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体外培养的海马神经元发育过程中兴奋性突触后位点分子组成的异质性。

Heterogeneity in the molecular composition of excitatory postsynaptic sites during development of hippocampal neurons in culture.

作者信息

Rao A, Kim E, Sheng M, Craig A M

机构信息

Department of Cell and Structural Biology, University of Illinois at Urbana-Champaign, Urbana, Illinois 61801, USA.

出版信息

J Neurosci. 1998 Feb 15;18(4):1217-29. doi: 10.1523/JNEUROSCI.18-04-01217.1998.

DOI:10.1523/JNEUROSCI.18-04-01217.1998
PMID:9454832
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6792722/
Abstract

To determine their roles in the assembly of glutamatergic postsynaptic sites, we studied the distributions of NMDA- and AMPA-type glutamate receptors; the NMDA receptor-interacting proteins alpha-actinin-2, PSD-95, and chapsyn; and the PSD-95-associated protein GKAP during the development of hippocampal neurons in culture. NMDA receptors first formed nonsynaptic proximal dendrite shaft clusters within 2-5 d. AMPA receptors were diffuse at this stage and began to cluster on spines at 9-10 d. NMDA receptor clusters remained partially nonsynaptic and mainly distinct from AMPA receptor clusters until after 3 weeks in culture, when the two began to colocalize at spiny synaptic sites. Thus, the localization of NMDA and AMPA receptors must be regulated by different mechanisms. alpha-Actinin-2 colocalized with the NMDA receptor only at spiny synaptic clusters, but not at shaft nonsynaptic or synaptic clusters, suggesting a modulatory role in the anchoring of NMDA receptor at spines. PSD-95, chapsyn, and GKAP were present at some, but not all, nonsynaptic NMDA receptor clusters during the first 2 weeks, indicating that none is essential for NMDA receptor cluster formation. When NMDA receptor clusters became synaptic, PSD-95 and GKAP were always present, consistent with an essential function in synaptic localization of NMDA receptors. Furthermore, PSD-95 and GKAP clustered opposite presynaptic terminals several days before either NMDA or AMPA receptors clustered at these presumptive postsynaptic sites. These results suggest that synapse development proceeds by formation of a postsynaptic scaffold containing PSD-95 and GKAP in concert with presynaptic vesicle clustering, followed by regulated attachment of glutamate receptor subtypes to this scaffold.

摘要

为了确定它们在谷氨酸能突触后位点组装中的作用,我们研究了NMDA型和AMPA型谷氨酸受体、与NMDA受体相互作用的蛋白α-辅肌动蛋白-2、PSD-95和Chapsyn以及与PSD-95相关的蛋白GKAP在培养的海马神经元发育过程中的分布。NMDA受体在2-5天内首先在非突触性近端树突干形成簇。在此阶段,AMPA受体呈弥散分布,并在9-10天时开始在棘突上聚集。在培养3周后,NMDA受体簇仍部分为非突触性,且主要与AMPA受体簇不同,此时两者开始在棘突突触位点共定位。因此,NMDA和AMPA受体的定位必定受不同机制调控。α-辅肌动蛋白-2仅在棘突突触簇处与NMDA受体共定位,而在树突干非突触或突触簇处则不然,这表明其在棘突处对NMDA受体的锚定起调节作用。在最初的2周内,PSD-95、Chapsyn和GKAP存在于部分而非全部非突触性NMDA受体簇中,这表明它们对NMDA受体簇的形成均非必需。当NMDA受体簇变为突触性时,PSD-95和GKAP总是存在,这与它们在NMDA受体突触定位中的重要功能一致。此外,在NMDA或AMPA受体在这些假定的突触后位点聚集的数天前,PSD-95和GKAP就在突触前终末对面聚集。这些结果表明,突触发育通过形成一个包含PSD-95和GKAP的突触后支架与突触前囊泡聚集协同进行,随后谷氨酸受体亚型被调控性地附着到该支架上。

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Characterization of guanylate kinase-associated protein, a postsynaptic density protein at excitatory synapses that interacts directly with postsynaptic density-95/synapse-associated protein 90.鸟苷酸激酶相关蛋白的特性,一种兴奋性突触处的突触后致密蛋白,可直接与突触后致密蛋白95/突触相关蛋白90相互作用。
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Disulfide-linked head-to-head multimerization in the mechanism of ion channel clustering by PSD-95.PSD-95介导离子通道聚集机制中的二硫键连接的头对头多聚化。
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Rapsyn is required for MuSK signaling and recruits synaptic components to a MuSK-containing scaffold.Rapsyn是MuSK信号传导所必需的,并将突触成分募集到含有MuSK的支架上。
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