Nex⁺ 上脊髓神经元中的 TNFR1/p38αMAPK 信号转导调节雌激素依赖性慢性神经病理性疼痛。
TNFR1/p38αMAPK signaling in Nex + supraspinal neurons regulates estrogen-dependent chronic neuropathic pain.
机构信息
Department of Biology, Drexel University, Papadakis Integrated Science Building, Philadelphia, PA 19104, USA.
Department of Anatomy and Cell Biology, The George Washington University School of Medicine and Health Sciences, Ross Hall, 2300 I (Eye) St NW, Rm.530A, Washington, D.C 20052, USA.
出版信息
Brain Behav Immun. 2024 Jul;119:261-271. doi: 10.1016/j.bbi.2024.03.050. Epub 2024 Apr 1.
Upregulation of soluble tumor necrosis factor (sTNF) cytokine signaling through TNF receptor 1 (TNFR1) and subsequent neuronal hyperexcitability are observed in both animal models and human chronic neuropathic pain (CNP). Previously, we have shown that estrogen modulates sTNF/TNFR1 signaling in CNP, which may contribute to female prevalence of CNP. The estrogen-dependent role of TNFR1-mediated supraspinal neuronal circuitry in CNP remains unknown. In this study, we interrogated the intersect between supraspinal TNFR1 mediated neuronal signaling and sex specificity by selectively removing TNFR1 in Nex + neurons in adult mice (NexCre::TNFR1). We determined that mechanical hypersensitivity induced by chronic constriction injury (CCI) decreases over time in males, but not in females. Subsequently, we investigated two downstream pathways, p38MAPK and NF-κB, important in TNFR1 signaling and injury response. We detected p38MAPK and NF-κB activation in male cortical tissue; however, p38MAPK phosphorylation was reduced in NexCre::TNFR1 males. We observed a similar recovery from acute pain in male mice following CCI when p38αMAPK was knocked out of supraspinal Nex + neurons (NexCre::p38αMAPK), while chronic pain developed in female mice. To explore the intersection between estrogen and inflammation in CNP we used a combination therapy of an estrogen receptor β (ER β) inhibitor with a sTNF/TNFR1 or general p38MAPK inhibitor. We determined both combination therapies lends therapeutic relief to females following CCI comparable to the response evaluated in male mice. These data suggest that TNFR1/p38αMAPK signaling in Nex + neurons in CNP is male-specific and lack of therapeutic efficacy following sTNF inhibition in females is due to ER β interference. These studies highlight sex-specific differences in pathways important to pain chronification and elucidate potential therapeutic strategies that would be effective in both sexes.
可溶性肿瘤坏死因子 (sTNF) 细胞因子信号通过 TNF 受体 1 (TNFR1) 的上调以及随后的神经元过度兴奋在动物模型和人类慢性神经性疼痛 (CNP) 中均有观察到。先前,我们已经表明,雌激素调节 CNP 中的 sTNF/TNFR1 信号,这可能有助于 CNP 中女性的患病率。TNFR1 介导的中枢神经系统神经元回路在 CNP 中的雌激素依赖性作用尚不清楚。在这项研究中,我们通过选择性去除成年小鼠中的 Nex+神经元中的 TNFR1(NexCre::TNFR1)来探究中枢神经系统 TNFR1 介导的神经元信号与性别特异性之间的交叉。我们发现,慢性缩窄性损伤 (CCI) 引起的机械性过敏在雄性中随时间推移而减轻,但在雌性中则不然。随后,我们研究了两个下游途径,p38MAPK 和 NF-κB,它们在 TNFR1 信号和损伤反应中很重要。我们检测到雄性皮质组织中的 p38MAPK 和 NF-κB 激活;然而,NexCre::TNFR1 雄性中的 p38MAPK 磷酸化减少。当将 p38αMAPK 从中枢神经系统中的 Nex+神经元(NexCre::p38αMAPK)敲除时,我们观察到雄性小鼠在 CCI 后急性疼痛的恢复相似,而雌性小鼠则发展为慢性疼痛。为了探索 CNP 中雌激素和炎症之间的交叉,我们使用雌激素受体 β (ER β) 抑制剂与 sTNF/TNFR1 或一般 p38MAPK 抑制剂的联合治疗。我们确定两种联合疗法均可为 CCI 后的雌性提供治疗缓解,与在雄性小鼠中评估的反应相当。这些数据表明,CNP 中 Nex+神经元中的 TNFR1/p38αMAPK 信号是雄性特异性的,并且雌性中 sTNF 抑制后缺乏治疗效果是由于 ER β 干扰。这些研究强调了对疼痛慢性化很重要的途径中的性别特异性差异,并阐明了对两性都有效的潜在治疗策略。
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