Impact of Alcohol on HIV Protease Inhibitor-induced ER Stress and Lipotoxicity

酒精对 HIV 蛋白酶抑制剂诱导的内质网应激和脂毒性的影响

基本信息

批准号：
8331653
负责人：
HUIPING Rose ZHOU
金额：
--
依托单位：
VA VETERANS ADMINISTRATION HOSPITAL
依托单位国家：
美国
项目类别：
财政年份：
2012
资助国家：
美国
起止时间：
2012-04-01 至 2016-03-31
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/8331653
关键词：
AIDS/HIV problem Alcohol abuse Alcohol consumption Alcoholic Liver Diseases Alcohols Apoptosis Apoptotic Attenuated CCAAT-Enhancer-Binding Proteins Calcium Caring Cessation of life Clinic Clinical Cytosol Development Endoplasmic Reticulum Epidemic Fatty Liver Functional disorder Future General Population Goals HIV HIV Infections HIV Protease Inhibitors Health Hepatic Hepatocyte Hepatotoxicity Highly Active Antiretroviral Therapy Homeostasis Homologous Protein Incidence Inflammation Injury Knock-out Life Link Lipids Liver Liver diseases Mediator of activation protein Medical Metabolic syndrome Mitochondria Molecular Mus Nutrient Pathogenesis Patients Pharmaceutical Preparations Play Population Prevalence Process Proteins Provider Quality of life Reporting Research Risk Factors Role Severities Signal Pathway Signal Transduction Stress Testing Therapeutic United States Veterans Wit alcohol misuse base cell type effective therapy endoplasmic reticulum stress human disease improved macrophage novel response

项目摘要

DESCRIPTION (provided by applicant): The hepatic lipotoxicity specifically associated with HIV protease inhibitors (PIs), the core component of highly active anti-retroviral therapy (HAART), has become a major concern in the clinic, especially in patients who consume alcohol. Alcohol abuse, which alone also produces liver toxicity, is one of the most important co-morbid risk factors for liver injury in HIV patient under current therapy. Despite the prevalence of this problem and its serious impact on the quality of life and continued therapy in HIV patients, the mechanism by which alcohol exacerbates HIV PI-induced hepatic lipotoxicity has not been identified. The goal of this proposal is to examine the potential impact of alcohol use/abuse on HIV PI- induced hepatic lipotoxicity and further elucidate the underlying cellular/molecular mechanisms. The central hypothesis of this study is that alcohol and HIV PIs additively induce hepatic lipotoxicity by activating the ER stress, subsequently disrupting lipid homeostasis and inducing apoptosis in hepatocytes. In this study, we will (1) determine the impact of alcohol on HIV PI-induced activation of ER stress, (2) determine the role of ER stress in alcohol and HIV PI-induced hepatic lipotoxicity and (3) identify the mechanism by which alcohol promotes HIV PI-induced ER stress and hepatic lipotoxicity. The long-term goal of this research is to understand the molecular/cellular mechanisms by which alcohol and HAART induce hepatic lipotoxicity. The burden of liver injury in HIV patients is expected to increase as the number of patients living wit HIV continues to rise. Understanding the mechanism by which alcohol and HIV PIs induce hepatotoxicity is of great clinical importance. Completion of these objectives will help identify new cellular mechanisms of alcohol and HIV PI-induced hepatic lipotoxicity, thereby enhancing our understanding of the mechanisms of HAART-associated liver diseases and providing novel information for the future development of new preventative and therapeutic strategies.

描述（由申请人提供）：与高效抗逆转录病毒疗法 (HAART) 核心成分 HIV 蛋白酶抑制剂 (PI) 特别相关的肝脂毒性已成为临床的主要关注点，尤其是饮酒患者。酗酒本身也会产生肝毒性，是当前治疗下 HIV 患者肝损伤最重要的共病危险因素之一。尽管这个问题很普遍，并且对 HIV 患者的生活质量和持续治疗产生严重影响，但酒精加剧 HIV PI 诱导的肝脂毒性的机制尚未确定。该提案的目的是检查饮酒/滥用酒精对 HIV PI 诱导的肝脂毒性的潜在影响，并进一步阐明潜在的细胞/分子机制。这项研究的中心假设是，酒精和 HIV PI 通过激活 ER 应激，进而破坏脂质稳态并诱导肝细胞凋亡，从而额外诱导肝脂毒性。在本研究中，我们将 (1) 确定酒精对 HIV PI 诱导的 ER 应激激活的影响，(2) 确定 ER 应激在酒精和 HIV PI 诱导的肝脂毒性中的作用，以及 (3) 通过以下方式确定其机制：其中酒精会促进 HIV PI 诱导的 ER 应激和肝脂毒性。本研究的长期目标是了解酒精和HAART诱导肝脂毒性的分子/细胞机制。随着艾滋病毒感染者人数的持续增加，预计艾滋病毒患者的肝损伤负担将会增加。了解酒精和 HIV PI 引起肝毒性的机制具有重要的临床意义。这些目标的完成将有助于确定酒精和HIV PI诱导的肝脂毒性的新细胞机制，从而增强我们对HAART相关肝病机制的理解，并为未来开发新的预防和治疗策略提供新的信息。