Martinez Alejandra N, Burmeister Amanda R, Ramesh Geeta, Doyle-Meyers Lara, Marriott Ian, Philipp Mario T
Division of Bacteriology and Parasitology, Tulane National Primate Research Center, 18703 Three Rivers Rd., Covington, LA, 70433, USA.
Department of Biology, University of North Carolina at Charlotte, 9201 University City Blvd., Charlotte, NC, 28223, USA.
J Neuroinflammation. 2017 Feb 15;14(1):37. doi: 10.1186/s12974-017-0813-x.
Substance P (SP) is produced at high levels in the central nervous system (CNS), and its target receptor, neurokinin 1 receptor (NK-1R), is expressed by glia and leukocytes. This tachykinin functions to exacerbate inflammatory responses at peripheral sites. Moreover, SP/NK-1R interactions have recently been associated with severe neuroinflammation and neuronal damage. We have previously demonstrated that NK-1R antagonists can limit neuroinflammatory damage in a mouse model of bacterial meningitis. Furthermore, we have since shown that these agents can attenuate Borrelia burgdorferi-induced neuronal and glial inflammatory mediator production in non-human primate brain explants and isolated neuronal cells.
In the present study, we have assessed the role played by endogenous SP/NK-1R interactions in damaging CNS inflammation in an established rhesus macaque model that faithfully reproduces the key clinical features of Lyme neuroborreliosis, using the specific NK-1R antagonist, aprepitant. We have utilized multiplex ELISA to quantify immune mediator levels in cerebrospinal fluid, and RT-PCR and immunoblot analyses to quantify cytokine and NK-1R expression, respectively, in brain cortex, dorsal root ganglia, and spinal cord tissues. In addition, we have assessed astrocyte number/activation status in brain cortical tissue by immunofluorescence staining and confocal microscopy.
We demonstrate that aprepitant treatment attenuates B. burgdorferi-induced elevations in CCL2, CXCL13, IL-17A, and IL-6 gene expression in dorsal root ganglia, spinal cord, and/or cerebrospinal fluid of rhesus macaques at 2 to 4 weeks following intrathecal infection. In addition, we demonstrate that this selective NK-1R antagonist also prevents increases in total cortical brain NK-1R expression and decreases in the expression of the astrocyte marker, glial fibrillary acidic protein, associated with B. burgdorferi infection.
The ability of a centrally acting NK-1R inhibitor to attenuate B. burgdorferi-associated neuroinflammatory responses and sequelae raises the intriguing possibility that such FDA-approved agents could be repurposed for use as an adjunctive therapy for the treatment of bacterial CNS infections.
P物质(SP)在中枢神经系统(CNS)中大量产生,其靶受体神经激肽1受体(NK-1R)在神经胶质细胞和白细胞中表达。这种速激肽的作用是加剧外周部位的炎症反应。此外,SP/NK-1R相互作用最近与严重的神经炎症和神经元损伤有关。我们之前已经证明,NK-1R拮抗剂可以在细菌性脑膜炎小鼠模型中限制神经炎症损伤。此外,我们后来还表明,这些药物可以减轻伯氏疏螺旋体在非人灵长类动物脑外植体和分离的神经元细胞中诱导的神经元和神经胶质炎症介质的产生。
在本研究中,我们使用特异性NK-1R拮抗剂阿瑞匹坦,评估了内源性SP/NK-1R相互作用在一个成熟的恒河猴模型中对损伤性中枢神经系统炎症所起的作用,该模型能如实地再现莱姆病神经螺旋体病的关键临床特征。我们利用多重酶联免疫吸附测定法(ELISA)来量化脑脊液中的免疫介质水平,并分别利用逆转录聚合酶链反应(RT-PCR)和免疫印迹分析来量化大脑皮质、背根神经节和脊髓组织中细胞因子和NK-1R的表达。此外,我们通过免疫荧光染色和共聚焦显微镜评估了大脑皮质组织中的星形胶质细胞数量/激活状态。
我们证明,在鞘内感染后2至4周,阿瑞匹坦治疗可减轻恒河猴背根神经节、脊髓和/或脑脊液中伯氏疏螺旋体诱导的CCL2、CXCL13、IL-17A和IL-6基因表达的升高。此外,我们证明这种选择性NK-1R拮抗剂还能防止大脑皮质中总NK-1R表达的增加以及与伯氏疏螺旋体感染相关的星形胶质细胞标志物胶质纤维酸性蛋白表达的降低。
一种中枢作用的NK-1R抑制剂减轻伯氏疏螺旋体相关神经炎症反应和后遗症的能力,引发了一个有趣的可能性,即这类经美国食品药品监督管理局(FDA)批准的药物可以重新用于作为细菌性中枢神经系统感染治疗的辅助疗法。
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