Induction of long-term hyperexcitability by memory-related cAMP signaling in isolated nociceptor cell bodies

Q2 Medicine
Alexis Bavencoffe , Michael Y. Zhu , Sanjay V. Neerukonda , Kayla N. Johnson , Carmen W. Dessauer , Edgar T. Walters
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引用次数: 0

Abstract

Persistent hyperactivity of nociceptors is known to contribute significantly to long-lasting sensitization and ongoing pain in many clinical conditions. It is often assumed that nociceptor hyperactivity is mainly driven by continuing stimulation from inflammatory mediators. We have tested an additional possibility: that persistent increases in excitability promoting hyperactivity can be induced by a prototypical cellular signaling pathway long known to induce late-phase long-term potentiation (LTP) of synapses in brain regions involved in memory formation. This cAMP-PKA-CREB-gene transcription-protein synthesis pathway was tested using whole-cell current clamp methods on small dissociated sensory neurons (primarily nociceptors) from dorsal root ganglia (DRGs) excised from previously uninjured (“naïve”) male rats. Six-hour treatment with the specific Gαs-coupled 5-HT4 receptor agonist, prucalopride, or with the adenylyl cyclase activator forskolin induced long-term hyperexcitability (LTH) in DRG neurons that manifested 12–24 h later as action potential (AP) discharge (ongoing activity, OA) during artificial depolarization to −45 mV, a membrane potential that is normally subthreshold for AP generation. Prucalopride treatment also induced significant long-lasting depolarization of resting membrane potential (from −69 to −66 mV), enhanced depolarizing spontaneous fluctuations (DSFs) of membrane potential, and produced trends for reduced AP threshold and rheobase. LTH was prevented by co-treatment of prucalopride with inhibitors of PKA, CREB, gene transcription, or protein synthesis. As in the induction of synaptic memory, many other cellular signals are likely to be involved. However, the discovery that this prototypical memory induction pathway can induce nociceptor LTH, along with reports that cAMP signaling and CREB activity in DRGs can induce hyperalgesic priming, suggest that early, temporary, cAMP-induced transcriptional and translational mechanisms can induce nociceptor LTH that might last for long periods. The present results also raise the question of whether reactivation of primed signaling mechanisms by re-exposure to inflammatory mediators linked to cAMP synthesis during subsequent challenges to bodily integrity can “reconsolidate” nociceptor memory, extending the duration of persistent hyperexcitability.
记忆相关的 cAMP 信号在离体痛觉感受器细胞体中诱导长期过度兴奋性
众所周知,在许多临床病症中,痛觉感受器的持续亢进在很大程度上导致了长期敏感化和持续疼痛。人们通常认为,痛觉感受器亢进主要是由炎症介质的持续刺激驱动的。我们还测试了另一种可能性:兴奋性的持续上升会促进过度活跃,而这种兴奋性的持续上升是由一种典型的细胞信号通路诱导的,这种信号通路长期以来一直被认为能诱导参与记忆形成的脑区突触的晚期长期电位(LTP)。研究人员使用全细胞电流钳方法,对从先前未受伤("天真")的雄性大鼠背根神经节(DRGs)中切除的小型离体感觉神经元(主要是痛觉感受器)进行了 cAMP-PKA-CREB 基因转录-蛋白合成途径测试。用特异性 Gαs 偶联 5-HT4 受体激动剂普鲁卡必利或腺苷酸环化酶激活剂福斯可林处理 DRG 神经元六小时后,可诱导其长期兴奋性过高(LTH),12-24 小时后表现为在人工去极化至 -45 mV 时出现动作电位(AP)放电(持续活动,OA),而这个膜电位通常是产生 AP 的阈下电位。普卡必利治疗也会诱导静息膜电位的显著持久去极化(从-69 到-66 mV),增强膜电位的去极化自发波动(DSFs),并产生 AP 阈值和流变基础降低的趋势。普鲁卡必利与 PKA、CREB、基因转录或蛋白质合成抑制剂联合处理可防止 LTH。与突触记忆的诱导一样,许多其他细胞信号也可能参与其中。然而,这一典型记忆诱导途径可诱导痛觉感受器 LTH 的发现,以及 DRGs 中 cAMP 信号传导和 CREB 活性可诱导超痛引物的报道表明,早期、暂时、cAMP 诱导的转录和翻译机制可诱导痛觉感受器 LTH,并可能持续很长时间。本研究结果还提出了一个问题,即在随后身体完整性受到挑战时,再次暴露于与 cAMP 合成有关的炎症介质是否会重新激活已启动的信号机制,从而 "重新巩固 "痛觉感受器记忆,延长持续过度兴奋的持续时间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Neurobiology of Pain
Neurobiology of Pain Medicine-Anesthesiology and Pain Medicine
CiteScore
4.40
自引率
0.00%
发文量
29
审稿时长
54 days
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