权益分类	功能权益	普通用户	{{item.name}}会员
{{category.name}}	{{benefitItem.name}}

CGRP CONTROL IN TRIGEMINAL NEURONS IN VITRO AND IN VIVO

CGRP 对三叉神经元的体外和体内控制

基本信息

批准号：
7081411
负责人：
PAUL L DURHAM
金额：
$ 19.24万
依托单位：
MISSOURI STATE UNIVERSITY
依托单位国家：
美国
项目类别：
财政年份：
2003
资助国家：
美国
起止时间：
2003-08-01 至 2007-07-31
项目状态：
已结题

项目摘要

DESCRIPTION (provided by applicant): The goal of the proposed research is to understand the mechanisms by which NO and TNFalpha regulate CGRP expression in cultured trigeminal neurons and an in vivo model of TMJ inflammation. CGRP is thought to play a key role in underlying pathology of TMJ disorders (TMJDs). High levels of the neuropeptide CGRP present in the synovial fluid during TMJDs are associated with pain. In addition to CGRP, the levels of NO and TNF have been reported to be elevated during TMJ inflammation. The cellular mechanisms by which CGRP expression is controlled during TMJDs are not known. In this proposal, I will test the hypothesis that NO and TNF directly stimulate CGRP gene expression in cultured trigeminal ganglia neurons and in vivo TMJ models. In addition, the role of NO and TNF in the pathogenesis of TMJ inflammation will be investigated. Studies proposed in the first aim will determine the effect of NO and TNF alone or in combination with other inflammatory mediators on CGRP release from trigeminal neurons. The second aim will focus on identifying the basal (unstimulated), and NO- and TNF-responsive regulatory sites in the CGRP promoter. Primary trigeminal cultures will be transiently transfected with CGRP-luciferase reporter constructs and reporter activity measured. The goal of the third aim is to elucidate the pathways involved in NO and TNF signaling in trigeminal neurons. Specific cyclase and kinase inhibitors and activators will be used to identify the major signaling pathway(s) involved in regulating CGRP. Further studies of individual pathways will utilize phosphospecific antibodies and signaling pathway detection kits. In the fourth aim, NO and TNF regulation of CGRP expression will be extended to in vivo models of TMJ inflammation. Also, the role of NO and TNF in the pathogenesis of TMJ inflammation in vivo will be investigated and whether specific inhibitors of signaling pathways can reduce TMJ inflammation. Results from these studies will provide valuable insight into the cellular and molecular mechanisms that control CGRP gene expression in trigeminal neurons that may lead to the development of novel therapeutic strategies for TMJDs and other inflammatory diseases.

描述（由申请人提供）：本研究的目的是了解NO和TNF α调节培养的三叉神经元和TMJ炎症体内模型中CGRP表达的机制。 CGRP被认为在颞下颌关节疾病（TMJDs）的潜在病理学中起关键作用。在TMJD期间，滑液中存在高水平的神经肽CGRP与疼痛相关。除CGRP外，据报道在TMJ炎症期间NO和TNF水平升高。在TMJD期间控制CGRP表达的细胞机制尚不清楚。在这个建议中，我将测试的假设，NO和TNF直接刺激CGRP基因表达在培养的三叉神经节神经元和在体内TMJ模型。此外，NO和TNF在TMJ炎症发病机制中的作用也将被研究。在第一个目标中提出的研究将确定NO和TNF单独或与其他炎症介质组合对三叉神经神经元CGRP释放的影响。第二个目标将集中在确定的基础（未受刺激），NO和TNF-反应的CGRP启动子的调节位点。原代三叉神经培养物将用CGRP-荧光素酶报告基因构建体瞬时转染，并测量报告基因活性。第三个目标是阐明三叉神经元中NO和TNF信号通路。特异性环化酶和激酶抑制剂和激活剂将用于鉴定参与调节CGRP的主要信号传导途径。进一步研究个别途径将利用磷酸特异性抗体和信号通路检测试剂盒。在第四个目标中，NO和TNF对CGRP表达的调节将扩展到TMJ炎症的体内模型。此外，NO和TNF在体内TMJ炎症发病机制中的作用将被研究，以及信号通路的特异性抑制剂是否可以减轻TMJ炎症。这些研究的结果将为控制三叉神经元CGRP基因表达的细胞和分子机制提供有价值的见解，这可能导致TMJD和其他炎症性疾病的新治疗策略的发展。