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小鼠早期癫痫发生的多组学研究揭示了磷酸化和去磷酸化导向的生长及突触减弱。

Multiomics of early epileptogenesis in mice reveals phosphorylation and dephosphorylation-directed growth and synaptic weakening.

作者信息

Hurtado Silva Mariella, van Waardenberg Ashley J, Mostafa Aya, Schoch Susanne, Dietrich Dirk, Graham Mark E

机构信息

Synapse Proteomics, Children's Medical Research Institute, The University of Sydney, Westmead, NSW 2145, Australia.

i-Synapse, Cairns, QLD 4870, Australia.

出版信息

iScience. 2024 Mar 19;27(4):109534. doi: 10.1016/j.isci.2024.109534. eCollection 2024 Apr 19.

Abstract

To investigate the phosphorylation-based signaling and protein changes occurring early in epileptogenesis, the hippocampi of mice treated with pilocarpine were examined by quantitative mass spectrometry at 4 and 24 h post-status epilepticus at vast depth. Hundreds of posttranscriptional regulatory proteins were the major early targets of increased phosphorylation. At 24 h, many protein level changes were detected and the phosphoproteome continued to be perturbed. The major targets of decreased phosphorylation at 4 and 24 h were a subset of postsynaptic density scaffold proteins, ion channels, and neurotransmitter receptors. Many proteins targeted by dephosphorylation at 4 h also had decreased protein abundance at 24 h, indicating a phosphatase-mediated weakening of synapses. Increased translation was indicated by protein changes at 24 h. These observations, and many additional indicators within this multiomic resource, suggest that early epileptogenesis is characterized by signaling that stimulates both growth and a homeostatic response that weakens excitability.

摘要

为了研究癫痫发生早期基于磷酸化的信号传导和蛋白质变化,在癫痫持续状态后4小时和24小时,对毛果芸香碱处理的小鼠海马进行了深度定量质谱分析。数百种转录后调节蛋白是磷酸化增加的主要早期靶点。在24小时时,检测到许多蛋白质水平变化,磷酸化蛋白质组持续受到干扰。在4小时和24小时时,磷酸化减少的主要靶点是突触后致密支架蛋白、离子通道和神经递质受体的一个子集。在4小时时被去磷酸化靶向的许多蛋白质在24小时时蛋白质丰度也降低,表明磷酸酶介导的突触减弱。24小时时的蛋白质变化表明翻译增加。这些观察结果以及这个多组学资源中的许多其他指标表明,早期癫痫发生的特征是刺激生长和减弱兴奋性的稳态反应的信号传导。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d67c/11005001/5983e5443a5c/fx1.jpg

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