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与阿尔茨海默病相关的共病轨迹:一项在美国理赔数据库中的匹配病例对照研究。

Comorbidity Trajectories Associated With Alzheimer's Disease: A Matched Case-Control Study in a United States Claims Database.

作者信息

Butler Lesley M, Houghton Richard, Abraham Anup, Vassilaki Maria, Durán-Pacheco Gonzalo

机构信息

F. Hoffmann-La Roche Ltd., Basel, Switzerland.

Genesis Research, Hoboken, NJ, United States.

出版信息

Front Neurosci. 2021 Oct 8;15:749305. doi: 10.3389/fnins.2021.749305. eCollection 2021.

Abstract

Trajectories of comorbidities among individuals at risk of Alzheimer's disease (AD) may differ from those aging without AD clinical syndrome. Therefore, characterizing the comorbidity burden and pattern associated with AD risk may facilitate earlier detection, enable timely intervention, and help slow the rate of cognitive and functional decline in AD. This case-control study was performed to compare the prevalence of comorbidities between AD cases and controls during the 5 years prior to diagnosis (or index date for controls); and to identify comorbidities with a differential time-dependent prevalence trajectory during the 5 years prior to AD diagnosis. Incident AD cases and individually matched controls were identified in a United States claims database between January 1, 2000 and December 31, 2016. AD status and comorbidities were defined based on the presence of diagnosis codes in administrative claims records. Generalized estimating equations were used to assess evidence of changes over time and between AD and controls. A principal component analysis and hierarchical clustering was performed to identify groups of AD-related comorbidities with respect to prevalence changes over time (or trajectory), and differences between AD and controls. Data from 186,064 individuals in the IBM MarketScan Commercial Claims and Medicare Supplementary databases were analyzed (93,032 AD cases and 93,032 non-AD controls). In total, there were 177 comorbidities with a ≥ 5% prevalence. Five main clusters of comorbidities were identified. Clusters differed between AD cases and controls in the overall magnitude of association with AD, in their diverging time trajectories, and in comorbidity prevalence. Three clusters contained comorbidities that notably increased in frequency over time in AD cases but not in controls during the 5-year period before AD diagnosis. Comorbidities in these clusters were related to the early signs and/or symptoms of AD, psychiatric and mood disorders, cerebrovascular disease, history of hazard and injuries, and metabolic, cardiovascular, and respiratory complaints. We demonstrated a greater comorbidity burden among those who later developed AD vs. controls, and identified comorbidity clusters that could distinguish these two groups. Further investigation of comorbidity burden is warranted to facilitate early detection of individuals at risk of developing AD.

摘要

阿尔茨海默病(AD)风险个体的共病轨迹可能与无AD临床综合征的衰老个体不同。因此,描述与AD风险相关的共病负担和模式可能有助于早期发现、及时干预,并有助于减缓AD患者认知和功能衰退的速度。本病例对照研究旨在比较AD病例与对照在诊断前5年(或对照的索引日期)期间共病的患病率;并确定在AD诊断前5年中具有不同时间依赖性患病率轨迹的共病。在2000年1月1日至2016年12月31日期间的美国索赔数据库中识别出AD发病病例和个体匹配的对照。AD状态和共病根据行政索赔记录中的诊断代码确定。使用广义估计方程评估AD与对照之间随时间变化的证据。进行主成分分析和层次聚类,以识别与AD相关的共病组在患病率随时间变化(或轨迹)以及AD与对照之间的差异方面的情况。对IBM MarketScan商业索赔和医疗保险补充数据库中的186,064名个体的数据进行了分析(93,032例AD病例和93,032名非AD对照)。总共有177种共病的患病率≥5%。确定了五个主要的共病簇。AD病例和对照在与AD的总体关联程度、不同的时间轨迹以及共病患病率方面存在差异。三个簇包含的共病在AD诊断前5年期间,AD病例中的频率随时间显著增加,而对照中则没有。这些簇中的共病与AD的早期体征和/或症状、精神和情绪障碍、脑血管疾病、危险和损伤史以及代谢、心血管和呼吸系统疾病有关。我们证明了后来发生AD的个体与对照相比共病负担更重,并识别出可以区分这两组的共病簇。有必要进一步研究共病负担,以促进对有发展为AD风险个体的早期发现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdc0/8531650/1c3b43038024/fnins-15-749305-g001.jpg

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