Alcohol Abuse and HIV-1: Mechanisms of Combined CNS Injury and Interventions

酒精滥用和 HIV-1：中枢神经系统联合损伤的机制和干预措施

• 批准号: 8283461
• 负责人: James Haorah
• 金额: $ 6.97万
• 依托单位: TEMPLE UNIV OF THE COMMONWEALTH
• 依托单位国家: 美国
• 财政年份: 2007
• 资助国家: 美国
• 起止时间: 2007-09-30 至 2012-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8283461
• 关键词: Acetaldehyde; Address; Affect; Alcohol abuse; Alcohol consumption; Alcohol dependence; Alcohol withdrawal syndrome; Alcoholism; Alcohols; American; Amino Acid Transporter; Animal Feed; Animal Model; Animals; Antioxidants; Antiviral Agents; Applications Grants; Arachidonic Acids; Astrocytes; Biological; Blood - brain barrier anatomy; Brain; Brain Injuries; Cells; Central Nervous System Infections; Cessation of life; Chronic; Clinical Research; Cognitive deficits; Collaborations; Cytochrome P-450 CYP2E1; Cytochromes; Cytokine Activation; Data; Dementia; Dependence; Down-Regulation; Encephalitis; Endothelium; Ethanol; Ethanol Metabolism; Evaluation; Excitatory Amino Acids; Exposure to; Free Radicals; Functional disorder; Future; Generations; Genetic Transcription; Glutamate Transporter; Glutamates; HIV Envelope Protein gp120; HIV-1; Health; Human; ITPR1 gene; Image; Immune; Immune response; Immune system; Immunosuppression; Impaired cognition; Impairment; In Vitro; Individual; Infection; Inflammation; Inflammation Mediators; Inflammatory; Injury; Interstitial Collagenase; Intervention; Investigation; Lead; Levocarnitine Acetyl; Link; Magnetic Resonance Spectroscopy; Maps; Matrix Metalloproteinases; Measures; Mediating; Mediator of activation protein; Metabolism; Metalloproteases; Microglia; Modeling; Molecular; Mononuclear; Mus; NADP; NOD/SCID mouse; Nerve Degeneration; Neuraxis; Neuroglia; Neuronal Injury; Neurons; Nitric Oxide; Non obese; Organ; Outcome; Oxidative Stress; Oxidative Stress Induction; Pathway interactions; Peripheral Blood Lymphocyte; Permeability; Pharmaceutical Preparations; Phenotype; Phospholipase A2; Phospholipase C; Phosphorylation; Production; Prostaglandins; Protein Tyrosine Kinase; Proteins; Radiology Specialty; Reaction; Reactive Oxygen Species; Regulation; Research; Role; Signal Pathway; Signal Transduction; Specimen; Stimulus; System; TLR4 gene; Testing; Therapeutic; Tight Junctions; Time; Toll-like receptors; Toxic effect; United States; Viremia; Western Blotting; Withdrawal Symptom; Work; Xanthine Oxidase; alcohol craving; alcohol exposure; astrogliosis; base; brain cell; brain tissue; central nervous system injury; chemokine; cytokine; diabetic; excitotoxicity; extracellular; feeding; human NOS2A protein; immunocytochemistry; in vivo; inhibitor/antagonist; insight; macrophage; methylxanthine; migration; monocyte; nerve injury; neuroimaging; neuroinflammation; neuropathology; neurotoxic; neurotoxicity; novel; oxidative damage; prevent; problem drinker; propentofylline; protective effect; protein expression; public health relevance; response; rho GTP-Binding Proteins; src-Family Kinases; therapeutic target; toll-like receptor 4; uptake; white matter

