首页> 外文期刊>Diabetic medicine: A journal of the British Diabetic Association >Incretin hormones, insulin, glucagon and advanced glycation end products in relation to cognitive function in older people with and without diabetes, a population‐based study
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Incretin hormones, insulin, glucagon and advanced glycation end products in relation to cognitive function in older people with and without diabetes, a population‐based study

机译:Incetin激素,胰岛素,胰高血糖素和先进的糖糖末端产品与老年人的认知功能有关,具有糖尿病,一种基于人口的研究

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Abstract Aim The aim of this observational study was to investigate relationships between physiological levels of glucometabolic biomarkers and cognitive test results in a population‐based setting. Methods Cross‐sectional data were obtained from the Swedish population‐based Malm? Diet and Cancer Study Re‐examination 2007–2012 comprising 3001 older people (mean age 72?years). Through oral glucose tolerance testing (OGTT), fasting and post‐load levels of serum insulin, plasma glucagon, serum glucose‐dependent insulinotropic peptide (GIP) and plasma glucagon‐like peptide‐1 (GLP‐1) were measured. Insulin resistance and insulin sensitivity levels were calculated. In 454 participants, advanced glycation end products (AGEs) were estimated through skin autofluorescence. Associations between biomarkers and two cognitive tests, the Mini‐Mental State Examination (MMSE) and A Quick Test of Cognitive Speed (AQT) respectively, were explored in multiple regression analyses. Results Positive associations following adjustments for known prognostic factors were found between MMSE scores and insulin sensitivity ( B ?=?0.822, P ?=?0.004), 2‐h plasma glucagon ( B ?=?0.596, P ?=?0.026), 2‐h serum GIP ( B ?=?0.581, P ?=?0.040) and 2‐h plasma GLP‐1 ( B ?=?0.585, P ?=?0.038), whereas negative associations were found between MMSE scores and insulin resistance ( B ?=??0.734, P ?=?0.006), fasting plasma GLP‐1 ( B ?=??0.544, P ?=?0.033) and AGEs ( B ?=??1.459, P ?=?0.030) were found. Conclusions Higher levels of insulin sensitivity, GIP and GLP‐1 were associated with better cognitive outcomes, but AGEs were associated with worse outcomes, supporting evidence from preclinical studies. Glucagon was linked to better outcomes, which could possibly reflect neuroprotective properties similar to the related biomarker GLP‐1 which has similar intracellular properties. Longitudinal and interventional studies are needed to further evaluate neuromodulating effects of these biomarkers. Abstract presented at the European Association for the Study of Diabetes (EASD) 2019, Barcelona, Spain
机译:摘要目的研究的目的是调查血糖素生物标志物的生理水平与基于人群的群体的认知测试之间的关系。方法从瑞典群体的麦芽获得横截面数据吗?饮食和癌症研究重新考试2007-2012包括3001名老年人(平均72岁?年)。通过口服葡萄糖耐量测试(OGTT),测量血清胰岛素,血浆胰高血糖素,血清血清血清胰岛素肽(GIP)和血浆胰糖型肽-1(GLP-1)的禁食和后载水平。计算胰岛素抵抗和胰岛素敏感水平。在454名参与者中,通过皮肤自发荧光估算高级糖化末端产品(年龄)。在多元回归分析中探讨了生物标志物和两种认知测试,迷你精神状态检查(MMSE)和认知速度(AQT)的快速测试的关联。结果在MMSE评分和胰岛素敏感度之间发现了已知预后因子的调整后的阳性关联(B?= 0.822,P?= 0.004),2-H血浆胰高血糖素(B?= 0.596,P?= 0.026), 2-H血清吉普(B?= 0.581,p?= 0.040)和2-H等离子体GLP-1(B?= 0.585,P?= 0.038),而在MMSE评分和胰岛素之间发现负联想阻力(b?=Δ?0.734,p?= 0.006),禁食等离子体glp-1(b?= 0.544,p?= 0.033)和年龄(b?= ?? 1.459,p?= 0.030 ) 被找到。结论胰岛素敏感性水平较高,GIP和GLP-1与更好的认知结果相关,但随着较差的结果,患有较差的结果,支持临床前研究的证据。胰高血糖素与更好的结果相关联,这可能反映与具有相似细胞内性质的相关生物标志物GLP-1类似的神经保护性能。需要纵向和介入研究,以进一步评估这些生物标志物的神经调节作用。摘要在欧洲糖尿病(Easd)2019年,巴塞罗那,西班牙研究

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