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Mapping the neuroanatomy of functional decline in Alzheimer's disease from basic to advanced activities of daily living

Mapping the neuroanatomy of functional decline in Alzheimer's disease from basic to advanced activities of daily living
Mapping the neuroanatomy of functional decline in Alzheimer's disease from basic to advanced activities of daily living
Background
Impairments in activities of daily living (ADL) are a criterion for Alzheimer’s disease (AD) dementia. However, ADL gradually decline in AD, impacting on advanced (a-ADL, complex interpersonal or social functioning), instrumental (IADL, maintaining life in community), and finally basic functions (BADL, activities related to physiological and self-maintenance needs). Information and communication technologies (ICT) have become an increasingly important aspect of daily functioning. Yet, the links of ADL, ICT, and neuropathology of AD dementia are poorly understood. Such knowledge is critical as it can provide biomarker evidence of functional decline in AD.

Methods
ADL were evaluated with the Technology–Activities of Daily Living Questionnaire (T-ADLQ) in 33 patients with AD and 30 controls. ADL were divided in BADL, IADL, and a-ADL. The three domain subscores were covaried against gray matter atrophy via voxel-based morphometry.

Results
Our results showed that three domain subscores of ADL correlate with several brain structures, with a varying degree of overlap between them. BADL score correlated mostly with frontal atrophy, IADL with more widespread frontal, temporal and occipital atrophy and a-ADL with occipital and temporal atrophy. Finally, ICT subscale was associated with atrophy in the precuneus.

Conclusions
The association between ADL domains and neurodegeneration in AD follows a traceable neuropathological pathway which involves different neural networks. This the first evidence of ADL phenotypes in AD characterised by specific patterns of functional decline and well-defined neuropathological changes. The identification of such phenotypes can yield functional biomarkers for dementias such as AD.
0340-5354
1310–1322
Slachevsky, A
d3f101c3-39bc-484f-a367-e25ba6f5502f
Forno, G
9119ed81-614d-4d2c-b302-7b69a2a498f7
Barraza, P
62a794d1-1502-4735-8f04-36930ee740da
Mioshi, E
5310242a-e90b-476d-a02d-51f13f973c8e
Delgado, C
71a58e76-d0a0-457a-abfc-ffa1e755950b
Lillo, P
359a4abf-438b-46d1-8716-c9583ed414db
Henriquez, F
19ef66aa-6f10-41fe-a210-0353c8b4f72f
Bravo, E
6345e0af-a729-4eb5-9f16-cfc9e9c2dfca
Farias, M
24c149c4-393c-4bd4-a7ca-f582a7cfcfed
Muñoz-Neira, C
911b6dc7-f34b-4cba-95a8-8bf3509ac614
Ibañez, A
82e6b410-7245-490e-8743-33710847c14c
MA, Parra
89c147aa-17a1-4b03-8a69-1ca1ab9cdf05
Hornberger, M
a48c1c63-422a-4c11-9a51-c7be0aa3026d
Slachevsky, A
d3f101c3-39bc-484f-a367-e25ba6f5502f
Forno, G
9119ed81-614d-4d2c-b302-7b69a2a498f7
Barraza, P
62a794d1-1502-4735-8f04-36930ee740da
Mioshi, E
5310242a-e90b-476d-a02d-51f13f973c8e
Delgado, C
71a58e76-d0a0-457a-abfc-ffa1e755950b
Lillo, P
359a4abf-438b-46d1-8716-c9583ed414db
Henriquez, F
19ef66aa-6f10-41fe-a210-0353c8b4f72f
Bravo, E
6345e0af-a729-4eb5-9f16-cfc9e9c2dfca
Farias, M
24c149c4-393c-4bd4-a7ca-f582a7cfcfed
Muñoz-Neira, C
911b6dc7-f34b-4cba-95a8-8bf3509ac614
Ibañez, A
82e6b410-7245-490e-8743-33710847c14c
MA, Parra
89c147aa-17a1-4b03-8a69-1ca1ab9cdf05
Hornberger, M
a48c1c63-422a-4c11-9a51-c7be0aa3026d

Slachevsky, A, Forno, G, Barraza, P, Mioshi, E, Delgado, C, Lillo, P, Henriquez, F, Bravo, E, Farias, M, Muñoz-Neira, C, Ibañez, A, MA, Parra and Hornberger, M (2019) Mapping the neuroanatomy of functional decline in Alzheimer's disease from basic to advanced activities of daily living. Journal of Neurology, 266, 1310–1322. (doi:10.1007/s00415-019-09260-w).

Record type: Article

Abstract

Background
Impairments in activities of daily living (ADL) are a criterion for Alzheimer’s disease (AD) dementia. However, ADL gradually decline in AD, impacting on advanced (a-ADL, complex interpersonal or social functioning), instrumental (IADL, maintaining life in community), and finally basic functions (BADL, activities related to physiological and self-maintenance needs). Information and communication technologies (ICT) have become an increasingly important aspect of daily functioning. Yet, the links of ADL, ICT, and neuropathology of AD dementia are poorly understood. Such knowledge is critical as it can provide biomarker evidence of functional decline in AD.

Methods
ADL were evaluated with the Technology–Activities of Daily Living Questionnaire (T-ADLQ) in 33 patients with AD and 30 controls. ADL were divided in BADL, IADL, and a-ADL. The three domain subscores were covaried against gray matter atrophy via voxel-based morphometry.

Results
Our results showed that three domain subscores of ADL correlate with several brain structures, with a varying degree of overlap between them. BADL score correlated mostly with frontal atrophy, IADL with more widespread frontal, temporal and occipital atrophy and a-ADL with occipital and temporal atrophy. Finally, ICT subscale was associated with atrophy in the precuneus.

Conclusions
The association between ADL domains and neurodegeneration in AD follows a traceable neuropathological pathway which involves different neural networks. This the first evidence of ADL phenotypes in AD characterised by specific patterns of functional decline and well-defined neuropathological changes. The identification of such phenotypes can yield functional biomarkers for dementias such as AD.

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More information

Published date: April 2019

Identifiers

Local EPrints ID: 504893
URI: http://eprints.soton.ac.uk/id/eprint/504893
DOI: doi:10.1007/s00415-019-09260-w
ISSN: 0340-5354
PURE UUID: 91f19b6b-43ed-452f-a174-1b6d4d3b83e8
ORCID for M Hornberger: ORCID iD orcid.org/0000-0002-2214-3788

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Date deposited: 19 Sep 2025 17:19
Last modified: 20 Sep 2025 02:31

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Contributors

Author: A Slachevsky
Author: G Forno
Author: P Barraza
Author: E Mioshi
Author: C Delgado
Author: P Lillo
Author: F Henriquez
Author: E Bravo
Author: M Farias
Author: C Muñoz-Neira
Author: A Ibañez
Author: Parra MA
Author: M Hornberger ORCID iD

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