Department of Anaesthesiology and Pain Medicine, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei Province, China.
Department of Anaesthesiology, The First Affiliated Hospital of Sun Yat-Sen University, Guangzhou, Guangdong Province, China.
J Pain. 2019 May;20(5):577-591. doi: 10.1016/j.jpain.2018.11.006. Epub 2018 Nov 27.
Central poststroke pain (CPSP) is a neuropathic pain syndrome arising after a lesion of the central nervous system owing to cerebrovascular insult. Impaired daily activities and reduced quality of life in people suffering from CPSP justify the need for improved treatment. The detailed mechanism of CPSP is not well understood, but central disinhibition has been suggested. Recent reports indicated that epoxyeicosatrienoic acids (EETs), the cytochrome P450 metabolites of arachidonic acid, promoted neuronal survival after stroke, displayed antinociception in peripheral inflammatory pain, and reduced neuronal excitability in seizure model. Here, we tested the hypothesis that 14,15-EET may attenuate CPSP by suppressing thalamic disinhibition through neurosteroids-δ-subunit-containing gamma-aminobutyric acid A receptors (δGABAR) signaling. In this study, we used a rat model of thalamic hemorrhagic stroke to induce CPSP. Pain behavioral tests revealed that CPSP rats exhibited mechanical allodynia, starting at day 7 postlesion and lasting at least 4 weeks. Analysis of the perithalamic lesion tissue from the brain of CPSP rats demonstrated a decrease of 14,15-EET content, steroidogenic acute regulatory protein expression, and allopregnanolone (AP) production. This was accompanied by reduced δGABAR expression in the medial thalamus at 4 weeks postlesion. Intrathalamic injection of exogenous 14,15-EET into the ventral posterior lateral nucleus attenuated mechanical allodynia, induced a marked increase in the abundance of the steroidogenic acute regulatory protein and AP along the lesion site and a concomitant increase in δGABAR expression in the medial thalamus under CPSP condition. However, this antinociceptive effect could be eliminated by the 5α-reductase inhibitor finasteride or dutasteride or GABAR antagonist bicuculline. Moreover, compared with the current first-line drug gabapentin for central neuropathic pain, an early treatment of EET showed greater efficacy in the secondary prevention of CPSP. Taken together, this study provided a proof of concept that EETs may have anti-CPSP effect by reserving normal thalamic inhibition through AP-δGABAR signaling. PERSPECTIVE: Agents targeting EETs may serve as potential therapeutic options for stroke, the use of which at the initial period could not only block further nerve damage but also prevent the occurrence of CPSP.
中枢性卒中后疼痛(CPSP)是一种由于脑血管损伤导致中枢神经系统损伤而引起的神经性疼痛综合征。患有 CPSP 的人日常活动受损,生活质量下降,这证明需要改进治疗方法。CPSP 的详细机制尚不清楚,但已经提出中枢抑制作用。最近的报告表明,花生四烯酸的细胞色素 P450 代谢物环氧二十碳三烯酸(EETs)促进了中风后的神经元存活,在外周炎症性疼痛中表现出镇痛作用,并减少了癫痫模型中的神经元兴奋性。在这里,我们通过神经甾体-δ-亚单位包含的γ-氨基丁酸 A 受体(δGABAR)信号来测试 14,15-EET 通过抑制丘脑去抑制作用来减轻 CPSP 的假设。在这项研究中,我们使用了丘脑出血性中风的大鼠模型来诱导 CPSP。疼痛行为测试表明,CPSP 大鼠表现出机械性痛觉过敏,从损伤后第 7 天开始,至少持续 4 周。对 CPSP 大鼠脑peri 丘脑损伤组织的分析表明,14,15-EET 含量、类固醇急性调节蛋白表达和异孕烯醇酮(AP)产生减少。这伴随着损伤后 4 周时内侧丘脑 δGABAR 表达减少。向腹后外侧核内注射外源性 14,15-EET 可减轻机械性痛觉过敏,在 CPSP 条件下,沿损伤部位明显增加类固醇急性调节蛋白和 AP 的丰度,并使内侧丘脑 δGABAR 表达增加。然而,这种镇痛作用可以通过 5α-还原酶抑制剂非那雄胺或度他雄胺或 GABAR 拮抗剂印防己毒素消除。此外,与用于治疗中枢性神经病理性疼痛的一线药物加巴喷丁相比,EET 的早期治疗在预防 CPSP 的二次发作方面显示出更大的疗效。综上所述,这项研究提供了一个概念证明,即 EETs 通过 AP-δGABAR 信号保留正常的丘脑抑制作用,可能具有抗 CPSP 作用。观点:靶向 EETs 的药物可能成为中风的潜在治疗选择,在初始阶段使用不仅可以阻止进一步的神经损伤,还可以预防 CPSP 的发生。
