有晚发性阿尔茨海默病家族史的后代的血管因素与炎症标志物

Vascular factors and markers of inflammation in offspring with a parental history of late-onset Alzheimer disease.

作者信息

van Exel Eric, Eikelenboom Piet, Comijs Hannie, Frölich Marijke, Smit Johannes H, Stek Max L, Scheltens Philip, Eefsting Jan E, Westendorp Rudi G J

机构信息

Department of Psychiatry, VU University Medical Center/GGZ-inGeest, Osdorpplein 880, 1068 TD, Amsterdam, the Netherlands.

出版信息

Arch Gen Psychiatry. 2009 Nov;66(11):1263-70. doi: 10.1001/archgenpsychiatry.2009.146.

DOI:10.1001/archgenpsychiatry.2009.146

PMID:19884614

Abstract

CONTEXT

Alzheimer disease (AD) is a complex disorder with a strong heritable component. Amyloid pathology, vascular factors, and inflammation are postulated to be involved in its pathogenesis, but causality has not been established unequivocally.

OBJECTIVE

To identify heritable traits in middle age that contribute to AD.

DESIGN

We used a proven family design, comparing middle-aged offspring with and without a parental history of AD. In such a design, the offspring under study are enriched for risk factors of AD but do not yet have the disease.

SETTING

The Netherlands.

PARTICIPANTS

Two hundred six offspring of 92 families with a parental history of late-onset AD and 200 offspring of 97 families without a parental history of AD.

MAIN OUTCOME MEASURES

The APOE epsilon4 genotype, vascular factors, production capacity of pro- and anti-inflammatory cytokines upon stimulation with lipopolysaccharide, and circulating markers of inflammation. All outcome measures were assessed in the offspring only and not in the parental generation.

RESULTS

More offspring with a parental history of AD carried APOE epsilon4 than those without a parental history of the disease (47% vs 21%, P < .001). Those with a parental history of AD also had higher systolic blood pressures (P = .006), higher diastolic blood pressures (P < .001), and lower ankle brachial indices (P = .005) when compared with offspring without a family history of dementia. Production capacity of pro-inflammatory cytokines in offspring with a parental history of AD was also different, with higher levels of IL-1beta (interleukin 1beta) (P < .001), IL-1beta to IL-1ra ratio (P < .001), tumor necrosis factor alpha (P = .008), IL-6 (P = .04), and interferon gamma (P = .01). All of these positive associations were independent of APOE epsilon4 genotype.

CONCLUSIONS

Hypertension and the expression of an innate pro-inflammatory cytokine profile in middle age are early risk factors of AD in old age. For the offspring of affected families, it provides clues for screening and preventive strategies, of which blood pressure control can be implemented directly.

摘要

背景

阿尔茨海默病（AD）是一种具有很强遗传成分的复杂疾病。淀粉样蛋白病理、血管因素和炎症被认为与发病机制有关，但因果关系尚未明确确立。

目的

确定中年时有助于患AD的遗传特征。

设计

我们采用了一种经过验证的家族设计，比较有和没有AD家族史的中年后代。在这种设计中，所研究的后代富含AD危险因素，但尚未患病。

地点

荷兰。

参与者

92个有晚发性AD家族史的家庭的206名后代和97个无AD家族史的家庭的200名后代。

主要观察指标

APOE ε4基因型、血管因素、脂多糖刺激后促炎和抗炎细胞因子的产生能力以及循环炎症标志物。所有观察指标仅在后代中评估，不在亲代中评估。

结果

有AD家族史的后代携带APOE ε4的比例高于无该疾病家族史的后代（47%对21%，P<.001）。与无痴呆家族史的后代相比，有AD家族史的后代收缩压更高（P=.006）、舒张压更高（P<.001）且踝臂指数更低（P=.005）。有AD家族史的后代促炎细胞因子的产生能力也不同，白细胞介素1β（IL-1β）（P<.001）、IL-1β与IL-1受体拮抗剂的比值（P<.001）、肿瘤坏死因子α（P=.008）、IL-6（P=.04）和干扰素γ（P=.01）水平更高。所有这些正相关均独立于APOE ε4基因型。