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皮质中间神经元突触特征的多维分析揭示了潜在的突触异质性。

Multidimensional analysis of cortical interneuron synaptic features reveals underlying synaptic heterogeneity.

作者信息

Dummer Patrick D, Lee Dylan I, Hossain Sakib, Wang Runsheng, Evard Andre, Newman Gabriel, Ho Claire, Schneider-Mizell Casey M, Menon Vilas, Au Edmund

机构信息

Department of Pathology and Cell Biology, Columbia Irving Medical Center, New York NY, 10032.

Department of Neurology, Columbia Irving Medical Center, New York NY, 10032.

出版信息

bioRxiv. 2024 Apr 17:2024.03.22.586340. doi: 10.1101/2024.03.22.586340.

Abstract

Cortical interneurons represent a diverse set of neuronal subtypes characterized in part by their striking degree of synaptic specificity. However, little is known about the extent of synaptic diversity because of the lack of unbiased methods to extract synaptic features among interneuron subtypes. Here, we develop an approach to aggregate image features from fluorescent confocal images of interneuron synapses and their post-synaptic targets, in order to characterize the heterogeneity of synapses at fine scale. We started by training a model that recognizes pre- and post-synaptic compartments and then determines the target of each genetically-identified interneuron synapse in vitro and in vivo. Our model extracts hundreds of spatial and intensity features from each analyzed synapse, constructing a multidimensional data set, consisting of millions of synapses, which allowed us to perform an unsupervised analysis on this dataset, uncovering novel synaptic subgroups. The subgroups were spatially distributed in a highly structured manner that revealed the local underlying topology of the postsynaptic environment. Dendrite-targeting subgroups were clustered onto subdomains of the dendrite along the proximal to distal axis. Soma-targeting subgroups were enriched onto different postsynaptic cell types. We also find that the two main subclasses of interneurons, basket cells and somatostatin interneurons, utilize distinct strategies to enact inhibitory coverage. Thus, our analysis of multidimensional synaptic features establishes a conceptual framework for studying interneuron synaptic diversity.

摘要

皮层中间神经元代表了多种神经元亚型,其部分特征在于它们显著的突触特异性程度。然而,由于缺乏无偏倚的方法来提取中间神经元亚型之间的突触特征,关于突触多样性的程度知之甚少。在这里,我们开发了一种方法,从中间神经元突触及其突触后靶点的荧光共聚焦图像中聚合图像特征,以便在精细尺度上表征突触的异质性。我们首先训练一个模型,该模型识别突触前和突触后隔室,然后在体外和体内确定每个基因鉴定的中间神经元突触的靶点。我们的模型从每个分析的突触中提取数百个空间和强度特征,构建一个由数百万个突触组成的多维数据集,这使我们能够对该数据集进行无监督分析,发现新的突触亚群。这些亚群以高度结构化的方式在空间上分布,揭示了突触后环境的局部潜在拓扑结构。靶向树突的亚群沿近端到远端轴聚集在树突的亚域上。靶向胞体的亚群在不同的突触后细胞类型上富集。我们还发现,中间神经元的两个主要亚类,篮状细胞和生长抑素中间神经元,采用不同的策略来实现抑制性覆盖。因此,我们对多维突触特征的分析建立了一个研究中间神经元突触多样性的概念框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7944/11042224/c401ba45f666/nihpp-2024.03.22.586340v2-f0001.jpg

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