, Philip Regan4, Won-Kyung Ho5, Kwangwook Cho4, Sunghoe Chang6.
Abstract
Despite being a highly enriched synaptic vesicle (SV) protein and a candidate gene for autism, the physiological function of SCAMP5 remains mostly enigmatic. Here, using optical imaging and electrophysiological experiments, we demonstrate that SCAMP5 plays a critical role in release site clearance at the active zone. Truncation analysis revealed that the 2/3 loop domain of SCAMP5 directly interacts with adaptor protein 2, and this interaction is critical for its role in release site clearance. Knockdown (KD) of SCAMP5 exhibited pronounced synaptic depression accompanied by a slower recovery of the SV pool. Moreover, it induced a strong frequency-dependent short-term depression of synaptic release, even under the condition of sufficient release-ready SVs. Super-resolution microscopy further proved the defects in SV protein clearance induced by KD. Thus, reduced expression of SCAMP5 may impair the efficiency of SV clearance at the active zone, and this might relate to the synaptic dysfunction observed in autism.Entities:
Keywords: SCAMP5; adaptor protein 2; autism spectrum disorder; endocytosis; presynaptic active zone; release site clearance; secretory carrier membrane protein; short-term depression; super-resolution microscopy
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Year: 2018 PMID: 29562188 DOI: 10.1016/j.celrep.2018.02.088
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423