年龄和肥胖对血小板淀粉样前体蛋白加工以及氧化应激和炎症的血浆标志物的影响。

The effect of age and obesity on platelet amyloid precursor protein processing and plasma markers of oxidative stress and inflammation.

机构信息

School of Sport, Exercise and Rehabilitation Sciences, College of Life and Environmental Sciences, University of Birmingham, UK.

出版信息

Exp Gerontol. 2020 Apr;132:110838. doi: 10.1016/j.exger.2020.110838. Epub 2020 Jan 22.

DOI:10.1016/j.exger.2020.110838

PMID:31981682

Abstract

INTRODUCTION

Advancing age is a major risk factor for a range of diseases such as, cardiovascular disease, diabetes, cancer and neurodegenerative diseases. In addition, over a third of the population are overweight and obesity is becoming more prevalent in younger people. Ageing and obesity are both linked to a chronic proinflammatory state and elevated oxidative stress, which have both been implicated in cardiovascular and neurodegenerative diseases. Platelets contain all the necessary machinery to process the Amyloid precursor protein AβPP, a pathway thought to be perturbed in Alzheimer's Disease (AD). The ratio of AβPP isoforms present in platelets, and the amount of alpha secretase ADAM10, that works to process AβPP, appear to be associated with cognitive decline and a diagnosis of Alzheimer's disease. The aim of this study was to assess changes in AβPP ratio, ADAM10 and markers of inflammation and oxidative stress with ageing and obesity.

MATERIALS AND METHODS

Ninety participants were recruited to this study to provide one blood sample. Platelet-rich plasma and platelet lysates were collected and the expression of AβPPr, proADAM10 and mADAM10 was assessed by Western blotting. In addition, markers of inflammation (IL-6) and oxidative stress (8-Isoprostane) were assessed in plasma.

RESULTS

Participants were placed into one of four groups based on their age and body mass index (Young/Lean, Young/obese, Old/Lean and Old/Obese). IL-6 was able to significantly distinguish obese from lean participants (AUC of 0.80, SE = 0.05, P < 0.001). Plasma isoprostanes were able to distinguish between both young/old (AUC of 0.73, SE = 0.05, P < 0.01), and obese/non-obese participants (AUC of 0.66, SE = 0.01, P < 0.01). Plasma protein carbonyls could distinguish young and old participants (AUC of 0.69, SE = 0.07 P < 0.02). Old Lean participants had significantly lower mADAM10 expression than both Young Lean and Young Obese participants (p < 0.05). Old obese participants had significantly lower proADAM10 expression compared to both Young Lean and Young Obese (p < 0.05). Both mADAM10 and proADAM10 were significantly decreased with advancing age (p < 0.05).

CONCLUSIONS

The findings presented in this study provide evidence that blood-based biomarkers related to the pathology of AD are altered with age and obesity in otherwise healthy adults. Ageing was more strongly associated with elevated markers of oxidative stress whereas obesity was associated with elevated inflammatory IL-6.

摘要

简介

随着年龄的增长，一系列疾病的风险因素也随之增加，如心血管疾病、糖尿病、癌症和神经退行性疾病。此外，超过三分之一的人口超重，肥胖在年轻人中也越来越普遍。衰老和肥胖都与慢性炎症状态和氧化应激升高有关，这两者都与心血管和神经退行性疾病有关。血小板包含加工淀粉样前体蛋白 AβPP 的所有必要机制，这一途径被认为在阿尔茨海默病（AD）中受到干扰。血小板中存在的 AβPP 同工型的比例，以及发挥加工 AβPP 作用的 α 分泌酶 ADAM10 的数量，似乎与认知能力下降和阿尔茨海默病的诊断有关。本研究的目的是评估随着年龄和肥胖的变化，AβPP 比值、ADAM10 以及炎症和氧化应激标志物的变化。

材料和方法

本研究招募了 90 名参与者提供一份血样。收集富含血小板的血浆和血小板裂解物，并通过 Western 印迹法评估 AβPPr、proADAM10 和 mADAM10 的表达。此外，还评估了血浆中的炎症标志物（IL-6）和氧化应激标志物（8-异前列腺素）。

结果

根据年龄和体重指数（年轻/瘦、年轻/肥胖、年老/瘦和年老/肥胖），将参与者分为四组之一。IL-6 能够显著区分肥胖和瘦的参与者（AUC 为 0.80，SE=0.05，P<0.001）。血浆异前列腺素能够区分年轻/年老（AUC 为 0.73，SE=0.05，P<0.01）和肥胖/非肥胖参与者（AUC 为 0.66，SE=0.01，P<0.01）。血浆蛋白羰基能够区分年轻和年老的参与者（AUC 为 0.69，SE=0.07，P<0.02）。与年轻的瘦和肥胖的参与者相比，年老的瘦参与者的 mADAM10 表达显著降低（p<0.05）。与年轻的瘦和肥胖的参与者相比，年老的肥胖参与者的 proADAM10 表达显著降低（p<0.05）。mADAM10 和 proADAM10 都随着年龄的增长而显著下降（p<0.05）。