Investigations into the mouse olivocochlear system

小鼠橄榄耳蜗系统的研究

• 批准号: 6865643
• 负责人: DOUGLAS E VETTER
• 金额: $ 39.63万
• 依托单位: TUFTS UNIVERSITY BOSTON
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-04-01 至 2009-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6865643
• 关键词: SDS polyacrylamide gel electrophoresis; corticotropin releasing factor; cyclic AMP; developmental neurobiology; ear hair cell; genetically modified animals; hearing; hormone receptor; immunoelectron microscopy; immunoprecipitation; laboratory mouse; neural transmission; noise induced deafness; olivocochlear bundle; phosphorylation; protein structure function; receptor expression; second messengers; voltage /patch clamp

DESCRIPTION (provided by applicant): Corticotropin releasing hormone (CRH) receptors, and urocortin, a member of the CRH family of peptides, has recently been discovered expressed in outer hair cells and olivocochlear terminals, respectively. While analysis of the role played by urocorUn, the only known ligand expressed in the inner ear capable of activating the CRH receptors, has been analyzed using urocortin deficient mice, nothing is known of the developmental expression pattern or role of the CRH receptors in the inner ear. The CRH receptors are G protein coupled receptors, and stimulate the cAMP second messenger-signaling cascade. We hypothesize that activation of the CRH receptors may represent one phenomenon underlying protection from noise induced hearing loss. The mechanisms of action may include phosphorylation and inactivation of the sK2 calcium-activated apamin-sensitive potassium channel. In order to further analyze the morphological aspects of the CRH system in the cochlea, its functional role in hearing and protection from noise induced hearing loss, and finally, to assess the cellular mechanisms of action associated with activation of the CRH receptors, three specific aims are proposed. First, we will establish the developmental and adult expression pattern of the CRH receptors in the inner ear. Successful completion of the experiments of this specific aim will establish the precise identity of the cells within the inner ear that express the CRH receptors, and identify the postsynaptic elements of the urocortin immunopositive fibers at the ultra structural level. Second, we will establish the functional roles CRH plays in hearing, and whether they participate in protection of the inner ear from noise induced hearing loss. This aim will be accomplished using mice that lack the gene for either the type 1 or the type 2 CRH receptor, or that lack both. Finally, we will use these mice to establish whether there are alterations in cAMP induced phosphorylation of targets in the outer hair cells following CRH receptors gene ablation. Success in this aim will allow us to identify individual proteins phosphorylated due to activation of the CRH receptors, as well as their role in modulating normal olivocochlear synaptic activity. This will functionally link the urocortin hormone/CRH receptor and classical ACh neurotransmitter systems together in a unified model explaining inner ear based protection from noise induced hearing loss.

描述（由申请人提供）：促肾上腺皮质激素释放激素（CRH）受体和尿皮质素是CRH肽家族的成员，最近被发现分别在外毛细胞和耳蜗末梢表达。虽然对urocorUn（唯一已知的内耳中表达的能够激活CRH受体的配体）的作用进行了分析，但对内耳中CRH受体的发育表达模式或作用一无所知。CRH受体是G蛋白偶联受体，刺激cAMP第二信使信号级联。我们假设CRH受体的激活可能代表了一种潜在的保护噪声引起的听力损失的现象。其作用机制可能包括sK2钙激活的阿帕胺敏感钾通道的磷酸化和失活。为了进一步分析耳蜗中CRH系统的形态学特征及其在听力和噪声性听力损失中的功能作用，并最终评估与CRH受体激活相关的细胞作用机制，本文提出了三个具体目标。首先，我们将建立CRH受体在内耳的发育和成年表达模式。成功完成这一特定目的的实验将建立内耳中表达CRH受体的细胞的精确身份，并在超结构水平上鉴定尿皮质素免疫阳性纤维的突触后元件。第二，我们将确定CRH在听力中的功能作用，以及它们是否参与保护内耳免受噪声性听力损失。这一目标将在缺乏1型或2型CRH受体基因的小鼠中实现，或者两者都缺乏。最后，我们将使用这些小鼠来确定在CRH受体基因消融后cAMP诱导的外毛细胞靶点磷酸化是否存在改变。这一目标的成功将使我们能够识别由于CRH受体激活而磷酸化的单个蛋白质，以及它们在调节正常耳蜗突触活性中的作用。这将在功能上将尿皮质激素/CRH受体和经典乙酰胆碱神经递质系统联系在一起，在一个统一的模型中解释内耳保护免受噪音引起的听力损失。