Group of Cellular Oncology, Biodonostia Health Research Institute, San Sebastian, Spain.
CIBER of Frailty and Healthy Aging (CIBERfes), Spain.
Aging (Albany NY). 2020 May 27;12(10):9982-9999. doi: 10.18632/aging.103295.
Frailty represents a state of vulnerability and increases the risk of negative health outcomes, which is becoming an important public health problem. Over recent years, multiple independent studies have attempted to identify biomarkers that can predict, diagnose, and monitor frailty at the biological level. Among them, several promising candidates have been associated with frailty status including antioxidants and free radicals, and also inflammatory response biomarkers. In this review, we will summarize the more recent advances in this field. Moreover, the identification of scales and measurements to detect and quantify frailty in aged mice, as well as the generation of mouse models, have started to unravel the underlying biological and molecular mechanisms of frailty. We will discuss them here with an emphasis on murine models with overexpression of glucose-6-phosphate dehydrogenase and loss of function of superoxide dismutase and interleukin 10, which reveal that altered oxidative stress and inflammation pathways are involved in the physiopathology of frailty. In summary, we provide the current available evidence, from both human cohorts and experimental animal models, that highlights oxidative damage and inflammation as relevant biomarkers and drivers of frailty.
衰弱代表一种脆弱状态,并增加负面健康结果的风险,这正在成为一个重要的公共卫生问题。近年来,多项独立研究试图确定可在生物学水平上预测、诊断和监测衰弱的生物标志物。其中,一些有前途的候选标志物与衰弱状态相关,包括抗氧化剂和自由基,以及炎症反应生物标志物。在这篇综述中,我们将总结该领域的最新进展。此外,识别用于检测和量化老年小鼠衰弱的量表和测量方法,以及生成小鼠模型,已开始揭示衰弱的潜在生物学和分子机制。我们将在这里讨论它们,重点是葡萄糖-6-磷酸脱氢酶过表达和超氧化物歧化酶和白细胞介素 10 功能丧失的小鼠模型,这些模型表明,氧化应激和炎症途径的改变与衰弱的病理生理学有关。总之,我们提供了来自人类队列和实验动物模型的现有证据,强调氧化损伤和炎症是与衰弱相关的生物标志物和驱动因素。
