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Longitudinal assessment of neuroimaging and clinical markers in autosomal dominant Alzheimer's disease: a prospective cohort study.
Lancet Neurol. 2015 Aug; 14(8):804-813.LN

Abstract

BACKGROUND

The biomarker model of Alzheimer's disease postulates a dynamic sequence of amyloidosis, neurodegeneration, and cognitive decline as an individual progresses from preclinical Alzheimer's disease to dementia. Despite supportive evidence from cross-sectional studies, verification with long-term within-individual data is needed.

METHODS

For this prospective cohort study, carriers of autosomal dominant Alzheimer's disease mutations (aged ≥21 years) were recruited from across the USA through referrals by physicians or from affected families. People with mutations in PSEN1, PSEN2, or APP were assessed at the University of Pittsburgh Alzheimer's Disease Research Center every 1-2 years, between March 23, 2003, and Aug 1, 2014. We measured global cerebral amyloid β (Aβ) load using (11)C-Pittsburgh Compound-B PET, posterior cortical metabolism with (18)F-fluorodeoxyglucose PET, hippocampal volume (age and sex corrected) with T1-weighted MRI, verbal memory with the ten-item Consortium to Establish a Registry for Alzheimer's Disease Word List Learning Delayed Recall Test, and general cognition with the Mini Mental State Examination. We estimated overall biomarker trajectories across estimated years from symptom onset using linear mixed models, and compared these estimates with cross-sectional data from cognitively normal control individuals (age 65-89 years) who were negative for amyloidosis, hypometabolism, and hippocampal atrophy. In the mutation carriers who had the longest follow-up, we examined the within-individual progression of amyloidosis, metabolism, hippocampal volume, and cognition to identify progressive within-individual changes (a significant change was defined as an increase or decrease of more than two Z scores standardised to controls).

FINDINGS

16 people with mutations in PSEN1, PSEN2, or APP, aged 28-56 years, completed between two and eight assessments (a total of 83 assessments) over 2-11 years. Significant differences in mutation carriers compared with controls (p<0·01) were detected in the following order: increased amyloidosis (7·5 years before expected onset), decreased metabolism (at time of expected onset), decreased hippocampal volume and verbal memory (7·5 years after expected onset), and decreased general cognition (10 years after expected onset). Among the seven participants with longest follow-up (seven or eight assessments spanning 6-11 years), three individuals had active amyloidosis without progressive neurodegeneration or cognitive decline, two amyloid-positive individuals showed progressive neurodegeneration and cognitive decline without further progressive amyloidosis, and two amyloid-positive individuals showed neither active amyloidosis nor progressive neurodegeneration or cognitive decline.

INTERPRETATION

Our results support amyloidosis as the earliest component of the biomarker model in autosomal dominant Alzheimer's disease. Our within-individual examination suggests three sequential phases in the development of autosomal dominant Alzheimer's disease-active amyloidosis, a stable amyloid-positive period, and progressive neurodegeneration and cognitive decline-indicating that Aβ accumulation is largely complete before progressive neurodegeneration and cognitive decline occur. These findings offer supportive evidence for efforts to target early Aβ deposition for secondary prevention in individuals with autosomal dominant Alzheimer's disease.

FUNDING

National Institutes of Health and Howard Hughes Medical Institute.

Links

PMC Free PDF

Authors+Show Affiliations

Yau WW
Department of Psychiatry, University of Pittsburgh, Pittsburgh, PA, USA.
Tudorascu DL
Department of Biostatistics, University of Pittsburgh, Pittsburgh, PA, USA.
McDade EM
Department of Neurology, University of Pittsburgh, Pittsburgh, PA, USA.
Ikonomovic S
Department of Neurology, University of Pittsburgh, Pittsburgh, PA, USA.
James JA
Department of Radiology, University of Pittsburgh, Pittsburgh, PA, USA.
Minhas D
Department of Radiology, University of Pittsburgh, Pittsburgh, PA, USA.
Mowrey W
Division of Biostatistics, Department of Epidemiology and Population Health, Albert Einstein College of Medicine, New York, NY, USA.
Sheu LK
Department of Psychology, University of Pittsburgh, Pittsburgh, PA, USA.
Snitz BE
Department of Neurology, University of Pittsburgh, Pittsburgh, PA, USA.
Weissfeld L
Statistics Collaborative, Inc, Washington, DC, USA.
Gianaros PJ
Department of Psychology, University of Pittsburgh, Pittsburgh, PA, USA.
Aizenstein HJ
Department of Psychiatry, University of Pittsburgh, Pittsburgh, PA, USA.
Price JC
Department of Radiology, University of Pittsburgh, Pittsburgh, PA, USA.
Mathis CA
Department of Radiology, University of Pittsburgh, Pittsburgh, PA, USA.
Lopez OL
Department of Neurology, University of Pittsburgh, Pittsburgh, PA, USA.
Klunk WE
Department of Psychiatry, University of Pittsburgh, Pittsburgh, PA, USA. Electronic address: klunkwe@upmc.edu.

