基质蛋白Hasp和Hig在突触间隙内呈分离分布,并在突触发生中发挥不同作用。
The Matrix Proteins Hasp and Hig Exhibit Segregated Distribution within Synaptic Clefts and Play Distinct Roles in Synaptogenesis.
作者信息
Nakayama Minoru, Suzuki Emiko, Tsunoda Shin-ichi, Hama Chihiro
机构信息
Faculty of Life Sciences, Kyoto Sangyo University, Kita-ku, Kyoto 603-8555, Japan.
Structural Biology Center, National Institute of Genetics and Department of Genetics, SOKENDAI, Mishima, Shizuoka 411-8540, Japan, and.
出版信息
J Neurosci. 2016 Jan 13;36(2):590-606. doi: 10.1523/JNEUROSCI.2300-15.2016.
UNLABELLED
The synaptic cleft is the space through which neurotransmitters convey neural information between two synaptic terminals. This space is presumably filled with extracellular matrix molecules involved in synaptic function or differentiation. However, little is known about the identities of the matrix components, and it remains unclear how these molecules organize the matrix in synaptic clefts. In this study, we identified Hasp, a Drosophila secretory protein containing CCP and WAP domains. Molecular genetic analysis revealed that Hasp diffuses extracellularly and is predominantly captured at synaptic clefts of cholinergic synapses. Furthermore, Hasp regulates levels of DLG and the nAChR subunits Dα6 and Dα7 at postsynaptic terminals. Hasp is required for trapping of another matrix protein, Hig, which is also secreted and diffused in the brain, at synaptic clefts of cholinergic synapses; however, Hig is dispensable for localization of Hasp at synaptic clefts. In addition, in the brains of triple mutants for the nAChR subunits Dα5, Dα6, and Dα7, the level of Hig, but not Hasp, was markedly reduced in synaptic regions, indicating that these nAChR subunits are required to anchor Hig to synaptic clefts. High-resolution microscopy revealed that Hasp and Hig exhibit segregated distribution within individual synaptic clefts, reflecting their differing roles in synaptogenesis. These data provide insight into how Hasp and Hig construct the synaptic cleft matrix and regulate the differentiation of cholinergic synapses, and also illuminate a previously unidentified architecture within synaptic clefts.
SIGNIFICANCE STATEMENT
The synapse has been extensively studied because it is essential for neurotransmission. By contrast, the space between the synaptic terminals, the synaptic cleft, is still an undeveloped research area despite its ubiquity in synapses. In fruit fly brains, we obtained evidence that the matrix protein Hasp and the previously identified Hig, both of which are secreted extracellularly, localize predominantly to synaptic clefts of cholinergic synapses, and modulate the levels of nAChR subunits on postsynaptic membranes. However, Hasp and Hig play differential roles in matrix formation and exhibit segregated distribution within synaptic clefts. These results reveal the molecular mechanisms of synaptic matrix construction and illuminate a molecular architecture within synaptic clefts previously unrevealed in any animal species.
未标记
突触间隙是神经递质在两个突触终末之间传递神经信息的空间。这个空间可能充满了参与突触功能或分化的细胞外基质分子。然而,对于这些基质成分的身份了解甚少,并且这些分子如何在突触间隙中组织基质仍不清楚。在本研究中,我们鉴定出了Hasp,一种含有CCP和WAP结构域的果蝇分泌蛋白。分子遗传学分析表明,Hasp在细胞外扩散,并主要在胆碱能突触的突触间隙中捕获。此外,Hasp调节突触后终末处DLG以及烟碱型乙酰胆碱受体(nAChR)亚基Dα6和Dα7的水平。Hasp是另一种基质蛋白Hig在胆碱能突触的突触间隙中捕获所必需的,Hig同样在大脑中分泌和扩散;然而,Hig对于Hasp在突触间隙中的定位是可有可无的。此外,在nAChR亚基Dα5、Dα6和Dα7的三突变体果蝇大脑中,突触区域中Hig的水平显著降低,但Hasp的水平未降低,这表明这些nAChR亚基是将Hig锚定到突触间隙所必需的。高分辨率显微镜显示,Hasp和Hig在单个突触间隙内呈现分离分布,这反映了它们在突触形成中不同的作用。这些数据为Hasp和Hig如何构建突触间隙基质以及调节胆碱能突触的分化提供了见解,同时也揭示了突触间隙内以前未被识别的结构。
意义声明
突触因其对神经传递至关重要而得到广泛研究。相比之下,突触终末之间的空间,即突触间隙,尽管在突触中普遍存在,但仍是一个未充分开发的研究领域。在果蝇大脑中,我们获得的证据表明,基质蛋白Hasp和先前鉴定出的Hig都在细胞外分泌,主要定位于胆碱能突触的突触间隙,并调节突触后膜上nAChR亚基的水平。然而,Hasp和Hig在基质形成中发挥不同作用,并在突触间隙内呈现分离分布。这些结果揭示了突触基质构建的分子机制,并揭示了在任何动物物种中以前都未揭示的突触间隙内的分子结构。
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