基因敲除
生物
感觉系统
信使核糖核酸
神经科学
多形体
细胞生物学
核糖核酸
基因
遗传学
核糖体
作者
Ali Bangash,Cankut Çubuk,Federico Iseppon,Rayan Haroun,Ana Paula Luiz,Manuel Arcangeletti,Samuel J. Gossage,Sonia Santana‐Varela,James J. Cox,Myles Lewis,John N. Wood,Jing Zhao
标识
DOI:10.1101/2024.01.11.575033
摘要
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 (+ Nerve Growth Factor (NGF)) 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 behaviour. Terminal-enriched transcripts encoding synaptic proteins (e.g. Synaptotagmin), non-coding RNAs, transcription factors (e.g. Znf431), proteins associated with trans-synaptic 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.
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