Mechanisms of Responses to Diesel Exhaust and Stress

对柴油机尾气和压力的反应机制

• 批准号: 7474598
• 负责人: ROBERT John LAUMBACH
• 金额: $ 13.26万
• 依托单位: UNIV OF MED/DENT NJ-R W JOHNSON MED SCH
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-09-23 至 2010-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7474598
• 关键词: Acute; Acute-Phase Proteins; Address; Air Pollutants; Air Pollution; Alveolar Macrophages; Animal Model; Animals; Antioxidants; Aorta; Apolipoprotein E; Atherosclerosis; Binding; Blood; Blood Circulation; Blood Coagulation Factor VII; Blood Vessels; Breathing; Bronchoalveolar Lavage; Cardiovascular Diseases; Cardiovascular system; Cell Adhesion Molecules; Cell Count; Cells; Coronary; Coronary artery; Corticosterone; Corticotropin-Releasing Hormone; Cultured Cells; Dependence; Deposition; Development Plans; Dichloromethylene Diphosphonate; Diesel Exhaust; Educational Activities; Enzyme-Linked Immunosorbent Assay; Epidemiologic Studies; Epinephrine; Exhibits; Exposure to; Factor VIII; Fibrinogen; Goals; Heart; Hepatic; Histology; Hormones; Hour; Human; Hyperlipidemia; Immunohistochemistry; In Situ Hybridization; Individual; Inflammation; Inflammatory; Inflammatory Response; Inhalation Toxicology; Injury; Interleukin-1; Interleukin-6; Knockout Mice; Laboratories; Learning; Lipids; Lipoproteins; Liposomes; Liver; Lung; Measures; Mediating; Mediator of activation protein; Mentorship; Messenger RNA; Metabolism; Modeling; Monitor; Mus; Norepinephrine; Numbers; Operative Surgical Procedures; Organ; Outcome Measure; Particulate Matter; Plasma; Plasminogen Activator Inhibitor 1; Plasminogen Inactivators; Play; Pneumonia; Predisposition; Procedures; Production; Proteins; Psychoneuroimmunology; Research; Research Personnel; Reverse Transcriptase Polymerase Chain Reaction; Risk; Role; Serum; Site; Staining method; Stains; Stress; Structure; Techniques; Testing; Thrombophilia; Thrombosis; Tissues; Toxic effect; Training; Travel; Tumor Necrosis Factor-alpha; Vascular Diseases; Western Blotting; Wild Type Mouse; air filter; atherothrombosis; biological adaptation to stress; cardiovascular risk factor; career; concept; cytokine; exhaust; exposed human population; lipid transport; lung injury; macrophage; monocyte; mortality; programs; protein expression; research and development; research study; response; restraint stress; stressor

DESCRIPTION (provided by applicant) The proposed career development and research plans will prepare the candidate to conduct independent research focusing on how the toxic effects of air pollutants may be modified in susceptible individuals, using animal models. Evidence from epidemiological studies indicates that individuals with pre-existing cardiovascular (CV) disease are at increased risk of CV effects from particulate matter air pollution (PM). The research plan will test the hypothesis that the CV effects of PM are mediated by systemic inflammatory responses to local injury and inflammation in the lungs, and that altered macrophage numbers and activity in lung and liver contribute to increased sensitivity of apolipoprotein E-deficient (ApoE-/-) mice to these effects. Moreover, toxic effects will be enhanced by co-exposure to stress. To test this hypothesis, the candidate will use freshly generated diesel exhaust (DE) as a model PM exposure. The first aim is to determine if ApoE-/- mice exhibit increased susceptibility to DE-induced pulmonary and systemic inflammation and prothrombotic activity. ApoE-/- and control mice will be exposed to DE (30-1000 mu/g/m3 PM) or control for 3-6 hours, with outcomes measured at 0-72 hours post-exposure. Markers of inflammation will be assessed in the lung, liver, blood, and blood vessels, including cell counts, cytokine expression, circulating acute phase proteins, and cell adhesion molecules. The second aim is to determine if increases in the sensitivity of ApoE-/- mice to DE are due to increased macrophage numbers and activity in the lung and liver. Dependence of DE-induced effects on macrophages will be tested by selectively depleting these cells using liposomes. The third aim is to determine if stress alters DE-induced inflammatory responses and prothrombotic activity. Inflammation and prothrombotic activity will be analyzed in ApoE-/- and control mice after exposure to DE with and without an acute stressor. Career development plans include mentorship and training in inhalation toxicology and psychoneuroimmunology through supervised research and structured educational activities. Laboratory techniques to be learned include animal exposures, surgery, cell culture, western blotting, ELISA, in situ hybridization, RT-PCR and histochemical procedures. The career development plan will enable the candidate to achieve his overall goal of conducting research that integrates animal studies with human exposure studies. The experimental studies will contribute to elucidating mechanisms underlying CV effects of PM.

描述（由申请人提供） 拟议的职业发展和研究计划将准备候选人进行独立的研究，重点是如何空气污染物的毒性影响可能会在易感人群中修改，使用动物模型。 来自流行病学研究的证据表明，预先存在心血管（CV）疾病的个体受颗粒物空气污染（PM）影响的CV风险增加。该研究计划将检验以下假设：PM的CV效应是由对肺部局部损伤和炎症的全身炎症反应介导的，肺和肝脏中巨噬细胞数量和活性的改变有助于载脂蛋白E缺陷（ApoE-/-）小鼠对这些效应的敏感性增加。 此外，共同暴露于压力会增强毒性效应。为了检验这一假设，候选人将使用新产生的柴油废气（DE）作为模型PM暴露。 第一个目的是确定ApoE-/-小鼠是否表现出对DE诱导的肺部和全身炎症以及促血栓形成活性的易感性增加。 ApoE-/-和对照小鼠将暴露于DE（30-1000 mu/g/m3 PM）或对照3-6小时，在暴露后0-72小时测量结果。 将在肺、肝、血液和血管中评估炎症标志物，包括细胞计数、细胞因子表达、循环急性期蛋白和细胞粘附分子。 第二个目的是确定ApoE-/-小鼠对DE的敏感性增加是否是由于肺和肝脏中巨噬细胞数量和活性增加。 DE诱导的效应对巨噬细胞的依赖性将通过使用脂质体选择性消耗这些细胞来测试。 第三个目的是确定应激是否改变DE诱导的炎症反应和促血栓形成活性。在暴露于DE（有和无急性应激物）后，将分析ApoE-/-和对照小鼠的炎症和促血栓形成活性。 职业发展计划包括指导和培训吸入毒理学和心理神经免疫学通过监督研究和结构化的教育活动。将要学习的实验室技术包括动物暴露、手术、细胞培养、蛋白质印迹、ELISA、原位杂交、RT-PCR和组织化学程序。职业发展计划将使候选人能够实现其总体目标，即进行将动物研究与人体暴露研究相结合的研究。这些实验研究将有助于阐明PM CV效应的机制。