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在小鼠感觉神经元胞体和末端疼痛转译组中鉴定出的镇痛靶点。

Analgesic targets identified in mouse sensory neuron somata and terminal pain translatomes.

机构信息

Molecular Nociception Group, Wolfson Institute for Biomedical Research, University College London WC1E 6BT, UK.

Centre for Experimental Medicine and Rheumatology, William Harvey Research Institute, Barts and The London School of Medicine and Dentistry, Queen Mary University of London, London EC1M 6BQ, UK.

出版信息

Cell Rep. 2024 Aug 27;43(8):114614. doi: 10.1016/j.celrep.2024.114614. Epub 2024 Aug 19.

Abstract

The relationship between transcription and protein expression is complex. We identified polysome-associated RNA transcripts in the somata and central terminals of mouse sensory neurons in control, painful (plus nerve growth factor), and pain-free conditions (Nav1.7-null mice). The majority (98%) of translated transcripts are shared between male and female mice in both the somata and terminals. Some transcripts are highly enriched in the somata or terminals. Changes in the translatome in painful and pain-free conditions include novel and known regulators of pain pathways. Antisense knockdown of selected somatic and terminal polysome-associated transcripts that correlate with pain states diminished pain behavior. Terminal-enriched transcripts included those encoding synaptic proteins (e.g., synaptotagmin), non-coding RNAs, transcription factors (e.g., Znf431), proteins associated with transsynaptic trafficking (HoxC9), GABA-generating enzymes (Gad1 and Gad2), and neuropeptides (Penk). Thus, central terminal translation may well be a significant regulatory locus for peripheral input from sensory neurons.

摘要

转录和蛋白质表达之间的关系很复杂。我们在正常、疼痛(加神经生长因子)和无痛(Nav1.7 基因敲除小鼠)条件下,鉴定了小鼠感觉神经元胞体和中枢末端与多核糖体相关的 RNA 转录本。在胞体和末端,雄性和雌性小鼠之间有 98%的翻译转录本是共享的。一些转录本在胞体或末端高度富集。在疼痛和无痛条件下,翻译组的变化包括已知和新的疼痛途径调节剂。针对与疼痛状态相关的选定胞体和末端多核糖体相关转录本进行反义敲低,可减轻疼痛行为。末端富集的转录本包括编码突触蛋白(如突触结合蛋白)、非编码 RNA、转录因子(如 Znf431)、与跨突触运输相关的蛋白质(如 HoxC9)、产生 GABA 的酶(如 Gad1 和 Gad2)和神经肽(如 Penk)。因此,中枢末端的翻译可能是感觉神经元外周输入的一个重要调节部位。

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