Inflammation, long-term diabetes characteristics, and cognitive decline

炎症、长期糖尿病特征和认知能力下降

• 批准号: 8409860
• 负责人: Michal Schnaider Beeri
• 金额: $ 7.83万
• 依托单位: ICAHN SCHOOL OF MEDICINE AT MOUNT SINAI
• 依托单位国家: 美国
• 财政年份: 2009
• 资助国家: 美国
• 起止时间: 2009-09-15 至 2014-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8409860
• 关键词: Affect; Age; Alleles; Alzheimer' s Disease; Area; Brain; Caring; Cessation of life; Characteristics; Charge; Client; Clinical; Clinical assessments; Cognition; Cognitive; Collaborations; Community Health; Comorbidity; Complex; Consensus; DNA; Data; Data Set; Databases; Dementia; Development; Diabetes Mellitus; Diagnosis; Diagnostic; Diagnostic Procedure; Encephalitis; Ensure; Functional disorder; Funding; Future; General Population; Glucose; Glycosylated hemoglobin A; Goals; Haptoglobins; Health; Health Services; Healthcare; Hippocampus (Brain); Hypertension; Impaired cognition; Individual; Inflammation; Inflammatory; Interleukin-6; Intervention; Intervention Studies; Israel; Laboratories; Lead; Lesion; Life; Link; Longitudinal Studies; Magnetic Resonance Imaging; Measurement; Medical; Medical Records; Medical center; Metformin; Neurologist; Non-Insulin-Dependent Diabetes Mellitus; Notification; Outcome; Patients; Pharmaceutical Preparations; Pharmacy facility; Physicians; Population; Population Study; Preventive; Process; Psychiatrist; Psychiatry; Public Health; Registries; Reporting; Research; Resources; Risk; Risk Factors; Role; Sampling; Structure; Superior temporal gyrus; Teleconferences; Time; Translating; aged; base; cardiovascular risk factor; clinically relevant; cohort; computerized; data sharing; diabetic; diabetic patient; entorhinal cortex; glycemic control; high risk; human old age (65+); illness length; inflammatory marker; insulin sensitizing drugs; medical schools; middle age; modifiable risk; neuropsychological; palliative; prospective; symposium; white matter

DESCRIPTION (provided by applicant): This prospective 5-year study will examine how long-term type 2 diabetes characteristics and inflammation affect the development of cognitive decline in a cohort of 1000 cognitively intact (at recruitment) diabetic individuals 65 years and older living in Tel-Aviv, Israel. This study is a collaboration of the Department of Psychiatry at the Mount Sinai School of Medicine (MSSM), NY, the Department of Psychiatry at the Sheba Medical Center, Israel, and the Department of Community Health of the Maccabi Health Services (MHS), the second largest HMO in Israel. It provides health care to a representative cross section of 1.7 million Israeli citizens, 11,000 of whom have diabetes and are above the age of 65 in the area of Tel-Aviv. The benefits of studying this population are: a) up to 10 years of data from the extraordinarily rich MHS Diabetes Registry, including HbA1c, anti-diabetic and other medication, duration of disease, hypertension and other diabetes related characteristics; b) fully computerized centrally processed MHS medical records, facilitating data access and analysis; c) no charge to patients for analyses by the MHS centralized laboratory, ensuring complete use; d) significantly subsidized medication from MHS pharmacies, which record every purchase (in contrast to subject report of medication prescribed); e) minimal loss to contact since ill subjects are cared for by MHS; and f) prompt death notification by ending of client funding. The dementia diagnostic procedures at Sheba will be fully integrated with those of the MSSM Alzheimer's Disease Research Center (ADRC). Subjects will be followed at 18-month intervals. Diagnostic consensus teleconferences including both Israeli and ADRC physicians will have clinical, neuropsychological, and MRI data collected by this project in addition to complete MHS laboratory and medical data. DNA will be collected and a data sharing plan is in place. The specific aims are to investigate the impact of baseline 1) inflammation, 2) poor long-term glycemic control, 3) diabetes medication, specifically metformin, and 4) MRI abnormalities, on the rate of cognitive decline. Additionally, the contribution of inflammation or MRI abnormalities to the associations of glycemic control or diabetes medication use with cognitive outcomes will be examined. Beyond investigating the relationship of cognitive decline in diabetes, identifying the impact of inflammation-a modifiable risk factor-within this relationship, has implications for mechanisms underlying incipient dementia in the general population, and could provide the basis for future intervention studies with potential great public health impact. Demonstrating how brain abnormalities link diabetes characteristics to cognitive decline would support a causative or contributive role of these characteristics in cognitive compromise. PUBLIC HEALTH RELEVANCE: This study of diabetic individuals will investigate the roles of inflammation, poor glycemic control, use of diabetes medications, and brain abnormalities at baseline on the rates of cognitive decline. Ultimately, our goal is to extend life without cognitive compromise. This study will point to interventions to assist individuals with diabetes, who are at high risk for dementia. Since rates of diabetes and dementia are disproportionately increasing, especially so as the population structure shifts strongly toward the aged, this study can be expected to have major public health implications. Furthermore, identifying the impact of inflammation and brain abnormalities on risk for cognitive impairment has implications for mechanisms of dementia in the general population, which may lead to even broader based preventive or palliative interventions for cognitive decline and dementia.

