Spinal glia activation in chronic stress-induced visceral hyperalgesia

慢性应激引起的内脏痛觉过敏中的脊髓胶质细胞激活

• 批准号: 7778816
• 负责人: SYLVIE BRADESI
• 金额: $ 21.59万
• 依托单位: BRENTWOOD BIOMEDICAL RESEARCH INSTITUTE
• 依托单位国家: 美国
• 财政年份: 2009
• 资助国家: 美国
• 起止时间: 2009-04-01 至 2014-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7778816
• 关键词: Address; Affect; Agonist; Antisense Oligonucleotides; Behavior assessment; Cardiac; Cells; Chest Pain; Chronic; Chronic stress; Clinical; Coculture Techniques; Data; Development; Disease; Endocrine; Enzyme-Linked Immunosorbent Assay; Equilibrium; Event; Exhibits; Experimental Animal Model; Experimental Designs; Experimental Models; Exposure to; Fibromyalgia; Functional Gastrointestinal Disorders; Glucocorticoids; Glutamate Transporter; Glutamates; Goals; Hyperalgesia; Hypersensitivity; Immune; Immune system; Immunohistochemistry; In Vitro; Inflammation; Interneurons; Interstitial Cystitis; Intestines; Irritable Bowel Syndrome; Link; Maintenance; Mediating; Mediator of activation protein; Modeling; Molecular; Neuraxis; Neurobiology; Neuroglia; Neurons; Nociception; Pain; Pathway interactions; Pattern; Peripheral; Persistent pain; Pharmacological Treatment; Play; Rattus; Reverse Transcriptase Polymerase Chain Reaction; Role; Signal Pathway; Signal Transduction; Site; Spinal; Spinal Cord; Spinal Injuries; Stress; Substance P; Symptoms; Synapses; Syndrome; System; TACR1 gene; Testing; Time; Visceral; Visceral pain; Water; Western Blotting; attenuation; base; chronic pain; colorectal distension; dorsal horn; effective therapy; immune activation; inhibitor/antagonist; innovation; knockout animal; nerve injury; new therapeutic target; novel; novel strategies; public health relevance; relating to nervous system; response; sensory system

DESCRIPTION (provided by applicant): The current proposal, for the first time, addresses the role of neuro-immune activation within the central nervous system as a plausible mechanism underlying the visceral pain component of many common functional gastrointestinal disorders (FGID) including irritable bowel syndrome (IBS). Although increasing evidence has emerged for the role of spinal glia in the mechanisms mediating persistent pain, its implication in visceral pain has not been evaluated. We propose the general hypothesis that chronic stress, known as a key factor in the first onset or exacerbation of IBS symptoms, triggers the activation of a spinal network comprising neurons and immune cells (glia), playing a central role in the modulation of visceral nociception. Using a rat model of chronic water avoidance stress, we propose to characterize the role of stress-induced spinal glia activation in the modulation of visceral sensitivity and determine the molecular pathways engaged in the initiation and maintenance of visceral hyperalgesia. Our first specific aim is to assess the temporal profile of spinal glia activation during and after chronic stress and to test the ability of inhibitors specific of glia to reduce stress- induced visceral hyperalgesia. The second specific aim relates to the characterization of molecular mechanisms linking chronic stress and spinal glial activation. The experimental design proposed in this application includes the behavioral assessment of visceral sensitivity in response to different pharmacological treatments (antagonists, agonists, oligonucleotide antisenses), combined with in vitro analysis using Western blotting, multiplex ELISA, immunohistochemistry and quantitative RT-PCR. The long-term goal of the proposed studies is the characterization of signaling pathways underlying the observed endocrine-neural- immune interactions using selective knockout animals and glia/neurons co-cultures. Targeting specific mediators of the glial-neuronal crosstalk may provide an innovative approach for the development of novel therapeutic targets for the treatment of chronic pain conditions associated with enhanced stress responsiveness. The concept of stress-induced modulation of glial-neurons signaling and its implication in long-term alteration of the sensory system may be generalized to many other stress-sensitive pain conditions, including interstitial cystitis, non-cardiac chest pain and fibromyalgia. PUBLIC HEALTH RELEVANCE: In the current proposal, we have developed the concept that chronic stress may induce activation of the immune system in the spinal cord, initiating a cascade of events that will affect the sensory system. This new approach has considerable implication for the development of novel therapeutic targets for the treatment of chronic pain conditions associated with enhanced stress responsiveness, including functional gastrointestinal disorders, for which effective treatment remains a clinical challenge.

描述（由申请方提供）：当前提案首次阐述了中枢神经系统内神经免疫激活的作用，作为许多常见功能性胃肠道疾病（FGID）（包括肠易激综合征（IBS））内脏痛成分的合理机制。虽然越来越多的证据表明脊髓胶质细胞在介导持续性疼痛的机制中发挥作用，但其在内脏痛中的作用尚未得到评估。我们提出的一般假设是，慢性应激，被称为IBS症状首次发作或恶化的关键因素，触发激活的脊髓网络，包括神经元和免疫细胞（神经胶质细胞），在内脏伤害感受的调制中发挥核心作用。使用大鼠模型的慢性避水应激，我们建议的特点的作用，应激诱导的脊髓胶质细胞激活的内脏敏感性的调制和确定的分子途径参与内脏痛觉过敏的启动和维持。我们的第一个具体目标是评估在慢性应激期间和之后脊髓胶质细胞激活的时间分布，并测试胶质细胞特异性抑制剂减少应激诱导的内脏痛觉过敏的能力。第二个具体目标涉及的分子机制的特点，连接慢性应激和脊髓神经胶质细胞活化。在本申请中提出的实验设计包括响应于不同药物治疗（拮抗剂、激动剂、寡核苷酸反义物）的内脏敏感性的行为评估，结合使用蛋白质印迹法、多重ELISA、免疫组织化学和定量RT-PCR的体外分析。拟议研究的长期目标是使用选择性敲除动物和神经胶质细胞/神经元共培养物表征观察到的内分泌-神经-免疫相互作用的信号通路。靶向神经胶质-神经元串扰的特异性介质可以为开发用于治疗与增强的应激反应相关的慢性疼痛病症的新型治疗靶点提供创新方法。神经胶质神经元信号传导的应激诱导调制的概念及其在感觉系统的长期改变中的意义可以推广到许多其他应激敏感性疼痛病症，包括间质性膀胱炎、非心源性胸痛和纤维肌痛。公共卫生相关性：在目前的提案中，我们已经提出了这样的概念，即慢性应激可能会诱导脊髓中免疫系统的激活，引发一系列影响感觉系统的事件。这种新方法对于开发用于治疗与增强的应激反应相关的慢性疼痛病症（包括功能性胃肠道疾病）的新型治疗靶点具有相当大的意义，对于功能性胃肠道疾病的有效治疗仍然是临床挑战。