Buck Institute for Research on Aging, Novato, California, United States of America.
Biofortis, Mérieux NutriSciences, Addison, Illinois, United States of America.
PLoS One. 2024 Sep 18;19(9):e0307951. doi: 10.1371/journal.pone.0307951. eCollection 2024.
Frailty is a geriatric syndrome characterized by chronic inflammation and metabolic insufficiency that creates vulnerability to poor outcomes with aging. We hypothesize that interventions which target common underlying mechanism of aging could ameliorate frailty. Ketone bodies are metabolites produced during fasting or on a ketogenic diet that have pleiotropic effects on inflammatory and metabolic aging pathways in laboratory animal models. Ketone esters (KEs) are compounds that induce ketosis without dietary changes, but KEs have not been studied in an older adult population. Our long-term goal is to examine if KEs modulate aging biology mechanisms and clinical outcomes relevant to frailty in older adults.
The primary objective of this randomized, placebo-controlled, double-blinded, parallel-group, pilot trial is to determine tolerability of 12-weeks of KE ingestion in a broad population of older adults (≥ 65 years). Secondary outcomes include safety and acute blood ketone kinetics. Exploratory outcomes include physical function, cognitive function, quality of life, aging biomarkers and inflammatory measures.
Community-dwelling adults who are independent in activities of daily living, with no unstable acute medical conditions (n = 30) will be recruited. The study intervention is a KE or a taste, appearance, and calorie matched placebo beverage. Initially, acute 4-hour ketone kinetics after 12.5g or 25g of KE consumption will be assessed. After collection of baseline safety, functional, and biological measurements, subjects will randomly be allocated to consume KE 25g or placebo once daily for 12-weeks. Questionnaires will assess tolerability daily for 2-weeks, and then via phone interview at bi-monthly intervals. Safety assessments will be repeated at week 4. All measures will be repeated at week 12.
This study will evaluate feasibility, tolerability, and safety of KE consumption in older adults and provide exploratory data across a range of aging-related endpoints. This data will inform design of larger trials to rigorously test KE effects on aging mechanisms and clinical outcomes relevant to frailty.
衰弱是一种老年综合征,其特征是慢性炎症和代谢不足,使老年人易发生不良后果。我们假设针对衰老的共同潜在机制的干预措施可以改善衰弱。酮体是在禁食或生酮饮食期间产生的代谢物,对实验室动物模型中的炎症和代谢衰老途径具有多效性。酮酯(KEs)是一种在不改变饮食的情况下诱导酮症的化合物,但尚未在老年人群中进行研究。我们的长期目标是研究 KEs 是否调节与老年人衰弱相关的衰老生物学机制和临床结局。
这项随机、安慰剂对照、双盲、平行组、初步试验的主要目的是确定在广泛的老年人群(≥65 岁)中,12 周 KE 摄入的耐受性。次要结局包括安全性和急性血液酮动力学。探索性结局包括身体功能、认知功能、生活质量、衰老生物标志物和炎症指标。
将招募生活在社区、日常生活活动独立、无不稳定急性医疗状况的成年人(n=30)。研究干预措施是 KE 或味道、外观和热量匹配的安慰剂饮料。最初,将评估 12.5g 或 25g KE 消耗后 4 小时的急性酮动力学。在收集基线安全性、功能和生物学测量值后,受试者将随机分配每天服用 KE 25g 或安慰剂,持续 12 周。耐受性将在第 2 周每天通过问卷评估,然后在每两个月通过电话访谈评估。第 4 周将重复安全性评估。所有测量值将在第 12 周重复。
本研究将评估 KE 在老年人中的摄入的可行性、耐受性和安全性,并提供一系列与衰老相关终点的探索性数据。这些数据将为设计更大规模的试验提供信息,以严格测试 KE 对与衰弱相关的衰老机制和临床结局的影响。
