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针对 RIBEYE A-和 B-结构域的直接金标记单克隆抗体的免疫胶体金电镜后分析表明了突触核糖核蛋白体装配的一个改良模型。

Analytical Post-Embedding Immunogold-Electron Microscopy with Direct Gold-Labelled Monoclonal Primary Antibodies against RIBEYE A- and B-Domain Suggests a Refined Model of Synaptic Ribbon Assembly.

机构信息

Institute of Anatomy, Department of Neuroanatomy, Medical School, Saarland University, 66421 Homburg, Germany.

Mathematical Institute, University of Bonn, 53115 Bonn, Germany.

出版信息

Int J Mol Sci. 2024 Jul 6;25(13):7443. doi: 10.3390/ijms25137443.

Abstract

Synaptic ribbons are the eponymous specializations of continuously active ribbon synapses. They are primarily composed of the RIBEYE protein that consists of a unique amino-terminal A-domain and carboxy-terminal B-domain that is largely identical to the ubiquitously expressed transcriptional regulator protein CtBP2. Both RIBEYE A-domain and RIBEYE B-domain are essential for the assembly of the synaptic ribbon, as shown by previous analyses of RIBEYE knockout and knockin mice and related investigations. How exactly the synaptic ribbon is assembled from RIBEYE subunits is not yet clear. To achieve further insights into the architecture of the synaptic ribbon, we performed analytical post-embedding immunogold-electron microscopy with direct gold-labelled primary antibodies against RIBEYE A-domain and RIBEYE B-domain for improved ultrastructural resolution. With direct gold-labelled monoclonal antibodies against RIBEYE A-domain and RIBEYE B-domain, we found that both domains show a very similar localization within the synaptic ribbon of mouse photoreceptor synapses, with no obvious differential gradient between the centre and surface of the synaptic ribbon. These data favour a model of the architecture of the synaptic ribbon in which the RIBEYE A-domain and RIBEYE B-domain are located similar distances from the midline of the synaptic ribbon.

摘要

突触棘是连续活跃的棘突触的命名特征。它们主要由 RIBEYE 蛋白组成,该蛋白由独特的氨基末端 A 结构域和羧基末端 B 结构域组成,B 结构域与广泛表达的转录调节蛋白 CtBP2 基本相同。以前对 RIBEYE 敲除和敲入小鼠的分析以及相关研究表明,RIBEYE A 结构域和 RIBEYE B 结构域对于突触棘的组装都是必不可少的。然而,突触棘究竟是如何由 RIBEYE 亚基组装而成的,目前尚不清楚。为了进一步深入了解突触棘的结构,我们采用了直接用金标记的针对 RIBEYE A 结构域和 RIBEYE B 结构域的单克隆抗体进行分析后包埋免疫金电子显微镜技术,以提高超微结构分辨率。使用直接用金标记的针对 RIBEYE A 结构域和 RIBEYE B 结构域的单克隆抗体,我们发现这两个结构域在小鼠光感受器突触的突触棘内具有非常相似的定位,在突触棘的中心和表面之间没有明显的差异梯度。这些数据支持这样一种模型,即 RIBEYE A 结构域和 RIBEYE B 结构域与突触棘的中线的距离相似。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a2d/11242772/70ad6fdf9870/ijms-25-07443-g001.jpg

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