BDNF mRNA转运的功能和机制。

Enrico Tongiorgi, Gabriele Baj
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引用次数: 30

摘要

记忆储存基础的长期变化需要将新合成的蛋白质传递到受影响的突触。虽然大多数这些蛋白质是在细胞体中产生的,但一些可塑性的关键分子可以在体细胞外隔室的突触中以沉默mrna的形式传递,在那里它们被局部翻译以响应特定的刺激。其中一种mRNA编码脑源性神经营养因子(BDNF),这是神经元发育的关键分子,在学习和记忆中起着关键作用,在几种神经精神疾病中表现出异常水平。BDNF mRNA在远端树突中积累,以响应刺激,触发NMDAR和TrkB受体的激活。单个BDNF蛋白由具有不同5' utr的几个剪接变体产生。我们已经证明,这些mRNA变体具有不同的亚细胞定位(体细胞,近端或远端树突状隔室),并且该蛋白质与其起源的转录本共定位。由于这些剪接变异体在各种刺激和抗抑郁药物的反应中也有差异表达,我们认为它们代表了局部调节BDNF蛋白表达的空间和时间密码。
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Functions and mechanisms of BDNF mRNA trafficking.

Long-lasting changes in the basis of memory storage require delivery of newly synthesized proteins to the affected synapses. While most of these proteins are generated in the cell body, several key molecules for plasticity can be delivered in the form of silent mRNAs at synapses in extra-somatic compartments where they are locally translated in response to specific stimuli. One such mRNA encodes brain derived neurotrophic factor (BDNF), a key molecule in neuronal development that plays a critical role in learning and memory, and which displays abnormal levels in several neuropsychiatric disorders. BDNF mRNA accumulates in distal dendrites in response to stimuli that trigger activation of NMDAR and TrkB receptors. A single BDNF protein is produced from several splice variants having different 5'UTRs. We have shown that these mRNA variants have a different subcellular localization (soma, proximal or distal dendritic compartment) and that the protein is co-localized with the transcript from which it originated. As these splice variants are also differentially expressed in response to various stimuli and antidepressants, we propose that they represent a spatial and temporal code to regulate BDNF protein expression locally.

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