MeSH

AdultAgedAged, 80 and overAlzheimer DiseaseAmyloid beta-PeptidesAmyloidosisAniline CompoundsBiomarkersCerebral CortexDisease ProgressionFemaleHippocampusHumansMaleMiddle AgedProspective StudiesThiazoles

Pub Type(s)

Journal Article
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

Language

eng

PubMed ID

26139022

Citation

Yau, Wai-Ying Wendy, et al. "Longitudinal Assessment of Neuroimaging and Clinical Markers in Autosomal Dominant Alzheimer's Disease: a Prospective Cohort Study." The Lancet. Neurology, vol. 14, no. 8, 2015, pp. 804-813.
Yau WW, Tudorascu DL, McDade EM, et al. Longitudinal assessment of neuroimaging and clinical markers in autosomal dominant Alzheimer's disease: a prospective cohort study. Lancet Neurol. 2015;14(8):804-813.
Yau, W. W., Tudorascu, D. L., McDade, E. M., Ikonomovic, S., James, J. A., Minhas, D., Mowrey, W., Sheu, L. K., Snitz, B. E., Weissfeld, L., Gianaros, P. J., Aizenstein, H. J., Price, J. C., Mathis, C. A., Lopez, O. L., & Klunk, W. E. (2015). Longitudinal assessment of neuroimaging and clinical markers in autosomal dominant Alzheimer's disease: a prospective cohort study. The Lancet. Neurology, 14(8), 804-813. https://doi.org/10.1016/S1474-4422(15)00135-0
Yau WW, et al. Longitudinal Assessment of Neuroimaging and Clinical Markers in Autosomal Dominant Alzheimer's Disease: a Prospective Cohort Study. Lancet Neurol. 2015;14(8):804-813. PubMed PMID: 26139022.
* Article titles in AMA citation format should be in sentence-case
TY - JOUR T1 - Longitudinal assessment of neuroimaging and clinical markers in autosomal dominant Alzheimer's disease: a prospective cohort study. AU - Yau,Wai-Ying Wendy, AU - Tudorascu,Dana L, AU - McDade,Eric M, AU - Ikonomovic,Snezana, AU - James,Jeffrey A, AU - Minhas,Davneet, AU - Mowrey,Wenzhu, AU - Sheu,Lei K, AU - Snitz,Beth E, AU - Weissfeld,Lisa, AU - Gianaros,Peter J, AU - Aizenstein,Howard J, AU - Price,Julie C, AU - Mathis,Chester A, AU - Lopez,Oscar L, AU - Klunk,William E, Y1 - 2015/06/29/ PY - 2015/04/01/received PY - 2015/05/13/revised PY - 2015/06/03/accepted PY - 2015/7/4/entrez PY - 2015/7/4/pubmed PY - 2015/10/16/medline SP - 804 EP - 813 JF - The Lancet. Neurology JO - Lancet Neurol VL - 14 IS - 8 N2 - BACKGROUND: The biomarker model of Alzheimer's disease postulates a dynamic sequence of amyloidosis, neurodegeneration, and cognitive decline as an individual progresses from preclinical Alzheimer's disease to dementia. Despite supportive evidence from cross-sectional studies, verification with long-term within-individual data is needed. METHODS: For this prospective cohort study, carriers of autosomal dominant Alzheimer's disease mutations (aged ≥21 years) were recruited from across the USA through referrals by physicians or from affected families. People with mutations in PSEN1, PSEN2, or APP were assessed at the University of Pittsburgh Alzheimer's Disease Research Center every 1-2 years, between March 23, 2003, and Aug 1, 2014. We measured global cerebral amyloid β (Aβ) load using (11)C-Pittsburgh Compound-B PET, posterior cortical metabolism with (18)F-fluorodeoxyglucose PET, hippocampal volume (age and sex corrected) with T1-weighted MRI, verbal memory with the ten-item Consortium to Establish a Registry for Alzheimer's Disease Word List Learning Delayed Recall Test, and general cognition with the Mini Mental State Examination. We estimated overall biomarker trajectories across estimated years from symptom onset using linear mixed models, and compared these estimates with cross-sectional data from cognitively normal control individuals (age 65-89 years) who were negative for amyloidosis, hypometabolism, and hippocampal atrophy. In the mutation carriers who had the longest follow-up, we examined the within-individual progression of amyloidosis, metabolism, hippocampal volume, and cognition to identify progressive within-individual changes (a significant change was defined as an increase or decrease of more than two Z scores standardised to controls). FINDINGS: 16 people with mutations in PSEN1, PSEN2, or APP, aged 28-56 years, completed between two and eight assessments (a total of 83 assessments) over 2-11 years. Significant differences in mutation carriers compared with controls (p<0·01) were detected in the following order: increased amyloidosis (7·5 years before expected onset), decreased metabolism (at time of expected onset), decreased hippocampal volume and verbal memory (7·5 years after expected onset), and decreased general cognition (10 years after expected onset). Among the seven participants with longest follow-up (seven or eight assessments spanning 6-11 years), three individuals had active amyloidosis without progressive neurodegeneration or cognitive decline, two amyloid-positive individuals showed progressive neurodegeneration and cognitive decline without further progressive amyloidosis, and two amyloid-positive individuals showed neither active amyloidosis nor progressive neurodegeneration or cognitive decline. INTERPRETATION: Our results support amyloidosis as the earliest component of the biomarker model in autosomal dominant Alzheimer's disease. Our within-individual examination suggests three sequential phases in the development of autosomal dominant Alzheimer's disease-active amyloidosis, a stable amyloid-positive period, and progressive neurodegeneration and cognitive decline-indicating that Aβ accumulation is largely complete before progressive neurodegeneration and cognitive decline occur. These findings offer supportive evidence for efforts to target early Aβ deposition for secondary prevention in individuals with autosomal dominant Alzheimer's disease. FUNDING: National Institutes of Health and Howard Hughes Medical Institute. SN - 1474-4465 UR - https://www.unboundmedicine.com/medline/citation/26139022/Longitudinal_assessment_of_neuroimaging_and_clinical_markers_in_autosomal_dominant_Alzheimer's_disease:_a_prospective_cohort_study_ DB - PRIME DP - Unbound Medicine ER -