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Ubiquitin-dependent protein degradation is necessary for long-term plasticity and memory

机译:泛素依赖性蛋白质降解对于长期的可塑性和记忆是必要的

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摘要

Synaptic plasticity is considered as a basis of learning and memory and, in its turn, is associated with the reconstruction of molecular complexes in the preand postsynaptic parts. One of the means of this reconstruction is ubiquitin-dependent degradation of proteins in proteasomes, which leads to local elimination of preliminarily defined proteins-targets strictly within a certain time period in order to subsequently modify molecular complexes, such as postsynaptic density, the presynaptic apparatus of neuromediator release, and the receptor apparatus of preand postsynaptic membranes. Here, we review the bases of the organization of ubiquitin-dependent protein degradation of proteins in proteasomes and its role in synaptic plasticity and consolidation, reconsolidation, and the extinction of memory. In addition, one section is focused on the analysis of novel data on the mechanisms of the regulation of ubiquitin-dependent protein degradation, because knowledge on the mechanisms of regulation helps one to better understand how the process of protein degradation interacts with other intracellular processes in the cell.
机译:突触可塑性被认为是学习和记忆的基础,而其又与突触前和突触后部分的分子复合物的重建有关。这种重建的方法之一是蛋白酶体中蛋白质的泛素依赖性降解,这导致严格在特定时间段内局部消除初步定义的蛋白质靶标,以便随后修饰分子复合物,例如突触后密度,突触前装置。神经介质的释放,以及突触前和突触后膜的受体装置在这里,我们审查了蛋白酶体中蛋白质的泛素依赖性蛋白质降解组织的基础,及其在突触可塑性和巩固,再巩固以及记忆消失中的作用。此外,由于对调节机制的了解有助于人们更好地理解蛋白质降解过程如何与其他细胞内过程相互作用,因此,一节专门研究有关泛素依赖性蛋白降解的调控机制的新数据的分析。细胞。

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