NMR STUDIES OF CYTOSOLIC METAL IONS AND OXIDATIVE STRESS

细胞质金属离子和氧化应激的核磁共振研究

• 批准号: 6804635
• 负责人: Raj K Gupta
• 金额: $ 29.23万
• 依托单位: ALBERT EINSTEIN COLLEGE OF MEDICINE
• 依托单位国家: 美国
• 财政年份: 1982
• 资助国家: 美国
• 起止时间: 1982-05-01 至 2007-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6804635
• 关键词: NMR; STUDIES; CYTOSOLIC; METAL; IONS

DESCRIPTION (provided by applicant): Our long-range goal is to elucidate the role of intracellular mineral ions (Na+, K+, free Mg2+ & free Ca2+) and oxidative stress in the pathophysiology of essential hypertension and type 2 diabetes. We seek to understand how the regulation of intracellular concentrations of essential metal ions and membrane lipids goes astray in health disorders, especially hypertension and diabetes. Our main research tool is NMR spectroscopy. Our laboratory played a key role in the development of NMR methods for measuring various intracellular cations and we also have considerable expertise in the use of 1H NMR for analyzing membrane phospholipid composition and the degree of membrane fatty acid unsaturation (double bonds) and average chain length. Oxidative stress, which may play a contributory role in the pathogenesis of diabetes as well as hypertension, causes peroxidative degradation of membrane lipids resulting in a loss of fatty acid double bonds that can be quantitated by 1H NMR. The following specific aims will be pursued: (1) To investigate the mechanism of altered renal sodium homeostasis in salt-sensitive hypertension; (2) To demonstrate that oxidative stress, which results in overproduction of reactive oxygen species (ROS), can cause loss of unsaturation in fatty acyl chains of membrane phospholipids as measured by 'H NMR, and to test the hypothesis that peroxidative degradation of lipids as measured by loss of membrane fatty acid unsaturation during oxidative stress results in intracellular ionic changes similar to those seen in essential hypertension; (3) To investigate a possible protective role of magnesium against oxidative stress and whether there is a decrease in antioxidant capacity, as measured by glutathione (GSH) levels, in tissues exposed to low Mg environment; (4) To test the hypothesis that a deficit in membrane fatty acid unsaturation is associated with human essential hypertension and to investigate if there is an alteration in sphingomyelin-ceramide pathway in hypertension; (5) To find out if impairment of nitric oxide synthesis by inhibition of nitric oxide synthase, which causes hypertension in a normal rat, produces membrane lipid changes similar to those seen in essential hypertension; (6) To test the hypothesis that hyperglycemia causes peroxidative degradation,of membrane lipids as measured by 1H NMR, especially in vascular tissue, and, if so, whether hyperglycemia associated loss of fatty acid unsaturation and intracellular ionic alterations can be reversed by dietary antioxidants such as vitamin C and E; (7) To investigate increased vulnerability of hypertensive as well as hyperglycemic kidney and myocardium to ischemic damage and its relationship to increased perexidative degradation of membrane lipids; and (8) To design, develop and test a method for non-invasive measurement of "intracellular sodium using triple-quantum filtered (TQ)23 Na NMR. The proposed NMR investigations of intracellular ions and oxidative stress in hypertension and hyperglycemia condition may eventually lead to better strategies for the management of these health disorders.

描述（由申请人提供）：我们的长期目标是阐明细胞内矿物质离子（Na+、K+、游离Mg 2+和游离Ca 2+）和氧化应激在原发性高血压和2型糖尿病的病理生理学中的作用。我们试图了解细胞内必需金属离子和膜脂质浓度的调节如何在健康疾病，特别是高血压和糖尿病中误入歧途。我们的主要研究工具是核磁共振光谱。我们的实验室在开发用于测量各种细胞内阳离子的NMR方法方面发挥了关键作用，并且我们在使用1H NMR分析膜磷脂成分和膜脂肪酸不饱和度（双键）和平均链长方面也具有相当的专业知识。氧化应激可能在糖尿病和高血压的发病机制中起促进作用，引起膜脂质的过氧化降解，导致脂肪酸双键的损失，其可以通过1H NMR定量。本研究的主要目的是：（1）探讨盐敏感性高血压肾钠稳态改变的机制;（2）为了证明导致活性氧（ROS）过量产生的氧化应激可导致膜磷脂的脂肪酰基链中的不饱和度的损失，如通过1H NMR测量的，并检验这样的假设：通过氧化应激期间膜脂肪酸不饱和度的丧失来测量脂质的过氧化降解会导致与原发性高血压中观察到的类似的细胞内离子变化;（3）研究镁对氧化应激的保护作用，以及在低镁环境中，组织中谷胱甘肽（GSH）水平是否降低;（4）验证膜脂肪酸不饱和度降低与原发性高血压相关的假说，并探讨高血压时是否存在鞘磷脂-神经酰胺通路的改变;（5）为了发现通过抑制一氧化氮合酶而导致的一氧化氮合成的损伤（其在正常大鼠中引起高血压）是否产生类似于在原发性高血压中所见的膜脂质变化;（6）检验高血糖症引起膜脂质过氧化降解的假设，如通过1H NMR测量的，特别是在血管组织中，如果是这样，高血糖相关的脂肪酸不饱和度丧失和细胞内离子改变是否可以通过膳食抗氧化剂如维生素C和E逆转;（七）探讨高血压和高血糖时肾脏和心肌缺血损伤的易感性增加及其与膜过氧化降解增加的关系脂质;（8）设计、开发和测试一种使用三量子滤波（TQ）23 Na NMR无创测量细胞内钠的方法。高血压和高血糖状态下细胞内离子和氧化应激的拟议NMR调查可能最终导致更好的策略，这些健康疾病的管理。