Nicotinamide riboside supplementation for treating elevated systolic blood pressure and arterial stiffness in middle-aged and older adults

补充烟酰胺核苷治疗中老年人收缩压升高和动脉僵硬度

• 批准号: 10085334
• 负责人: DOUGLAS R SEALS
• 金额: $ 15.35万
• 依托单位: UNIVERSITY OF COLORADO
• 依托单位国家: 美国
• 财政年份: 2019
• 资助国家: 美国
• 起止时间: 2019-02-01 至 2023-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/10085334
• 关键词: Adherence; Adult; Aftercare; Age; Age-Years; Aging; Antihypertensive Agents; Aorta; Arteries; Automobile Driving; Biological Availability; Biomedical Research; Blood Pressure; Caloric Restriction; Cardiovascular Diseases; Carotid Arteries; Cessation of life; Chronic; Chronic Disease; Chronic Kidney Failure; Clinic; Clinical; Clinical Trials; Cognitive; Collagen; Dementia; Deposition; Diet; Disease; Double-Blind Method; Elderly; Evidence based intervention; Future; Gold; Guidelines; Heart Diseases; Hour; Human; Hypertension; Impaired cognition; Individual; Inflammation; Intervention; Life Style; Link; Measures; Mediating; Mus; Muscle Tonus; Obesity; Oral; Organ; Overweight; Oxidative Stress; Peripheral Blood Mononuclear Cell; Pharmaceutical Preparations; Pharmacology; Phase; Physiologic pulse; Pilot Projects; Placebos; Prevalence; Randomized; Regimen; Research Priority; Rest; Risk; Risk Factors; Safety; Site; Skeletal Muscle; Smooth Muscle; Stroke; Structure; Subgroup; Supplementation; Translating; Update; Vascular Smooth Muscle; Vasoconstrictor Agents; Woman; age related; aged; arterial stiffness; base; bone mass; capsule; cardiovascular disorder risk; cardiovascular risk factor; circulating biomarkers; comorbidity; demographics; disorder risk; effective intervention; evidence base; healthy lifestyle; men; middle age; mimetics; modifiable risk; muscle form; nicotinamide riboside supplementation; nicotinamide-beta-riboside; novel; older men; older women; oral supplementation; primary outcome; reduced muscle mass; secondary outcome; standard measure; vasoconstriction

Project Summary More than 90% of cardiovascular diseases (CVD) and cognitive impairment/dementia occur in men and women >50 years of age. Changes in age demographics in the U.S. predict progressive increases in these disorders without effective, evidence-based interventions. The age-related increase in systolic blood pressure (SBP) is a major factor driving the increased risk of these disorders in later middle-aged and older (MA/O) adults. This increase in SBP is due primarily to stiffening of the large elastic arteries, as indicated by increased carotid-femoral pulse wave velocity (CFPWV), which reflects stiffening of the aorta. Aortic stiffening with aging is mediated by structural and functional (increased vascular smooth muscle tone) changes in the arterial wall stimulated by oxidative stress and chronic low-grade inflammation. New BP guidelines describe a casual (resting) SBP of 120-129 mmHg as “elevated” and SBP of 130-139 mmHg as “stage 1 hypertension”, as these levels account for much of the increased risk of CVD and other BP-influenced disorders of aging. Importantly, ~50% of adults age >50 have SBP within these ranges. The first-line treatment for lowering SBP in these ranges is lifestyle-based therapy. In this context, we have shown that caloric restriction (CR) reduces SBP and CFPWV in older mice and in overweight/obese MA/O humans, but adherence is poor and CR reduces muscle and bone mass. As a result, we have since shown that boosting NAD+ bioavailability to stimulate SIRT-1, a “CR mimetic” approach, reduces CFPWV and oxidative stress in old mice, and we recently took the first step in translating these findings in a small pilot study of MA/O adults (n=24). We found that supplementation with nicotinamide riboside, a natural, commercially available precursor of NAD+ and novel CR mimetic, was well-tolerated and increased NAD+ bioavailability in the overall group, and reduced SBP (-8 mmHg) and CFPWV in a subgroup (n=13) with baseline SBP of 120-139 mmHg. Here we propose a randomized, placebo controlled, double-blind, single-site phase IIa clinical trial to assess the safety and efficacy of oral nicotinamide riboside (500 mg capsules 2x/day; NIAGEN®; ChromaDex Inc.) for 3 months vs. placebo (n=59/group) for decreasing SBP and aortic stiffness in MA/O men and women (50-79 years) with SBP in the elevated/stage 1 hypertension (120-139 mmHg) range. We hypothesize that treatment will be safe and well-tolerated, and will reduce SBP and CFPWV, as related to increases in systemic NAD+ bioavailability and reductions in vasoconstrictor factors, oxidative stress and inflammation. Aim 1: To measure casual SBP (primary outcome) before/after nicotinamide riboside vs. placebo treatment; Aim 2: To measure 24-hour ambulatory SBP and CFPWV (secondary outcomes) before and after treatment; Aim 3: To determine the safety and tolerability of treatment with nicotinamide riboside vs. placebo; Aim 4: To measure systemic NAD+ and NAD+–related metabolite concentrations, as well as circulating markers of vasoconstriction factors, oxidative stress and inflammation before and after treatment.

