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NECAB1 和 NECAB2 是 CB1/CCK-阳性 GABA 能中间神经元中常见的钙结合蛋白。

NECAB1 and NECAB2 are Prevalent Calcium-Binding Proteins of CB1/CCK-Positive GABAergic Interneurons.

机构信息

Momentum Laboratory of Molecular Neurobiology, Institute of Experimental Medicine, Budapest 1083, Hungary.

Roska Tamás Doctoral School of Sciences and Technology, Faculty of Information Technology and Bionics, Pázmány Péter Catholic University, Budapest 1083, Hungary.

出版信息

Cereb Cortex. 2021 Feb 5;31(3):1786-1806. doi: 10.1093/cercor/bhaa326.

Abstract

The molecular repertoire of the "Ca2+-signaling toolkit" supports the specific kinetic requirements of Ca2+-dependent processes in different neuronal types. A well-known example is the unique expression pattern of calcium-binding proteins, such as parvalbumin, calbindin, and calretinin. These cytosolic Ca2+-buffers control presynaptic and somatodendritic processes in a cell-type-specific manner and have been used as neurochemical markers of GABAergic interneuron types for decades. Surprisingly, to date no typifying calcium-binding proteins have been found in CB1 cannabinoid receptor/cholecystokinin (CB1/CCK)-positive interneurons that represent a large population of GABAergic cells in cortical circuits. Because CB1/CCK-positive interneurons display disparate presynaptic and somatodendritic Ca2+-transients compared with other interneurons, we tested the hypothesis that they express alternative calcium-binding proteins. By in silico data mining in mouse single-cell RNA-seq databases, we identified high expression of Necab1 and Necab2 genes encoding N-terminal EF-hand calcium-binding proteins 1 and 2, respectively, in CB1/CCK-positive interneurons. Fluorescent in situ hybridization and immunostaining revealed cell-type-specific distribution of NECAB1 and NECAB2 throughout the isocortex, hippocampal formation, and basolateral amygdala complex. Combination of patch-clamp electrophysiology, confocal, and STORM super-resolution microscopy uncovered subcellular nanoscale differences indicating functional division of labor between the two calcium-binding proteins. These findings highlight NECAB1 and NECAB2 as predominant calcium-binding proteins in CB1/CCK-positive interneurons.

摘要

“Ca2+-信号工具箱”的分子组成支持不同神经元类型中 Ca2+-依赖性过程的特定动力学要求。一个众所周知的例子是钙结合蛋白(如 parvalbumin、calbindin 和 calretinin)的独特表达模式。这些细胞溶质 Ca2+缓冲剂以细胞类型特异性的方式控制突触前和体树突过程,并已被用作 GABA 能中间神经元类型的神经化学标志物数十年。令人惊讶的是,迄今为止,在 CB1 大麻素受体/胆囊收缩素(CB1/CCK)阳性中间神经元中尚未发现典型的钙结合蛋白,而 CB1/CCK 阳性中间神经元代表皮质回路中 GABA 能细胞的大群体。由于 CB1/CCK 阳性中间神经元与其他中间神经元相比显示出不同的突触前和体树突 Ca2+瞬变,我们测试了它们表达替代钙结合蛋白的假设。通过在小鼠单细胞 RNA-seq 数据库中的计算机数据挖掘,我们在 CB1/CCK 阳性中间神经元中鉴定出编码 N 端 EF 手钙结合蛋白 1 和 2 的 Necab1 和 Necab2 基因的高表达。荧光原位杂交和免疫染色显示,NECAB1 和 NECAB2 在整个大脑皮质、海马结构和基底外侧杏仁核复合体中具有细胞类型特异性分布。膜片钳电生理学、共聚焦和 STORM 超分辨率显微镜的组合揭示了亚细胞纳米尺度差异,表明两种钙结合蛋白之间存在功能分工。这些发现强调了 NECAB1 和 NECAB2 是 CB1/CCK 阳性中间神经元中主要的钙结合蛋白。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b245/7869086/c4a3c102b09f/bhaa326f1.jpg

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