Divergent Cortical Tau Positron Emission Tomography Patterns Among Patients With Preclinical Alzheimer Disease

正电子发射断层摄影术 匹兹堡化合物B 神经影像学 阿尔茨海默病神经影像学倡议 颞叶 磁共振成像 阿尔茨海默病 医学 心理学 认知功能衰退 淀粉样蛋白(真菌学) 疾病 神经科学 痴呆 内科学 病理 癫痫 放射科
作者
Christina Young,Joseph R. Winer,Kyan Younes,Karly Alex Cody,Tobey J. Betthauser,Sterling C. Johnson,Aaron P. Schultz,Reisa A. Sperling,Michael D. Greicius,Inma Cobos,Kathleen L. Poston,Elizabeth C. Mormino,Michael W. Weiner,Paul S. Aisen,Ronald C. Petersen,Clifford R. Jack,William J. Jagust,John Q. Trojanowki,Arthur W. Toga,Laurel A. Beckett,Robert C. Green,Andrew J. Saykin,John C. Morris,Richard K. Perrin,Leslie M. Shaw,Zaven S. Khachaturian,Maria C. Carrillo,William Z. Potter,Lisa L. Barnes,Marie A. Bernard,Hector M. González,Carole Ho,John K. Hsiao,Jonathan Jackson,Eliezer Masliah,Donna Masterman,Ozioma C. Okonkwo,Laurie M. Ryan,Nina Silverberg,Adam S. Fleisher,Diana Truran Sacrey,J. Fockler,Cat Conti,Dallas P. Veitch,John Neuhaus,Chengshi Jin,Rachel L. Nosheny,Mariam Ashford,Derek Flenniken,Adrienne Kormos,T. J. Montine,Michael S. Rafii,Rema Raman,Gustavo Guerrero Jiménez,Michael C. Donohue,Devon Gessert,Jennifer Salazar,Caileigh Zimmerman,Yuliana Cabrera,Sarah Walter,Garrett Miller,Godfrey A Coker,Taylor Clanton,Lindsey Hergesheimer,Stephanie A. Smith,Olusegun Adegoke,Payam Mahboubi,Shelley C. Moore,Jeremy Pizzola,Elizabeth M. Shaffer,Danielle J Harvey,A. Forghanian-Arani,Bret J. Borowski,Chad Ward,Christopher G. Schwarz,David R. Jones,Jeff Gunter,Kejal Kantarci,Matthew L. Senjem,Prashanthi Vemuri,Robert L. Reid,Nick C. Fox,Ian B. Malone,Paul M. Thompson,Sophia I. Thomopoulos,Talia M. Nir,Neda Jahanshad,Charles DeCarli,Alexander Knaack,Evan Fletcher,Duygu Tosun,Stephanie H Chen,Mark Choe,Karen Crawford,Paul A Yuschkevich,Sandhitsu R. Das,Robert A. Koeppe,Eric M. Reiman,Kewei Chen,Chet Mathis
出处
期刊:JAMA Neurology [American Medical Association]
卷期号:79 (6): 592-592 被引量:6
标识
DOI:10.1001/jamaneurol.2022.0676
摘要

Characterization of early tau deposition in individuals with preclinical Alzheimer disease (AD) is critical for prevention trials that aim to select individuals at risk for AD and halt the progression of disease.To evaluate the prevalence of cortical tau positron emission tomography (PET) heterogeneity in a large cohort of clinically unimpaired older adults with elevated β-amyloid (A+).This cross-sectional study examined prerandomized tau PET, amyloid PET, structural magnetic resonance imaging, demographic, and cognitive data from the Anti-Amyloid Treatment in Asymptomatic AD (A4) Study from April 2014 to December 2017. Follow-up analyses used observational tau PET data from the Alzheimer's Disease Neuroimaging Initiative (ADNI), the Harvard Aging Brain Study (HABS), and the Wisconsin Registry for Alzheimer's Prevention and the Wisconsin Alzheimer's Disease Research Center (together hereinafter referred to as Wisconsin) to evaluate consistency. Participants were clinically unimpaired at the study visit closest to the tau PET scan and had available amyloid and tau PET data (A4 Study, n = 447; ADNI, n = 433; HABS, n = 190; and Wisconsin, n = 328). No participants who met eligibility criteria were excluded. Data were analyzed from May 11, 2021, to January 25, 2022.Individuals with preclinical AD with heterogeneous cortical tau PET patterns (A+T cortical+) were identified by examining asymmetrical cortical tau signal and disproportionate cortical tau signal relative to medial temporal lobe (MTL) tau. Voxelwise tau patterns, amyloid, neurodegeneration, cognition, and demographic characteristics were examined.The 447 A4 participants (A+ group, 392; and normal β-amyloid group, 55), with a mean (SD) age of 71.8 (4.8) years, included 239 women (54%). A total of 36 individuals in the A+ group (9% of the A+ group) exhibited heterogeneous cortical tau patterns and were further categorized into 3 subtypes: asymmetrical left, precuneus dominant, and asymmetrical right. A total of 116 individuals in the A+ group (30% of the A+ group) showed elevated MTL tau (A+T MTL+). Individuals in the A+T cortical+ group were younger than those in the A+T MTL+ group (t61.867 = -2.597; P = .03). Across the A+T cortical+ and A+T MTL+ groups, increased regional tau was associated with reduced hippocampal volume and MTL thickness but not with cortical thickness. Memory scores were comparable between the A+T cortical+ and A+T MTL+ groups, whereas executive functioning scores were lower for the A+T cortical+ group than for the A+T MTL+ group. The prevalence of the A+T cortical+ group and tau patterns within the A+T cortical+ group were consistent in ADNI, HABS, and Wisconsin.This study suggests that early tau deposition may follow multiple trajectories during preclinical AD and may involve several cortical regions. Staging procedures, especially those based on neuropathology, that assume a uniform trajectory across individuals are insufficient for disease monitoring with tau imaging.
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