Dansereau Marc-André, Midavaine Élora, Bégin-Lavallée Valérie, Belkouch Mounir, Beaudet Nicolas, Longpré Jean-Michel, Mélik-Parsadaniantz Stéphane, Sarret Philippe
Département de Pharmacologie & Physiologie, Institut de Pharmacologie de Sherbrooke, Faculté de médecine et des sciences de la santé, Université de Sherbrooke, 3001, 12e Avenue Nord, Sherbrooke, Quebec, J1H 5N4, Canada.
Centre de Recherche Institut de la Vision, Université Pierre et Marie Curie, INSERM, UMR_S968, CNRS, UMR_7210, Paris, France.
J Neuroinflammation. 2021 Mar 23;18(1):79. doi: 10.1186/s12974-021-02125-y.
Pain is reported as the leading cause of disability in the common forms of inflammatory arthritis conditions. Acting as a key player in nociceptive processing, neuroinflammation, and neuron-glia communication, the chemokine CCL2/CCR2 axis holds great promise for controlling chronic painful arthritis. Here, we investigated how the CCL2/CCR2 system in the dorsal root ganglion (DRG) contributes to the peripheral inflammatory pain sensitization.
Repeated intrathecal (i.t.) administration of the CCR2 antagonist, INCB3344 was tested for its ability to reverse the nociceptive-related behaviors in the tonic formalin and complete Freund's adjuvant (CFA) inflammatory models. We further determined by qPCR the expression of CCL2/CCR2, SP and CGRP in DRG neurons from CFA-treated rats. Using DRG explants, acutely dissociated primary sensory neurons and calcium mobilization assay, we also assessed the release of CCL2 and sensitization of nociceptors. Finally, we examined by immunohistochemistry following nerve ligation the axonal transport of CCL2, SP, and CGRP from the sciatic nerve of CFA-treated rats.
We first found that CFA-induced paw edema provoked an increase in CCL2/CCR2 and SP expression in ipsilateral DRGs, which was decreased after INCB3344 treatment. This upregulation in pronociceptive neuromodulators was accompanied by an enhanced nociceptive neuron excitability on days 3 and 10 post-CFA, as revealed by the CCR2-dependent increase in intracellular calcium mobilization following CCL2 stimulation. In DRG explants, we further demonstrated that the release of CCL2 was increased following peripheral inflammation. Finally, the excitation of nociceptors following peripheral inflammation stimulated the anterograde transport of SP at their peripheral nerve terminals. Importantly, blockade of CCR2 reduced sensory neuron excitability by limiting the calcium mobilization and subsequently decreased peripheral transport of SP towards the periphery. Finally, pharmacological inhibition of CCR2 reversed the pronociceptive action of CCL2 in rats receiving formalin injection and significantly reduced the neurogenic inflammation as well as the stimuli-evoked and movement-evoked nociceptive behaviors in CFA-treated rats.
Our results provide significant mechanistic insights into the role of CCL2/CCR2 within the DRG in the development of peripheral inflammation, nociceptor sensitization, and pain hypersensitivity. We further unveil the therapeutic potential of targeting CCR2 for the treatment of painful inflammatory disorders.
疼痛被认为是常见炎症性关节炎导致残疾的主要原因。趋化因子CCL2/CCR2轴在伤害性信号传导、神经炎症和神经元-神经胶质细胞通讯中起关键作用,对控制慢性疼痛性关节炎具有巨大潜力。在此,我们研究了背根神经节(DRG)中的CCL2/CCR2系统如何促成外周炎性疼痛敏化。
反复鞘内注射CCR2拮抗剂INCB3344,测试其在强直性福尔马林和完全弗氏佐剂(CFA)炎症模型中逆转伤害性相关行为的能力。我们通过qPCR进一步测定了CFA处理大鼠DRG神经元中CCL2/CCR2、P物质(SP)和降钙素基因相关肽(CGRP)的表达。利用DRG外植体、急性解离的初级感觉神经元和钙动员试验,我们还评估了CCL2的释放和伤害感受器的敏化。最后,我们通过免疫组织化学检查了神经结扎后CFA处理大鼠坐骨神经中CCL2、SP和CGRP的轴突运输。
我们首先发现,CFA诱导的爪部水肿导致同侧DRG中CCL2/CCR2和SP表达增加,INCB3344处理后表达降低。这种伤害性感受神经调质的上调伴随着CFA处理后第3天和第10天伤害性神经元兴奋性增强,这表现为CCL2刺激后CCR2依赖性细胞内钙动员增加。在DRG外植体中,我们进一步证明外周炎症后CCL2的释放增加。最后,外周炎症后伤害感受器的兴奋刺激了SP在其外周神经末梢的顺行运输。重要的是,阻断CCR2通过限制钙动员降低感觉神经元兴奋性,随后减少SP向周围的外周运输。最后,CCR2的药理学抑制逆转了接受福尔马林注射大鼠中CCL2的促伤害作用,并显著降低了CFA处理大鼠的神经源性炎症以及刺激诱发和运动诱发的伤害性相关行为。
我们的结果为DRG内CCL2/CCR2在外周炎症、伤害感受器敏化和疼痛超敏反应发展中的作用提供了重要的机制见解。我们进一步揭示了靶向CCR2治疗疼痛性炎症性疾病的治疗潜力。
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