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CYTOKINES, BEHAVIOR, AND MENTAL HEALTH

细胞因子、行为和心理健康

基本信息

批准号：
2693408
负责人：
Keith W Kelley
金额：
$ 26.58万
依托单位：
UNIVERSITY OF ILLINOIS AT URBANA-CHAMPAIGN
依托单位国家：
美国
项目类别：
财政年份：
1995
资助国家：
美国
起止时间：
1995-09-01 至 2003-05-31
项目状态：
已结题

项目摘要

DESCRIPTION: (Applicant's Abstract): Individuals suffering from CNS-related pathologies, such as AIDS-related dementia and Alzheimer's disease, display a variety of behavioral and neurological symptoms including memory loss, lack of motivation and deterioration of motor functions. The proinflamatory cytokines TFNa and IL-1b are expressed in the brain in response to these diseases as well as to other insults, such as stroke, trauma, and peripheral inflammation. The potent anti-inflammatory cytokines IL-4 and IL-10 have recently been localized to the CNS, and the emerging idea is that both acute and chronic inflammatory pathologies are regulated by the balance of proinflammatory and anti-inflammatory cytokines in the brain. The investigators' preliminary data showing the IL-4 and IGF-I are active in the CNS to inhibit sickness behavior induced by centrally administered LPS support this concept. Receptors for both IL-4 and IGF-I utilize a cytoplasmic docking molecule known as Insulin-Receptor Substrate-1 (IRS-1) or IRS-2 (formally known as IL-4 receptor phosphorylated substrate). The cytoplasmic docking molecules activate Phosphatidylinositol 3-Kinase (PI 3-kinase), an enzyme recently shown to be critical in protecting against cellular insults and promoting the survival of many cells, including neurons and perhaps glia. The investigators hypothesize that activation of the IRS/PI 3-kinase proteins is a common element int he signaling pathways utilized by receptors for anti-inflammatory cytokines in the CNS, and that this activations pathway is inhibited by TNFa and IL-1b. Unfortunately, the localization, expression, activation (tyrosine phosphorylation) and inhibition (serine phosphorylation) of IRS proteins in the CNS have not been identified. The investigators indicate that they now have strong preliminary data showing that both IRS-1 and IRS-2 are expressed in primary mouse glia and neurons and that IL-4, IL-10, and IGF-I activate PI 3-kinase in glial cells. The possibility that proinflammatory cytokines can directly inhibit the protective actions of anti-inflammatory cytokines in the brain would be a pivotal discovery. Indeed, IRS-recruited PI 3-kinase activity may be a critical intermediate signaling molecule in this process and is likely to provide a novel target for intervention in neuropathologies. The investigators indicate that they have developed all of the techniques and generated preliminary data to support the hypothesis of a common IRS/PI 3-kinase signaling pathways by which proinflammatory cytokines antagonize the activities of anti-inflammatory cytokine receptors in the CNS. These experiments are needed to understand the critical signaling molecules that are likely to regulate the events that lead to debilitating and costly inflammatory afflictions in the brain.

描述：（申请人的摘要）：患有 CNS相关的病理，如艾滋病相关的痴呆症和阿尔茨海默氏症疾病，表现出各种行为和神经症状，包括记忆力减退，缺乏动力和运动功能恶化。的促炎细胞因子TFNa和IL-1b在脑中表达对这些疾病以及对其他损伤的反应，例如中风，创伤和外周炎症。有效的抗炎细胞因子 IL-4和IL-10最近已经定位于CNS，并且新兴的IL-4和IL-10在CNS中表达。观点是急性和慢性炎症病理都受到调节，通过促炎细胞因子和抗炎细胞因子的平衡，个脑袋研究人员的初步数据显示，IL-4和IGF-I是在中枢神经系统中具有活性，可抑制中枢神经系统诱发的疾病行为。给予的LPS支持这一概念。 IL-4和IGF-I受体利用称为胰岛素受体底物-1的细胞质对接分子 IRS-1或IRS-2（正式称为IL-4受体磷酸化底物）。细胞质对接分子激活磷脂酰肌醇3-激酶（PI 3-激酶），一种最近被证明在保护免受细胞损伤和促进许多细胞的存活，包括神经元也许还有胶质细胞。研究人员假设， IRS/PI 3-激酶蛋白是信号通路中的常见元件由CNS中抗炎细胞因子的受体利用，并且该活化途径被TNF α和IL-1b抑制。可惜定位、表达、活化（酪氨酸磷酸化）和抑制（丝氨酸磷酸化）IRS蛋白在中枢神经系统还没有鉴定调查人员表示，他们现在有强大的初步数据显示IRS-1和IRS-2在原发性肝癌中表达， IL-4、IL-10和IGF-I激活PI 3-激酶在神经胶质细胞中。促炎性细胞因子可以直接抑制脑中抗炎细胞因子的保护作用将是一个关键性的发现事实上，IRS募集的PI 3-激酶活性可能是这一过程中的关键中间信号分子，可能为神经病理学的干预提供新的靶点。的调查人员表示，他们已经开发了所有的技术，生成的初步数据支持共同IRS/PI的假设 3-促炎细胞因子拮抗的激酶信号通路 CNS中抗炎细胞因子受体的活性。这些需要实验来了解关键的信号分子，很可能会对导致经济衰退和代价高昂的脑部炎症