在成年大鼠运动神经元死亡过程中,脊髓肿瘤坏死因子-α受体1对膈神经长期易化(pLTF)的需求存在差异。
Spinal TNF-α receptor 1 is differentially required for phrenic long-term facilitation (pLTF) over the course of motor neuron death in adult rats.
作者信息
Lewis Ryan D, Keilholz Amy N, Smith Catherine L, Burd Ethan A, Nichols Nicole L
机构信息
Department of Biological Chemistry, Grinnell College, Grinnell, IA, United States.
Department of Veterinary Pathobiology, College of Veterinary Medicine, University of Missouri, Columbia, MO, United States.
出版信息
Front Physiol. 2024 Dec 5;15:1488951. doi: 10.3389/fphys.2024.1488951. eCollection 2024.
INTRODUCTION
Intrapleural injections of cholera toxin B conjugated to saporin (CTB-SAP) result in selective respiratory (, phrenic) motor neuron death and mimics aspects of motor neuron disease [(, amyotrophic lateral sclerosis (ALS) and spinal muscular atrophy (SMA)], such as breathing deficits. This rodent model allows us to study the impact motor neuron death has on the output of surviving phrenic motor neurons as well as the compensatory mechanisms that are recruited. Microglial density in the phrenic motor nucleus as well as cervical gene expression of markers associated with inflammation (., tumor necrosis factor α; TNF-α) are increased following CTB-SAP-induced phrenic motor neuron death, and ketoprofen (nonsteroidal anti-inflammatory drug) delivery attenuated phrenic long-term facilitation (pLTF) in 7 day (d) CTB-SAP rats but enhanced pLTF in 28d CTB-SAP rats.
METHODS
Here, we worked to determine the impact of TNF-α in the phrenic motor nucleus by: 1) quantifying TNFR1 (a high affinity transmembrane receptor for TNF-α) expression; 2) investigating astrocytes (glial cells known to release TNF-α) by performing a morphological analysis in the phrenic motor nucleus; and 3) determining whether acute TNFR1 inhibition differentially affects phrenic plasticity over the course of CTB-SAP-induced motor neuron loss by delivering an inhibitor for TNF-α receptor 1 (sTNFR1i) in 7d and 28d male CTB-SAP and control rats.
RESULTS
Results revealed that TNFR1 expression was increased on phrenic motor neurons of 28d CTB-SAP rats ( < 0.05), and that astrocytes were increased and exhibited reactive morphology (consistent with an activated phenotype; < 0.05) in the phrenic motor nucleus of CTB-SAP rats. Additionally, we found that pLTF was attenuated in 7d CTB-SAP rats but enhanced in 28d CTB-SAP rats ( < 0.05) following intrathecal sTNFR1i delivery.
CONCLUSION
This work suggests that we could harness TNFR1 as a potential therapeutic agent in CTB-SAP rats and patients with respiratory motor neuron disease by increasing compensatory plasticity in surviving neurons to improve phrenic motor neuron function and breathing as well as quality of life. Future studies will focus on microglial and astrocytic cytokine release, the role they play in the differential mechanisms of pLTF utilized by 7d and 28d CTB-SAP rats, and potential therapies that target them.
引言
向胸膜腔内注射与皂草素结合的霍乱毒素B(CTB-SAP)会导致选择性呼吸(即膈神经)运动神经元死亡,并模拟运动神经元疾病(如肌萎缩侧索硬化症(ALS)和脊髓性肌萎缩症(SMA))的某些方面,例如呼吸功能缺陷。这种啮齿动物模型使我们能够研究运动神经元死亡对存活的膈神经运动神经元输出的影响以及所募集的代偿机制。CTB-SAP诱导膈神经运动神经元死亡后,膈神经运动核中的小胶质细胞密度以及与炎症相关标志物(如肿瘤坏死因子α;TNF-α)的颈部基因表达增加,并且给予酮洛芬(一种非甾体抗炎药)可减弱7天(d)CTB-SAP大鼠的膈神经长期易化(pLTF),但增强28d CTB-SAP大鼠的pLTF。
方法
在此,我们通过以下方式来确定TNF-α在膈神经运动核中的影响:1)量化TNFR1(TNF-α的高亲和力跨膜受体)的表达;2)通过对膈神经运动核进行形态学分析来研究星形胶质细胞(已知可释放TNF-α的神经胶质细胞);3)通过在7d和28d雄性CTB-SAP大鼠及对照大鼠中给予TNF-α受体1抑制剂(sTNFR1i),来确定急性TNFR1抑制在CTB-SAP诱导的运动神经元丢失过程中是否对膈神经可塑性有不同影响。
结果
结果显示,28d CTB-SAP大鼠的膈神经运动神经元上TNFR1表达增加(P<0.05),并且CTB-SAP大鼠的膈神经运动核中星形胶质细胞数量增加并呈现反应性形态(与活化表型一致;P<0.05)。此外,我们发现鞘内注射sTNFR1i后,7d CTB-SAP大鼠的pLTF减弱,但28d CTB-SAP大鼠的pLTF增强(P<0.05)。
结论
这项研究表明,我们可以将TNFR1作为一种潜在的治疗药物应用于CTB-SAP大鼠和呼吸运动神经元疾病患者,通过增加存活神经元的代偿可塑性来改善膈神经运动神经元功能、呼吸以及生活质量。未来的研究将聚焦于小胶质细胞和星形胶质细胞释放的细胞因子、它们在7d和28d CTB-SAP大鼠所利用的pLTF差异机制中所起的作用以及针对它们的潜在治疗方法。
Zotero 插件