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Investigation of Nephrotic Syndrome

肾病综合症的调查

基本信息

批准号：
9143746
负责人：
Lionel Claudius Clement
金额：
$ 3.42万
依托单位：
UNIVERSITY OF ALABAMA AT BIRMINGHAM
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：
2012-08-01 至 2016-07-31
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/9143746
关键词：
ANGPTL4 gene Address Adipose tissue Affect Basement membrane Binding Binding Proteins Biological Biology Blood Circulation Charge Cholesterol Complex Data Development Development Plans Diffuse Disease Edema Endothelium Event Extravasation Foot Process Foundations Gene Expression Glucocorticoid Receptor Glucocorticoids Glycoproteins Goals Grant High Density Lipoproteins Hour Human Hyperlipidemia Hypertriglyceridemia Hypoalbuminemia In Vitro Investigation K-Series Research Career Programs Kidney Failure Laboratories Link Lipase Lipids Lipoprotein Binding Manuscripts Mediating Mediator of activation protein Medicine Mentors Mus Nature Nephrosis Nephrotic Syndrome Organ Pathogenesis Patients Plasma Post-Translational Protein Processing Protein Secretion Proteins Proteinuria Proteomics Publishing Puromycin Rattus Recombinant Proteins Regulation Renal glomerular disease Reporter Research Response Elements Role Sialic Acids Signal Transduction Staging Surface Techniques TimeLine Tissues Training Transgenic Organisms Triglycerides Up-Regulation Vascular Endothelium Work Writing apolipoprotein C-II base career development expectation glomerular basement membrane hypercholesterolemia improved lipoprotein lipase lipoprotein lipase inhibitor meetings particle podocyte promoter receptor responsible research conduct sialylation skills study characteristics uptake

项目摘要

DESCRIPTION (provided by applicant): Nephrotic syndrome is a major cause of kidney failure, and patients with this condition develop large amounts of proteinuria and elevated levels of plasma lipids (triglycerides and cholesterol). The immediate goal of the PI / applicant is to study in detail the mechanisms behind the development of hypertriglyceridemia in nephrotic syndrome. The PI's long term goal is to develop specific mechanism-based therapy for hyperlipidemia in nephrotic syndrome. The career development plan has been developed by the applicant, the primary mentor, and the two co-mentors to provide new and enhanced training in lipid biology, proteomic techniques, cell signaling, communication and presentation skills, grant and manuscript writing, and responsible conduct of research. There is a progressive increase in independence and greater involvement of the co-mentors in the later years of the grant. Timelines for each Specific Aim, allocation of independent laboratory space, periodic meetings of the applicant with the mentoring committee, expectations from the applicant and the specific role of each mentor are addressed in detail in the career development plan. In addition, the applicant is expected to write smaller foundation grants in the earlier years, and a R01 application in the last two years of the K Award. Research work currently being conducted by the PI has revealed an important role of Angiopoietin-like-4 (Angptl4) in the development of nephrotic syndrome in primary glomerular diseases like minimal change disease. Angptl4 is a secreted glycoprotein that is a known inhibitor of lipoprotein lipase and increased plasma levels of this protein result in the development of hypertriglyceridemia (a component of hyperlipidemia). Studies conducted by the PI reveal that increased secretion of this protein from the podocyte results in the development of proteinuria (Clement LC Nature Medicine 2011). In this proposal, the applicant will study the regulation of Angptl4 gene expression in the podocyte by glucocorticoids, and investigate the development of hypertriglyceridemia resulting from podocyte secretion of Angptl4 into the circulation in nephrotic syndrome. Hypothesis: The upregulation of podocyte Angptl4 expression in minimal change disease is reduced by treatment with glucocorticoids, and is mediated via binding of the glucocorticoid receptor to a negative glucocorticoid response element in the Angptl4 promoter. In primary glomerular disease, the sialylation of podocyte secreted Angptl4 influences its ability to leak into the circulation, inhibt lipoprotein lipase activity, and produce hypertriglyceridemia. Circulating Angptl4 is transported on the surface of HDL and inhibits endothelium bound lipoprotein lipase directly, and via its interaction with apolipoproteins C-II and C-III. In Specific Aim 1, the regulation of the Angptl4 promoter activity by glucocorticoids will be studied. In Specific Aim 2, the influence of sialylatin and other forms of posttranslational modification in the leakage of podocyte secreted Angptl4 into the circulation and the resulting development of hypertriglyceridemia will be investigated. In Specific Aim 3, putative interactions of Angptl4 with apolipoproteins C-II (activator of lipoprotei lipase) and C-III, (inhibitor of lipoprotein lipase) on the surface of HDL will be studied.

描述(申请人提供)：肾病综合征是肾衰竭的主要原因，患有这种疾病的患者会出现大量的蛋白尿和血浆脂类(甘油三酯和胆固醇)水平升高。PI/申请者的近期目标是详细研究肾病综合征中高甘油三酯血症的发生机制。PI的长期目标是开发针对肾病综合征高脂血症的特定机制疗法。职业发展计划由申请者、主要导师和两名共同导师制定，旨在提供新的和加强的培训，内容包括脂质生物学、蛋白质组技术、细胞信号、沟通和陈述技能、补助金和手稿写作以及负责任的研究指导。在赠款的最后几年，独立性逐步增强，共同导师的参与也越来越多。职业发展计划详细阐述了每个具体目标的时间表、独立实验室空间的分配、申请者与指导委员会的定期会议、申请者的期望以及每个导师的具体作用。此外，预计申请者将在前几年撰写较小的基金会赠款，并在K奖的最后两年提交R01申请。PI目前正在进行的研究揭示了血管生成素样蛋白4(ANGPTL4)在微小病变等原发性肾小球疾病中肾病综合征的发生发展中的重要作用。ANGPTL4是一种分泌型糖蛋白，是一种已知的脂蛋白脂酶抑制剂，这种蛋白的血浆水平增加会导致高甘油三酯血症(高脂血症的一个组成部分)。PI进行的研究表明，足细胞分泌这种蛋白质的增加会导致蛋白尿的发生(Clement LC Natural Medicine，2011)。在这项提案中，申请人将研究糖皮质激素对足细胞中ANGPTL4基因表达的调节，并研究肾病综合征患者足细胞分泌ANGPTL4进入循环所导致的高甘油三酯血症的发展。假设：在微小病变病中，足细胞ANGPTL4的表达上调被糖皮质激素治疗减少，并通过糖皮质激素受体与ANGPTL4启动子中的负糖皮质激素反应元件结合而介导。在原发性肾小球疾病中，足细胞分泌ANGPTL4的唾液酸化影响其渗入循环的能力，抑制脂蛋白脂酶活性，并产生高甘油三酯血症。循环中的ANGPTL4通过与载脂蛋白C-II和C-III相互作用，在高密度脂蛋白表面转运，直接抑制内皮脂蛋白脂酶活性。在具体目标1中，我们将研究糖皮质激素对ANGPTL4启动子活性的调节。在具体目标2中，将研究唾液酸苷和其他形式的翻译后修饰对足细胞分泌的ANGPTL4泄漏到循环中的影响以及由此导致的高甘油三酯血症的发展。在……里面具体目标3，研究ANGPTL4与高密度脂蛋白表面载脂蛋白C-II(脂蛋白脂酶激活剂)和C-III(脂蛋白脂酶抑制物)之间可能的相互作用。