HIV SYNDROME X & PROTEASE INHIBITORS: HUMAN STUDIES

艾滋病毒X综合症

• 批准号: 6390919
• 负责人: GERALD M. REAVEN
• 金额: $ 49.97万
• 依托单位: STANFORD UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2000
• 资助国家: 美国
• 起止时间: 2000-09-01 至 2005-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6390919
• 关键词: AIDS; HIV infections; adipose tissue; clinical research; coronary disorder; glucose tolerance; hepatitis C virus; human subject; hyperinsulinism; insulin sensitivity /resistance; nonblood lipoprotein; noninsulin dependent diabetes mellitus; protease inhibitor

This proposal is based on the premise that insulin action varies widely in patients with HIV/AIDS, and that the untoward effects of protease inhibitors (Pis) occur in individuals with pre- existing insulin resistance. It is also postulated that type 2 diabetes, is more likely to develop in patients co-infected with hepatitis-C virus (HCV). To test these hypotheses we will determine glucose tolerance, lipoprotein, insulin action on muscle and adipose tissue, insulin secretory function, and plasma concentration of soluble cellular adhesion molecules in 150 individuals, 125 patients with HIV/AIDS (50 percent co-infected with HCV) in whom treatment with Pis is soon to be initiated, and 25 subjects with HCV only. The results of these studies will: 1) define the pre-treatment variation in insulin action and secretion in these patients; 2) test the hypothesis that pre- existing insulin resistance and hyperinsulinemia determines prevalence of risk factors for type 2 diabetes and coronary heart disease (CHD): and 3) compare risk factors for CHD and type 2 diabetes in HCV-positive and HCV-negative patients with HIV/AIDS. All baseline measurements will be repeated three months after treatment with Pis. These data will provide a prospective assessment of the effect of Pis on relevant variables, as well testing the hypotheses that: 1) the more insulin resistant and hyperinsulinemic an individual at baseline, the greater the untoward impact of PI: 2) the lipolytic effect of Pis results in day-long elevations in plasma FFA concentrations, that correlate closely with the decrease in insulin action and dyslipedemia in PI-treated patients; and 3) the increase in risk factors for type 2 diabetes will be accentuated in patients co-infected with HCV. Patients with HIV/AIDS will then be studied to see if replacing saturated fat (SF) with monounsaturated (MF)/polyunsaturated (PF), rather than carbohydrate (CHO), is more likely to maximally attenaute the abnormalities in PI-treated patients secondary to insulin resistance and hyperinsulinemia and lower LDL-cholesterol concentration. Specifically, patients will be studied after two randomly assigned dietary periods of four weeks (divided by a two-week washout period), consuming diets containing (as percent of calories) either 15 percent protein. 55 percent CHO and 30 percent fat, or, 15 percent, 40 percent CHO and 45 percent fat. SF will be less than 10 percent of calories in both diets, and the MF/PF ratio kept constant. Measurements will be made of fasting and postprandial plasma glucose, insulin, FFA, triglyceride, and lipoprotein at hourly intervals from 8 AM to 4 PM. It is postulated that all CHD risk factors will be accentuated on the 55 percent CHO diet. The results of these studies will help explain why untoward metabolic and clinical events occur with PI treatment, and define the diet most likely to decrease risk of type 2 diabetes and CHD in these patients.

该建议基于以下前提：胰岛素作用在HIV/AIDS患者中变化很大，蛋白酶抑制剂（PI）的不良反应发生在预先存在胰岛素抵抗的个体中。 也有人推测，2型糖尿病更可能在合并感染丙型肝炎病毒（HCV）的患者中发展。 为了检验这些假设，我们将确定葡萄糖耐量，脂蛋白，胰岛素对肌肉和脂肪组织的作用，胰岛素分泌功能，血浆中可溶性细胞粘附分子的浓度在150个人，125例HIV/AIDS患者（50%合并感染HCV），其中Pis治疗即将开始，和25名受试者与HCV。 这些研究的结果将：1）确定这些患者中胰岛素作用和分泌的治疗前变化; 2）检验预先存在的胰岛素抵抗和高胰岛素血症决定2型糖尿病和冠心病（CHD）风险因素的患病率的假设;和3）比较HCV阳性和HCV阴性HIV/AIDS患者中CHD和2型糖尿病的风险因素。所有基线测量将在PI治疗后3个月重复进行。 这些数据将提供Pis对相关变量影响的前瞻性评估，以及检验以下假设：1）基线时个体的胰岛素抵抗和高胰岛素血症越严重，PI的不良影响越大：2）Pis的脂解作用导致血浆FFA浓度全天升高，这与PI治疗患者的胰岛素作用降低和血脂异常密切相关;和3）在合并感染HCV的患者中，2型糖尿病的危险因素的增加将加重。然后将对HIV/AIDS患者进行研究，以观察用单不饱和（MF）/多不饱和（PF）替代饱和脂肪（SF）而不是碳水化合物（CHO）是否更可能最大限度地减轻PI治疗患者继发于胰岛素抵抗和高胰岛素血症以及LDL-胆固醇浓度降低的异常。 具体来说，患者将在两个随机分配的为期四周的饮食期（除以两周的洗脱期）后进行研究，饮食中含有（以卡路里百分比计）15%的蛋白质。 55%的CHO和30%的脂肪，或者，15%，40%的CHO和45%的脂肪。在两种饮食中，SF将低于10%的热量，MF/PF比率保持不变。 从上午8点到下午4点，每小时测量一次空腹和餐后血糖、胰岛素、游离脂肪酸、甘油三酯和脂蛋白。 据推测，55%的CHO饮食会加重所有CHD风险因素。这些研究的结果将有助于解释为什么PI治疗会发生不良代谢和临床事件，并确定最有可能降低这些患者2型糖尿病和CHD风险的饮食。