MRI patterns of atrophy associated with progression to AD in amnestic mild cognitive impairment

萎缩 认知障碍 医学 认知 神经科学 磁共振成像 心理学 病理 放射科
作者
Jennifer L. Whitwell,Maria M. Shiung,Scott A. Przybelski,Stephen D. Weigand,D. S. Knopman,B. F. Boeve,R. C. Petersen,Clifford R. Jack
出处
期刊:Neurology [Lippincott Williams & Wilkins]
卷期号:70 (7): 512-520 被引量:350
标识
DOI:10.1212/01.wnl.0000280575.77437.a2
摘要

Objective: To compare the patterns of gray matter loss in subjects with amnestic mild cognitive impairment (aMCI) who progress to Alzheimer disease (AD) within a fixed clinical follow-up time vs those who remain stable. Methods: Twenty-one subjects with aMCI were identified from the Mayo Clinic Alzheimer9s research program who remained clinically stable for their entire observed clinical course (aMCI-S), where the minimum required follow-up time from MRI to last follow-up assessment was 3 years. These subjects were age- and gender-matched to 42 aMCI subjects who progressed to AD within 18 months of the MRI (aMCI-P). Each subject was then age- and gender-matched to a control subject. Voxel-based morphometry (VBM) was used to assess patterns of gray matter atrophy in the aMCI-P and aMCI-S groups compared to the control group, and compared to each other. Results: The aMCI-P group showed bilateral loss affecting the medial and inferior temporal lobe, temporoparietal association neocortex, and frontal lobes, compared to controls. The aMCI-S group showed no regions of gray matter loss when compared to controls. When the aMCI-P and aMCI-S groups were compared directly, the aMCI-P group showed greater loss in the medial and inferior temporal lobes, the temporoparietal neocortex, posterior cingulate, precuneus, anterior cingulate, and frontal lobes than the aMCI-S group. Conclusions: The regions of loss observed in subjects with amnestic mild cognitive impairment (aMCI) who progressed to Alzheimer disease (AD) within 18 months of the MRI are typical of subjects with AD. The lack of gray matter loss in subjects with aMCI who remained clinically stable for their entire observed clinical course is consistent with the notion that patterns of atrophy on MRI at baseline map well onto the subsequent clinical course. GLOSSARY: AD = Alzheimer disease; ADNI = Alzheimer9s Disease Neuroimaging Initiative; ADPR = Alzheimer9s Disease Patient Registry; ADRC = Mayo Clinic Alzheimer9s Disease Research Center; aMCI = amnestic mild cognitive impairment; APOE e4 = apolipoprotein epsilon 4; AVLT = Auditory Verbal Learning Test; CDR-SB = CDR sum of boxes; DCT = discrete cosine transformation; FDR = false discovery rate; FWHM = full-width at half-maximum; GM = gray matter; MMSE = Mini-Mental State Examination; MNI = Montreal Neurological Institute; NIA = National Institute on Aging; TIV = total intracranial volume; VBM = voxel-based morphometry; WM = white matter; WMH = white matter hyperintensity.

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