DESCRIPTION (provided by applicant): Alcohol is the most commonly used and abused drug in the United States. Deleterious alcohol-related health effects, attributed to internal organ toxicity, include irreversible brain tissue injury. Brain tissue of chronic alcoholics features neurodegeneration paralleling neuro-cognitive deficits. The causes of HIV-1-associated neurotoxicity, clinically manifesting as HIV-1 associated dementia (HAD), include excitotoxic effects of glutamate, secretory products of chronically activated glial cells, and oxidative stress, similar culprits to ones mediating alcohol-induced neuronal injury. Alcohol abuse and HIV-1 infection of central nervous system (CNS) could result in combined toxic effects leading to neuronal demise and cognitive dysfunction. The current grant application is focused on putative mechanisms of enhanced neurotoxicity in the setting of alcohol abuse and HIV-1 CNS infection. Specifically, we will study unique aspects of astrocyte dysfunction caused by HIV-1 CNS infection and alcohol abuse. We hypothesize that astrocyte dysfunction caused by alcohol metabolites and oxidative stress results in (1) increased glutamate levels via down regulation of excitatory amino acid transporter (EAAT-2, the primary astrocyte glutamate scavenger) causing neuronal injury; (2) production of pro-inflammatory factors (via activation of Src kinases and phospholipase A2); and (3) enhanced activity of metalloproteases (MMPs) resulting in loss of blood brain barrier (BBB) integrity. We mechanistically address the role of oxidative stress in astrocytes leading to production of pro-inflammatory molecules and impairment of glutamate uptake by astrocytes. Using a combination of in vitro systems, an HIVE animal model chronically exposed to alcohol, and in vivo magnetic resonance spectroscopy, we will investigate the astrocyte dysfunction as a focal point of combined effects of HIV-1 and alcohol abuse in the CNS. We will address the following questions: (1) What are the underlying mechanisms causing astrocyte pro-inflammatory phenotype in the setting of alcohol abuse and HIV-1 CNS infection that cause activation of MMPs and BBB dysfunction? (Aim 1); (2) What is the role/contribution of enhanced production of reactive oxygen species, Rho GTPases, and NF-?B signaling in diminished expression and function of EAAT-2 in astrocytes? (Aim 2); (3) How effective are the therapeutics that target oxidative stress and EAAT-2 dysregulation in ameliorating neurotoxicity and BBB impairment in an animal model for HIV-1 encephalitis and alcohol abuse? (Aim 3). Antioxidants and specific signaling inhibitors will be utilized to delineate pathways involved in these effects. We believe that the proposed works are highly significant as they will uncover novel mechanisms involved in the combined effects of HIV-1 and alcohol abuse in the CNS and propose therapeutic approaches based on these investigations. Public Health Relevance: Alcohol is abused by millions of Americans has long lasting toxic effects on the central nervous system. Clinical studies indicated that alcohol dependence has an additive effect on cognitive deficits associated with HIV-1 infection. Current proposal aims to understand mechanisms of combined effects of HIV-1 and alcohol abuse in the brain and to propose neuroprotective therapies.

描述（由申请人提供）：酒精是美国最常用和滥用的药物。归因于内部器官毒性的有害酒精相关的健康影响包括不可逆的脑组织损伤。慢性酒精中毒的脑组织具有神经退行性平行的神经认知缺陷。 HIV-1相关的神经毒性的原因，临床上表现为HIV-1相关痴呆（HAD），包括谷氨酸的兴奋性毒性作用，长期激活的神经胶质细胞的分泌产物和氧化胁迫的分泌产物，类似的罪魁祸首，类似于介导酒精诱发的神经元损伤的元素。中枢神经系统（CNS）的酒精滥用和HIV-1感染可能会导致毒性作用，导致神经元灭亡和认知功能障碍。当前的赠款应用集中在酗酒和HIV-1 CNS感染中的推定神经毒性的假定机制上。具体而言，我们将研究由HIV-1 CNS感染和酗酒引起的星形胶质细胞功能障碍的独特方面。我们假设由酒精代谢物引起的星形胶质细胞功能障碍和氧化应激导致（1）通过降低兴奋性氨基酸转运蛋白（EAAT-2，主要星形胶质细胞谷氨酸清除剂），导致谷氨酸水平升高，导致神经元损伤； （2）产生促炎性因子（通过激活SRC激酶和磷脂酶A2）； （3）金属蛋白酶（MMP）的活性增强，导致血脑屏障（BBB）完整性丧失。我们从机械上解决了氧化应激在星形胶质细胞中的作用，导致促炎分子的产生以及星形胶质细胞对谷氨酸摄取的损害。使用体外系统的组合，长期暴露于酒精的蜂巢动物模型以及体内磁共振光谱，我们将研究星形胶质细胞功能障碍，这是CNS中HIV-1和酒精滥用的综合作用的焦点。我们将解决以下问题：（1）在酒精滥用和HIV-1 CNS感染的情况下引起星形胶质细胞促炎表型的基本机制是什么？ （目标1）; （2）增强活性氧，Rho GTPases和NF-？B信号在星形胶质细胞中EAAT-2的表达和功能下降的作用/贡献是什么？ （目标2）; （3）针对HIV-1脑炎和酗酒的动物模型，靶向氧化应激和EAAT-2失调的治疗疗法在改善神经毒性和BBB损害中的有效性如何？ （目标3）。将利用抗氧化剂和特定的信号抑制剂来描述与这些作用有关的途径。我们认为，提出的作品非常重要，因为它们将发现中枢神经系统中HIV-1和酗酒的综合作用涉及的新型机制，并根据这些研究提出了治疗方法。 公共卫生相关性：数百万美国人滥用酒精对中枢神经系统的毒性影响持续持久。临床研究表明，酒精依赖性对与HIV-1感染相关的认知缺陷具有附加作用。当前的建议旨在了解HIV-1和酗酒在大脑中的综合作用的机制，并提出神经保护疗法。