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Alzheimer Disease as a Clinical-Biological Construct—An International Working Group Recommendation

生物标志物 疾病 医学 时间轴 心理学 构造(python库) 梅德林 病理 化学 计算机科学 程序设计语言 生物化学 考古 政治学 法学 历史
作者
Bruno Dubois,Nicolas Villain,Lon S. Schneider,Nick C. Fox,Noll L. Campbell,Douglas Galasko,Miia Kivipelto,Frank Jessen,Bernard Hanseeuw,Merçé Boada,Frederik Barkhof,Agneta Nordberg,Lutz Froelich,Gunhild Waldemar,Kristian Steen Frederiksen,Alessandro Padovani,Vincent Planche,Christopher C. Rowe,Alexandre Bejanin,Agustín Ibáñez,Stefano F. Cappa,Paulo Caramelli,Ricardo Nitríni,Ricardo Allegri,Andrea Slachevsky,Leonardo Cruz de Souza,Andrea Bozoki,Eric Widera,Kaj Blennow,Craig Ritchie,Marc Agronin,F. Lopera,Lisa Delano‐Wood,Stéphanie Bombois,Richard Lévy,Madhav Thambisetty,Jean Georges,David T. Jones,Helen Lavretsky,Jonathan M. Schott,Jennifer R. Gatchel,Sandra Swantek,Paul Newhouse,Howard Feldman,Giovanni B. Frisoni
出处
期刊:JAMA Neurology [American Medical Association]
标识
DOI:10.1001/jamaneurol.2024.3770
摘要

Importance Since 2018, a movement has emerged to define Alzheimer disease (AD) as a purely biological entity based on biomarker findings. The recent revision of the Alzheimer Association (AA) criteria for AD furthers this direction. However, concerns about a purely biological definition of AD being applied clinically, the understanding of AD by society at large, and the translation of blood-based biomarkers into clinical practice prompt these International Working Group (IWG) updated recommendations. Objective To consider the revised AA criteria and to offer an alternative definitional view of AD as a clinical-biological construct for clinical use. The recommendations of the 2021 IWG diagnostic criteria are updated for further elaborating at-risk and presymptomatic states. Evidence Review PubMed was searched for articles published between July 1, 2020, and March 1, 2024, using the terms “biomarker” OR “amyloid” OR “tau” OR “neurodegeneration” OR “preclinical” OR “CSF” OR “PET” OR “plasma” AND “Alzheimer’s disease.” The references of relevant articles were also searched. Findings In the new AA diagnostic criteria, AD can be defined clinically as encompassing cognitively normal people having a core 1 AD biomarker. However, recent literature shows that the majority of biomarker-positive cognitively normal individuals will not become symptomatic along a proximate timeline. In the clinical setting, disclosing a diagnosis of AD to cognitively normal people with only core 1 AD biomarkers represents the most problematic implication of a purely biological definition of the disease. Conclusions and Relevance The ultimate aim of the field was to foster effective AD treatments, including preventing symptoms and dementia. The approach of diagnosing AD without a clinical and biological construct would be unwarranted and potentially concerning without a clear knowledge of when or whether symptoms will ever develop. It is recommended that those who are amyloid-positive only and, more generally, most biomarker-positive cognitively normal individuals, should not be labeled as having AD. Rather, they should be considered as being at risk for AD. The expansion of presymptomatic AD is viewed as a better diagnostic construct for those with a specific pattern of biomarkers, indicating that they are proximate to the expression of symptoms in the near future.
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