Brain ischemia attenuates neuropeptide biosynthesis

脑缺血减弱神经肽生物合成

• 批准号: 6871568
• 负责人: AN ZHOU
• 金额: $ 32.26万
• 依托单位: LEGACY EMANUEL HOSPITAL AND HEALTH CENTER
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-12-15 至 2008-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6871568
• 关键词: carboxypeptidase; cell death; cerebral ischemia /hypoxia; enzyme activity; enzyme induction /repression; gene expression; genetically modified animals; laboratory mouse; laboratory rat; molecular pathology; neurons; neuropeptides; prohormone convertase; protein biosynthesis; protein quantitation /detection; proteomics; secretion; stroke; tissue /cell culture

DESCRIPTION (provided by applicant): Neuropeptides play crucial roles in maintaining normal function of the brain and the brain's response to stresses, e.g. ischemia. Virtually all known neuropeptides are processed from larger precursors by the action of a set of processing enzymes in the secretory pathway. The biological function of precursor forms may differ profoundly from that of final processed forms to include even a switch from pro-apoptotic rather than anti-apoptotic function. Little is known about how the biosynthetic processing of neuropeptides may be affected by ischemic stress in the brain. Our preliminary studies indicate that ischemia causes attenuation in the activation of key neuropeptide processing enzymes and an accumulation of certain neuropeptides in precursor forms. Our hypothesis is: ischemia has adverse effects on the functional status of the neuropeptide processing system, thus impairing the ability of brain cells to produce certain protective peptide factors. This ischemia-induced attenuation of neuropeptide processing contributes to post-ischemia cell death in the brain. In the proposed study, we will first examine changes in the expression levels of several key neuropeptide processing enzymes and their enzymatic activities in ischemic rat brains. Then, we will determine the levels and molecular forms of neuropeptides that are known to have modulatory roles in the brain after ischemia and to require the action of processing enzymes investigated in this study for proper processing. Using in vitro ischemia models in cultured cells, we will investigate how ischemic stress may influence the activation and maturation processes of the processing enzymes and alter the production and secretion of neuropeptides. In parallel, we will analyze peptides secreted from ischemic cells using a quantitative proteomic approach. Finally, we will investigate if animals with specific deficiencies in neuropeptide processing may be more vulnerable to ischemic stress and determine if peptides secreted from processing-deficient neuronal cells may cause or exaggerate ischemic cells death. The proposed study will offer a novel mechanism concerning how ischemic stroke may damage the brain by attenuating neuropeptide processing. Our long-term goal is to elucidate the molecular mechanisms of neuropeptide processing-mediated stress response of the brain.

描述（由申请人提供）：神经肽在维持脑的正常功能和脑对应激（例如缺血）的反应中起关键作用。几乎所有已知的神经肽都是通过分泌途径中一组加工酶的作用从较大的前体加工而来的。前体形式的生物学功能可能与最终加工形式的生物学功能有很大不同，甚至包括从促凋亡功能而不是抗凋亡功能的转换。关于脑缺血应激如何影响神经肽的生物合成过程知之甚少。我们的初步研究表明，缺血导致衰减的关键神经肽加工酶的激活和积累的某些神经肽的前体形式。我们的假设是：局部缺血对神经肽加工系统的功能状态具有不利影响，从而损害脑细胞产生某些保护性肽因子的能力。这种缺血诱导的神经肽加工的衰减有助于脑中的缺血后细胞死亡。在这项研究中，我们将首先研究缺血大鼠脑中几种关键神经肽加工酶的表达水平及其酶活性的变化。然后，我们将确定神经肽的水平和分子形式，已知这些神经肽在缺血后的大脑中具有调节作用，并且需要本研究中研究的加工酶的作用来进行适当的加工。利用体外培养细胞的缺血模型，我们将研究缺血应激如何影响加工酶的激活和成熟过程，并改变神经肽的产生和分泌。同时，我们将使用定量蛋白质组学方法分析缺血细胞分泌的肽。最后，我们将调查是否有特定缺陷的神经肽加工的动物可能更容易受到缺血性应激，并确定是否从加工缺陷的神经元细胞分泌的肽可能会导致或夸大缺血性细胞死亡。这项研究将提供一种新的机制，即缺血性中风如何通过减弱神经肽加工来损害大脑。我们的长期目标是阐明神经肽加工介导的脑应激反应的分子机制。