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伤害感受器翻译组的持续变化在小鼠模型中调控痛觉过敏致敏。

Persistent changes in nociceptor translatomes govern hyperalgesic priming in mouse models.

作者信息

Sankaranarayanan Ishwarya, Kume Moeno, Mohammed Ayaan, Mwirigi Juliet M, Inturi Nikhil Nageswar, Munro Gordon, Petersen Kenneth A, Tavares-Ferreira Diana, Price Theodore J

机构信息

Pain Neurobiology Research Group, Department of Neuroscience, Center for Advanced Pain Studies, School of Behavioral and Brain Sciences, University of Texas at Dallas, Richardson, Texas.

Hoba Therapeutics ApS, Copenhagen, Denmark.

出版信息

bioRxiv. 2024 Aug 8:2024.08.07.606891. doi: 10.1101/2024.08.07.606891.

Abstract

Hyperalgesic priming is a model system that has been widely used to understand plasticity in painful stimulus-detecting sensory neurons, called nociceptors. A key feature of this model system is that following priming, stimuli that do not normally cause hyperalgesia now readily provoke this state. We hypothesized that hyperalgesic priming occurs due to reorganization of translation of mRNA in nociceptors. To test this hypothesis, we used paclitaxel treatment as the priming stimulus and translating ribosome affinity purification (TRAP) to measure persistent changes in mRNA translation in Nav1.8+ nociceptors. TRAP sequencing revealed 161 genes with persistently altered mRNA translation in the primed state. We identified as upregulated and as downregulated. We confirmed a functional role for these genes, wherein a GPR88 agonist causes pain only in primed mice and established hyperalgesic priming is reversed by Meteorin. Our work demonstrates that altered nociceptor translatomes are causative in producing hyperalgesic priming.

摘要

痛觉过敏启动是一种模型系统,已被广泛用于理解在称为伤害感受器的疼痛刺激检测感觉神经元中的可塑性。该模型系统的一个关键特征是,在启动之后,通常不会引起痛觉过敏的刺激现在很容易引发这种状态。我们假设痛觉过敏启动是由于伤害感受器中mRNA翻译的重组所致。为了验证这一假设,我们使用紫杉醇治疗作为启动刺激,并采用翻译核糖体亲和纯化(TRAP)技术来测量Nav1.8+伤害感受器中mRNA翻译的持续变化。TRAP测序揭示了在启动状态下有161个基因的mRNA翻译持续改变。我们确定了上调和下调的基因。我们证实了这些基因的功能作用,其中GPR88激动剂仅在启动的小鼠中引起疼痛,而已建立的痛觉过敏启动可被Meteorin逆转。我们的工作表明,伤害感受器翻译组的改变是产生痛觉过敏启动的原因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d1c3/11326310/1ef41841d800/nihpp-2024.08.07.606891v1-f0001.jpg

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