项目摘要 90%以上的心血管疾病(CVD)和认知障碍/痴呆发生在男性和 女性&>50岁。美国年龄结构的变化预测这些人会逐渐增加 在没有有效的循证干预措施的情况下，更容易导致精神障碍。与年龄相关的收缩期血液增加 压力(SBP)是导致中老年人罹患这些疾病风险增加的主要因素 (MA/O)成人。SBP的增加主要是由于大的弹性动脉僵硬，如下图所示 颈动脉-股动脉脉搏波速度(CFPWV)增加，反映主动脉硬化。主动脉 结构和功能(血管平滑肌张力增加)是由衰老引起的僵硬。 氧化应激和慢性低度炎症刺激的动脉壁改变。 新的BP指南将临时(静息)SBP为120-129毫米汞柱，SBP为130-139 MmHg1级高血压，因为这些水平是心血管疾病和其他疾病风险增加的主要原因 血压影响的衰老障碍。重要的是，约50%的50岁成年人的SBP在这些范围内。这个 在这些范围内降低SBP的一线治疗是基于生活方式的治疗。在这方面，我们已经表明 卡路里限制(CR)降低了老年小鼠和超重/肥胖MA/O人类的SBP和CFPWV， 但粘附性差，CR会减少肌肉和骨量。因此，我们已经证明了 提高NAD+的生物利用度以刺激SIRT-1，一种“CR模拟”方法，降低CFPWV和氧化 老年小鼠的压力，我们最近在MA/O的一项小型先导性研究中翻译了这些发现 成人(n=24)。我们发现，补充烟酰胺核苷，一种天然的，商业上可以获得的 NAD+前体和新型CR模拟物耐受性良好，总体上提高了NAD+的生物利用度 组，降低SBP(-8 mm Hg)和CFPWV(n=13)，基础SBP为120-139 mm Hg。 在这里，我们提出了一项随机、安慰剂对照、双盲、单部位IIa期临床试验 评估口服烟酰胺核苷(500毫克胶囊，每天2次；NIAGEN®；ChromaDex)的安全性和有效性 Inc.)持续3个月与安慰剂(n=59/组)相比，降低MA/O男性和女性的SBP和主动脉僵硬 (50-79岁)SBP升高/1期高血压(120-139毫米汞柱)。我们假设 治疗将是安全和耐受性良好的，并将降低SBP和CFPWV，这与系统性高血压的增加有关。 NAD+生物利用度和血管收缩因子、氧化应激和炎症的减少。 目的1：测量烟酰胺核苷与安慰剂治疗前/后的随机SBP(主要结果)； 目的：测定治疗前后24小时动态SBP和CFPWV(二次结局)； 目的3：比较烟酰胺核苷与安慰剂治疗的安全性和耐受性； 目的4：测量全身NAD+和NAD+相关代谢物浓度以及循环 治疗前后血管收缩因子、氧化应激和炎症的标志物。