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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >Insulin metabolism and the risk of Alzheimer disease: the Rotterdam Study.
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Insulin metabolism and the risk of Alzheimer disease: the Rotterdam Study.

机译:胰岛素代谢和老年痴呆症的风险疾病:鹿特丹学习。

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OBJECTIVE: Diabetes mellitus has been associated with an increased risk of Alzheimer disease (AD), but how it exerts its effect remains controversial. Possible pathophysiologic mechanisms are glucose toxicity and a direct effect of insulin on amyloid metabolism. Most studies had short follow-up, and longer-term effects of diabetes on AD risk are unknown. We investigated whether fasting glucose and insulin levels and insulin resistance are associated with the risk of AD and whether this risk is constant over time. METHODS: The study was based on 3,139 participants of the Rotterdam Study, a population-based cohort study. All subjects were free from dementia, did not have a history of diabetes, and had fasting levels of glucose and insulin measured at baseline. Insulin resistance was estimated with the homeostasis model assessment. We investigated how fasting glucose, insulin, and insulin resistance are related to the risk of AD in 3 different strata according to time-to-event, using Cox proportional hazards models. RESULTS: During follow-up, 211 participants developed AD, 71 of them within 3 years of baseline. Levels of insulin and insulin resistance were associated with a higher risk of AD within 3 years of baseline. After 3 years, the risk was no longer increased. Glucose was not associated with a higher risk of AD. There was no interaction of APOE epsilon4 carriership and insulin metabolism on the risk of AD. CONCLUSIONS: Our findings suggest that insulin metabolism influences the clinical manifestation of AD only within 3 years.
机译:目的:糖尿病有关与阿尔茨海默病(AD)的风险增加但它如何发挥其效应依然存在有争议的。机制是葡萄糖毒性和直接胰岛素对淀粉样蛋白代谢的影响。研究短期随访和长期糖尿病对广告的影响是未知的风险。调查是否空腹血糖和胰岛素水平和胰岛素抵抗相关广告的风险,这种风险是否常数随着时间的推移。鹿特丹研究的参与者以人群为基础的队列研究。无痴呆,没有的历史糖尿病、空腹血糖水平和胰岛素在基线测量。估计与稳态模型评估。胰岛素和胰岛素抵抗相关广告在3种不同地层的风险比较,使用Cox比例风险模型。参与者发达的广告,其中有71在3年的基线。阻力是伴随着更高的风险广告在3年内的基线。不再增加风险。广告的风险更高。交互的APOE epsilon4 carriership和胰岛素代谢风险的广告。结论:我们的研究表明,胰岛素代谢影响的临床表现广告只在3年。

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