描述（由申请人提供）：这项为期5年的前瞻性研究将研究长期2型糖尿病特征和炎症如何影响以色列特拉维夫1000名65岁及以上认知功能完整（招募时）糖尿病患者的认知功能下降。这项研究是由纽约西奈山医学院（MSSM）精神病学系，以色列Sheba医疗中心精神病学系和以色列第二大HMO Maccabi卫生服务（MHS）社区卫生部合作进行的。它向特拉维夫地区具有代表性的170万以色列公民提供保健服务，其中11 000人患有糖尿病，年龄在65岁以上。研究这一人群的好处是：a）来自非常丰富的MHS糖尿病登记处的长达10年的数据，包括HbA 1c、抗糖尿病药物和其他药物、疾病持续时间、高血压和其他糖尿病相关特征; B）完全计算机化的集中处理的MHS医疗记录，便于数据访问和分析; c）由卫生部中央实验室对病人进行分析不收费，确保完全使用; d）卫生部药房提供大量补贴的药物，记录每次购买（与处方药物的受试者报告相反）; e）由于生病的受试者由MHS护理，因此联系损失最小;和f）通过终止客户资助及时通知死亡。Sheba的痴呆症诊断程序将与MSSM阿尔茨海默病研究中心（ADRC）的诊断程序完全整合。将每隔18个月对受试者进行随访。除了完整的MHS实验室和医疗数据外，包括以色列和ADRC医生在内的诊断共识电话会议还将获得本项目收集的临床、神经心理学和MRI数据。将收集DNA，并制定数据共享计划。具体目的是研究基线1）炎症，2）长期血糖控制不良，3）糖尿病药物（特别是二甲双胍）和4）MRI异常对认知下降率的影响。此外，还将检查炎症或MRI异常对血糖控制或糖尿病药物使用与认知结局相关性的影响。除了调查糖尿病认知能力下降的关系，确定炎症的影响-一种可改变的风险因素-在这种关系中，对一般人群中早期痴呆症的潜在机制有影响，并可能为未来的干预研究提供基础，具有潜在的巨大公共卫生影响。证明大脑异常如何将糖尿病特征与认知能力下降联系起来，将支持这些特征在认知损害中的因果或贡献作用。公共卫生关系：这项糖尿病个体研究将调查炎症、血糖控制不良、糖尿病药物使用和基线时大脑异常对认知能力下降率的作用。最终，我们的目标是在不损害认知的情况下延长寿命。这项研究将指出干预措施，以帮助糖尿病患者，谁是痴呆症的高风险。由于糖尿病和痴呆症的发病率不成比例地增加，特别是随着人口结构向老年人的强烈转变，这项研究预计将对公共卫生产生重大影响。此外，确定炎症和大脑异常对认知障碍风险的影响对一般人群中痴呆症的机制具有影响，这可能导致对认知衰退和痴呆症的更广泛的预防或姑息干预。