Atrophy patterns in early clinical stages across distinct phenotypes of Alzheimer's disease

被引:183
作者
Ossenkoppele, Rik [1 ,2 ,3 ,4 ,5 ]
Cohn-Sheehy, Brendan I. [1 ]
La Joie, Renaud [2 ]
Vogel, Jacob W. [2 ]
Moeller, Christiane [3 ,4 ]
Lehmann, Manja [1 ,6 ]
van Berckel, Bart N. M. [2 ]
Seeley, William W. [1 ]
Pijnenburg, Yolande A. [3 ,4 ]
Gorno-Tempini, Maria L. [1 ]
Kramer, Joel H. [1 ]
Barkhof, Frederik
Rosen, Howard J. [1 ]
van der Flier, Wiesje M. [3 ,4 ,7 ]
Jagust, William J. [2 ]
Miller, Bruce L. [1 ]
Scheltens, Philip [3 ,4 ]
Rabinovici, Gil D. [1 ,2 ]
机构
[1] Univ Calif San Francisco, Memory & Aging Ctr, Dept Neurol, San Francisco, CA 94158 USA
[2] Univ Calif Berkeley, Helen Wills Neurosci Inst, Berkeley, CA 94720 USA
[3] Vrije Univ Amsterdam Med Ctr, Dept Neurol, Amsterdam, Netherlands
[4] Vrije Univ Amsterdam Med Ctr, Alzheimer Ctr, Amsterdam, Netherlands
[5] Vrije Univ Amsterdam Med Ctr, Dept Radiol & Nucl Med, Amsterdam, Netherlands
[6] UCL, Inst Neurol, Dementia Res Ctr, London, England
[7] Vrije Univ Amsterdam Med Ctr, Dept Epidemiol & Biostat, Amsterdam, Netherlands
关键词
Alzheimer's disease; magnetic resonance imaging (MRI); posterior cortical atrophy; logopenic variant primary progressive aphasia; early-onset dementia; default mode network; language; memory; vision; atrophy; voxel-based morphometry; PRIMARY PROGRESSIVE APHASIA; POSTERIOR CORTICAL ATROPHY; NATIONAL INSTITUTE; ASSOCIATION WORKGROUPS; DIAGNOSTIC GUIDELINES; LEARNING-DISABILITY; GLUCOSE-METABOLISM; CINGULATE CORTEX; BRAIN ATROPHY; ONSET;
D O I
10.1002/hbm.22927
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
Alzheimer's disease (AD) can present with distinct clinical variants. Identifying the earliest neurodegenerative changes associated with each variant has implications for early diagnosis, and for understanding the mechanisms that underlie regional vulnerability and disease progression in AD. We performed voxel-based morphometry to detect atrophy patterns in early clinical stages of four AD phenotypes: Posterior cortical atrophy (PCA, visual variant, n = 93), logopenic variant primary progressive aphasia (lvPPA, language variant, n = 74), and memory-predominant AD categorized as early age-of-onset (EOAD, <65 years, n = 114) and late age-of-onset (LOAD, >65 years, n = 114). Patients with each syndrome were stratified based on: (1) degree of functional impairment, as measured by the clinical dementia rating (CDR) scale, and (2) overall extent of brain atrophy, as measured by a neuroimaging approach that sums the number of brain voxels showing significantly lower gray matter volume than cognitively normal controls (n = 80). Even at the earliest clinical stage (CDR=0.5 or bottom quartile of overall atrophy), patients with each syndrome showed both common and variant-specific atrophy. Common atrophy across variants was found in temporoparietal regions that comprise the posterior default mode network (DMN). Early syndrome-specific atrophy mirrored functional brain networks underlying functions that are uniquely affected in each variant: Language network in lvPPA, posterior cingulate cortex-hippocampal circuit in amnestic EOAD and LOAD, and visual networks in PCA. At more advanced stages, atrophy patterns largely converged across AD variants. These findings support a model in which neurodegeneration selectively targets both the DMN and syndrome-specific vulnerable networks at the earliest clinical stages of AD. Hum Brain Mapp 36:4421-4437, 2015. (c) 2015 Wiley Periodicals, Inc.
引用
收藏
页码:4421 / 4437
页数:17
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