| Literature DB >> 33753902 |
Jong-Heon Kim1, Hyun-Gug Jung2,3, Ajung Kim2, Hyun Soo Shim4, Seung Jae Hyeon4, Young-Sun Lee3, Jin Han5, Jong Hoon Jung6, Jaekwang Lee6, Hoon Ryu4,7,8, Jae-Yong Park3, Eun Mi Hwang9, Kyoungho Suk10,11.
Abstract
Hevin, also known as SPARC-like protein 1 (SPARCL1 or SC1), is a synaptogenic protein secreted by astrocytes and modulates the formation of glutamatergic synapses in the developing brain by interacting with synaptic adhesion proteins, such as neurexin and neuroligin. Here, we identified the neuron-specific vesicular protein calcyon as a novel interaction partner of hevin and demonstrated that this interaction played a pivotal role in synaptic reorganization after an injury in the mature brain. Astrocytic hevin was upregulated post-injury in a photothrombotic stroke model. Hevin was fragmented by MMP3 induced during the acute stage of brain injury, and this process was associated with severe gliosis. At the late stage, the functional hevin level was restored as MMP3 expression decreased. The C-terminus of hevin interacted with the N-terminus of calcyon. By using RNAi and binding competitor peptides in an ischemic brain injury model, we showed that this interaction was crucial in synaptic and functional recoveries in the sensory-motor cortex, based on histological and electrophysiological analyses. Regulated expression of hevin and calcyon and interaction between them were confirmed in a mouse model of traumatic brain injury and patients with chronic traumatic encephalopathy. Our study provides direct evidence for the causal relationship between the hevin-calcyon interaction and synaptic reorganization after brain injury. This neuron-glia interaction can be exploited to modulate synaptic reorganization under various neurological conditions.Entities:
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Year: 2021 PMID: 33753902 PMCID: PMC8408247 DOI: 10.1038/s41418-021-00772-5
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 12.067