Cognitive and functional changes associated with Aβ pathology and the progression to mild cognitive impairment

Insel, Philip S.; Donohue, Michael C.; Mackin, R. Scott; Aisen, Paul S.; Hansson, Oskar; Weiner, Michael W.; Mattsson, Niklas

Cognitive and functional changes associated with Aβ pathology and the progression to mild cognitive impairment

Mark

Insel, Philip S. ^LU ; Donohue, Michael C. ; Mackin, R. Scott ; Aisen, Paul S. ; Hansson, Oskar ^LU

; Weiner, Michael W. and Mattsson, Niklas ^LU

(2016) In Neurobiology of Aging 48. p.172-181

Abstract: Cognitively-normal people with evidence of β-amyloid (Aβ) pathology and subtle cognitive dysfunction are believed to be at high risk for progression to mild cognitive impairment due to Alzheimer's disease (AD). Clinical trials in later stages of AD typically include a coprimary endpoint to demonstrate efficacy on both cognitive and functional assessments. Recent trials focus on cognitively-normal people, but functional decline has not been explored for trial designs in this group. The goal of this study was therefore to characterize cognitive and functional decline in (1) cognitively-normal people converting to mild cognitive impairment (MCI) and (2) cognitively-normal β-amyloid-positive (Aβ+) people. Specifically, we sought to identify... (More); Cognitively-normal people with evidence of β-amyloid (Aβ) pathology and subtle cognitive dysfunction are believed to be at high risk for progression to mild cognitive impairment due to Alzheimer's disease (AD). Clinical trials in later stages of AD typically include a coprimary endpoint to demonstrate efficacy on both cognitive and functional assessments. Recent trials focus on cognitively-normal people, but functional decline has not been explored for trial designs in this group. The goal of this study was therefore to characterize cognitive and functional decline in (1) cognitively-normal people converting to mild cognitive impairment (MCI) and (2) cognitively-normal β-amyloid-positive (Aβ+) people. Specifically, we sought to identify and compare the cognitive and functional assessments and their weighted combinations that maximize the longitudinal decline specific to these 2 groups. We studied 68 people who converted from normal cognition to MCI and 70 nonconverters, as well as 137 Aβ+ and 210 β-amyloid-negative cognitively-normal people. We used bootstrap aggregation and cross-validated mixed-models to estimate the distribution of weights applied to cognitive and functional outcomes to form composites. We also evaluated best subset optimization. Using optimized composites, we estimated statistical power for a variety of clinical trial scenarios. Overall, 55.4% of cognitively-normal to MCI converters were Aβ+. Large gains in power estimates were obtained when requiring participants to have both subtle cognitive dysfunction and Aβ pathology compared with requiring Aβ pathology alone. Additional power resulted when including functional as well as cognitive outcomes as part of the composite. Composites formed by applying equal weights to all measures provided the highest estimates of cross-validated power, although similar to both continuous weight optimization and best subset optimization. Using a composite to detect a 30% slowing of decline, 80% power was obtained for predicted Aβ+ converters with 375 completers/arm for a 30-month trial using a combination of cognitive/ functional measures. In the Aβ+ group, power to approach levels suitable for a phase III clinical trial would require considerably larger sample sizes. Composites incorporating both cognitive and functional measures may substantially increase the power of a trial in a preclinical (Aβ+) AD population with subtle evidence of cognitive dysfunction.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/99f1e2f1-340d-4f58-9eac-8f36b9a80e5b

author

Insel, Philip S. ^LU ; Donohue, Michael C. ; Mackin, R. Scott ; Aisen, Paul S. ; Hansson, Oskar ^LU

; Weiner, Michael W. and Mattsson, Niklas ^LU

organization

publishing date

2016-12

type

Contribution to journal

publication status

published

subject

keywords

Clinical trials, Cognition, Composite, Function, Mild cognitive impairment, β-amyloid

in

Neurobiology of Aging

volume

48

pages

10 pages

publisher

Elsevier

external identifiers

pmid:27710807
wos:000386977300018
scopus:84991609096

ISSN

0197-4580

DOI

10.1016/j.neurobiolaging.2016.08.017

language

English

LU publication?

yes

id

99f1e2f1-340d-4f58-9eac-8f36b9a80e5b

date added to LUP

2016-11-02 13:04:48

date last changed

2024-04-19 11:26:37

@article{99f1e2f1-340d-4f58-9eac-8f36b9a80e5b,
  abstract     = {{<p>Cognitively-normal people with evidence of β-amyloid (Aβ) pathology and subtle cognitive dysfunction are believed to be at high risk for progression to mild cognitive impairment due to Alzheimer's disease (AD). Clinical trials in later stages of AD typically include a coprimary endpoint to demonstrate efficacy on both cognitive and functional assessments. Recent trials focus on cognitively-normal people, but functional decline has not been explored for trial designs in this group. The goal of this study was therefore to characterize cognitive and functional decline in (1) cognitively-normal people converting to mild cognitive impairment (MCI) and (2) cognitively-normal β-amyloid-positive (Aβ+) people. Specifically, we sought to identify and compare the cognitive and functional assessments and their weighted combinations that maximize the longitudinal decline specific to these 2 groups. We studied 68 people who converted from normal cognition to MCI and 70 nonconverters, as well as 137 Aβ+ and 210 β-amyloid-negative cognitively-normal people. We used bootstrap aggregation and cross-validated mixed-models to estimate the distribution of weights applied to cognitive and functional outcomes to form composites. We also evaluated best subset optimization. Using optimized composites, we estimated statistical power for a variety of clinical trial scenarios. Overall, 55.4% of cognitively-normal to MCI converters were Aβ+. Large gains in power estimates were obtained when requiring participants to have both subtle cognitive dysfunction and Aβ pathology compared with requiring Aβ pathology alone. Additional power resulted when including functional as well as cognitive outcomes as part of the composite. Composites formed by applying equal weights to all measures provided the highest estimates of cross-validated power, although similar to both continuous weight optimization and best subset optimization. Using a composite to detect a 30% slowing of decline, 80% power was obtained for predicted Aβ+ converters with 375 completers/arm for a 30-month trial using a combination of cognitive/ functional measures. In the Aβ+ group, power to approach levels suitable for a phase III clinical trial would require considerably larger sample sizes. Composites incorporating both cognitive and functional measures may substantially increase the power of a trial in a preclinical (Aβ+) AD population with subtle evidence of cognitive dysfunction.</p>}},
  author       = {{Insel, Philip S. and Donohue, Michael C. and Mackin, R. Scott and Aisen, Paul S. and Hansson, Oskar and Weiner, Michael W. and Mattsson, Niklas}},
  issn         = {{0197-4580}},
  keywords     = {{Clinical trials; Cognition; Composite; Function; Mild cognitive impairment; β-amyloid}},
  language     = {{eng}},
  pages        = {{172--181}},
  publisher    = {{Elsevier}},
  series       = {{Neurobiology of Aging}},
  title        = {{Cognitive and functional changes associated with Aβ pathology and the progression to mild cognitive impairment}},
  url          = {{http://dx.doi.org/10.1016/j.neurobiolaging.2016.08.017}},
  doi          = {{10.1016/j.neurobiolaging.2016.08.017}},
  volume       = {{48}},
  year         = {{2016}},
}

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Cognitive and functional changes associated with Aβ pathology and the progression to mild cognitive impairment