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绘制参与长时程记忆保留的哺乳动物 CPEB3 朊病毒亚结构域的纤丝核心。

Mapping the Fibril Core of the Prion Subdomain of the Mammalian CPEB3 that is Involved in Long Term Memory Retention.

机构信息

School of Chemistry, Indian Institute of Science Education and Research Thiruvananthapuram, Trivandrum 695551, India.

School of Biology, Indian Institute of Science Education and Research Thiruvananthapuram, Trivandrum 695551, India.

出版信息

J Mol Biol. 2021 Jul 23;433(15):167084. doi: 10.1016/j.jmb.2021.167084. Epub 2021 May 31.

Abstract

Long-term memory storage is modulated by the prion nature of CPEB3 forming the molecular basis for the maintenance of synaptic facilitation. Here we report that the first prion sub-domain PRD1 of mouse CPEB3 can autonomously form amyloid fibrils in vitro and punctate-like structures in vivo. A ninety-four amino acid sequence within the PRD1 domain, PRD1-core, displays high propensity towards aggregation and associated amyloid characteristics. PRD1-core is characterized using electron microscopy, X-ray diffraction, and solution-state NMR deuterium exchange experiments. Secondary structure elements deduced from solid-state NMR reveal a β-rich core comprising of forty amino acids at the N-terminus of PRD1-core. The synthesized twenty-three amino acid long peptide containing the longest rigid segment (E124-H145) of the PRD1-core rapidly self-aggregates and forms fibrils, indicating a limited aggregation-prone region that could potentially activate the aggregation of the full-length protein. This study provides the first step in identifying the structural trigger for the CPEB3 aggregation process.

摘要

长期记忆存储受 CPEB3 的朊病毒性质调节,形成维持突触易化的分子基础。在这里,我们报告说,小鼠 CPEB3 的第一个朊病毒亚结构域 PRD1 可以在体外自主形成淀粉样纤维,在体内形成点状结构。PRD1 结构域内的 94 个氨基酸序列,PRD1-核心,表现出高聚集倾向和相关的淀粉样特征。使用电子显微镜、X 射线衍射和溶液状态 NMR 氘交换实验对 PRD1-core 进行了表征。从固态 NMR 推断出的二级结构元素揭示了富含 β 的核心,包含 PRD1-core N 端的四十个氨基酸。合成的含有 PRD1-core 最长刚性片段(E124-H145)的 23 个氨基酸长肽迅速自聚集并形成纤维,表明存在潜在的有限聚集倾向区域,可能激活全长蛋白的聚集。这项研究为鉴定 CPEB3 聚集过程的结构触发因素迈出了第一步。

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