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Mechanisms of Sensitization to TNF hepatotoxicity in ALD

ALD 中 TNF 肝毒性的致敏机制

基本信息

批准号：
7800454
负责人：
ZHENYUAN SONG
金额：
$ 11.03万
依托单位：
UNIVERSITY OF ILLINOIS AT CHICAGO
依托单位国家：
美国
项目类别：
财政年份：
2005
资助国家：
美国
起止时间：
2005-09-15 至 2010-08-31
项目状态：
已结题

项目摘要

DESCRIPTION (provided by applicant): Alcoholic liver disease (ALD) continues to be an important health problem in the United States. Abnormal hepatic methionine metabolism is an acquired metabolic abnormality in ALD and the effects of chronic alcohol intake on hepatic methionine metabolism are initially seemingly paradoxic. Whereas alcohol consumption causes hepatic deficiency of S-adenosylmethionie (SAMe), it elevates hepatic homocysteine levels, a product of SAMe metabolism. Decreased SAMe levels and elevated homocysteine levels may contribute to alcohol induced liver injury. The effect of alcohol on S-adenosylhomocysteine (SAH) levels, another metabolite in the methionine metabolism pathway, has received little investigative attention. It is our working hypothesis that tumor necrosis factor (TNF) in conjunction with certain metabolic abnormalities observed in ALD, such as altered intracellular methylation status due to abnormal methionine/SAMe/SAH metabolism play an etiologic role in the development of liver injury in ALD. We postulate that chronic alcohol abuse causes increased gut permeability and endotoxemia, generation of reactive oxygen intermediates, activation of Kupffer cell NFkB with increased TNF production, decreased hepatocyte MAT activity with subsequent SAMe deficiency, increased S-adenosylhomocysteine (SAH) concentrations, inhibition of transmethylation reactions, decreased hepatic methylation status, elevated expression/ activation/activity of proteins sensitive to intracellular methylation status such as caspase-8, mitochondrial dysfunction, increased susceptibility to hepatic TNF cytotoxicity, and subsequent liver injury. In this proposal, we will evaluate inhibition of hepatic transmethylation reactions by chronic alcohol exposure as a mechanism for hepatic sensitization to TNF-induced cytotoxicity in a relevant model of ALD. The specific objectives of this project are as follows: 1. Evaluate the effects of inhibition of hepatic transmethylation reactions on "sensitization" to TNF hepatotoxicity; 2. Investigate possible mechanisms by which inhibition of transmethylation reactions sensitizes hepatocytes to TNF hepatotoxicity; and 3. Evaluate the effects of chronic alcohol consumption (+/- SAMe supplementation) on hepatic methylation status and sensitization to TNF-hepatotoxicity in rats intragastrically fed alcohol. This research will be performed with structured mentoring support and a detailed training program designed to maximize my opportunity to become an independent NIH-funded investigator.

描述（由申请人提供）：酒精性肝病（ALD）仍然是美国重要的健康问题。肝脏蛋氨酸代谢异常是ALD患者的一种获得性代谢异常，慢性酒精摄入对肝脏蛋氨酸代谢的影响最初似乎是矛盾的。而酒精消费导致S-腺苷甲硫氨酸（SAMe）的肝脏缺乏，它提高了肝脏同型半胱氨酸水平，SAMe代谢的产物。 SAMe水平降低和同型半胱氨酸水平升高可能有助于酒精诱导的肝损伤。酒精对S-腺苷高半胱氨酸（SAH）水平（蛋氨酸代谢途径中的另一种代谢物）的影响很少受到研究关注。我们的工作假设是，肿瘤坏死因子（TNF）与在酒精性肝脏病中观察到的某些代谢异常（例如由于甲硫氨酸/SAMe/SAH代谢异常而导致的细胞内甲基化状态改变）一起在酒精性肝脏病肝损伤的发展中发挥病因作用。我们推测，慢性酒精滥用导致肠道通透性增加和内毒素血症，活性氧中间体的产生，库普弗细胞NF κ B的激活和TNF的产生增加，肝细胞MAT活性降低和随后的SAMe缺乏，S-腺苷高半胱氨酸（SAH）浓度增加，甲基化反应的抑制，肝甲基化状态降低，对细胞内甲基化状态敏感的蛋白质（例如胱天蛋白酶-8）的表达/活化/活性升高、线粒体功能障碍、对肝TNF细胞毒性的易感性增加以及随后的肝损伤。在这个提议中，我们将评估慢性酒精暴露对肝甲基转移反应的抑制作用，作为ALD相关模型中肝对TNF诱导的细胞毒性敏感的机制。本项目的具体目标如下：1.评价抑制肝脏甲基转移反应对TNF肝毒性“致敏”的影响; 2.研究抑制转甲基化反应使肝细胞对TNF肝毒性敏感的可能机制;和3.评价长期饮酒（+/- SAMe补充）对灌胃酒精大鼠肝脏甲基化状态和TNF肝毒性致敏的影响。这项研究将在结构化的指导支持和详细的培训计划下进行，旨在最大限度地提高我成为独立NIH资助研究者的机会。