The Alzheimer’s Prevention Initiative Composite Cognitive Test Score

Ayutyanont, Napatkamon; Langbaum, Jessica B.; Hendrix, Suzanne; Chen, Kewei; Fleisher, Adam; Friesenhahn, Michel; Ward, Michael E.; Aguirre, Carlos; Acosta‐Baena, Natalia; Madrigal, Lucía; Muñoz, Claudia; Tirado, Victoria; Moreno, Sonia; Tariot, Pierre N.; Lopera, Francisco; Reiman, Eric M.

doi:10.4088/jcp.13m08927

Cited by 71 publications

(42 citation statements)

References 39 publications

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“…This API composite cognitive test score and the approach taken to develop it appears to fit into the framework provided by the Food and Drug Administration’s recent draft guidance concerning a cognitive assessment serving as a primary efficacy measure in preclinical AD trials (51). Moreover, the composite identified in the present study was comprised of the same cognitive domains/assessments with the exception of one (present study included a test of visual spatial ability – Symbol Digits Modalities ) as a composite cognitive endpoint identified in cognitively healthy ADAD mutation carriers, despite substantial differences in the cohorts’ neuropsychological test batteries (52). This consistency is noteworthy as confirmation of the composite’s performance in an independent population, as well as suggesting that there is extensive overlap in the pattern of cognitive decline between the two forms of the disease even though they strike at different ages, and may have different preclinical and clinical time courses, underlying etiologies, and biological processes.…”

Section: Discussionmentioning

confidence: 99%

An empirically derived composite cognitive test score with improved power to track and evaluate treatments for preclinical Alzheimer's disease

Langbaum¹,

Hendrix

Ayutyanont³

et al. 2014

Alzheimer's & Dementia

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Background There is growing interest in the evaluation of preclinical Alzheimer’s disease (AD) treatments. As a result, there is a need to identify a cognitive composite that is sensitive to tracking preclinical AD decline to be used as a primary endpoint in treatment trials. Methods Longitudinal data from initially cognitively normal, 70–85 year old participants in three cohort studies of aging and dementia from the Rush Alzheimer’s Disease Center were examined to empirically define a composite cognitive endpoint that is sensitive to detecting and tracking cognitive decline prior to the onset of cognitive impairment. The mean to standard deviation ratios (MSDR) of change over time were calculated in a search for the optimal combination of cognitive tests/sub-tests drawn from the neuropsychological battery in cognitively normal participants who subsequently progressed to clinical stages of AD during a two and five year period, using data from those who remained unimpaired during the same time period to correct for aging and practice effects. Combinations that performed well were then evaluated for representation of relevant cognitive domains, robustness across individual years prior to diagnosis, and occurrence of selected items within top performing combinations. Results The optimal composite cognitive test score is comprised of 7 cognitive tests/sub-tests with an MSDR=0.964. By comparison, the most sensitive individual test score, Logical Memory – Delayed Recall, MSDR= 0.64. Conclusions We have identified a composite cognitive test score representing multiple cognitive domains that has improved power compared to the most sensitive single test item to track preclinical AD decline and evaluate preclinical AD treatments. We are confirming the power of the composite in independent cohorts, and with other analytical approaches, which may result in refinements, and have designated it as the primary endpoint in the Alzheimer’s Prevention Initiative’s preclinical treatment trials for individuals at high imminent risk for developing symptoms due to late-onset AD.

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Section: Discussionmentioning

confidence: 99%

An empirically derived composite cognitive test score with improved power to track and evaluate treatments for preclinical Alzheimer's disease

Langbaum¹,

Hendrix

Ayutyanont³

et al. 2014

Alzheimer's & Dementia

Self Cite

111

140

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“…Whereas ongoing clinical trials on early stage AD such as the A4 trial and the API trial have proposed differing cognitive composites using the same weights across multiple cognitive domains [17, 23], we sought to improve these by mathematically optimizing the weights so that the sample sizes for adequately powering such trials could be minimized. We proposed a multivariate mixed model for repeated measures to jointly model the longitudinal progression of multiple outcomes.…”

Section: Discussionmentioning

confidence: 99%

“…A large cognitive battery has been administered in DIAN participants [45], covering a wide range of domains. Based on recent reports on cognitive domains that may exhibit early progression from the ongoing A4 trial [17] and the API trial [23] as well as a preliminary analysis on the DIAN database, to demonstrate the application of our proposed methodology, we have chosen the following six candidates of the cognitive tests that can be considered for powering the upcoming Phase III cognitive endpoint trial: the total score of the MMSE [21], a widely used screening test that evaluates overall cognitive function by examining orientation to place, orientation to time, attention, concentration, language, ability to recall previously given words and visual-spatial skills. The Score of MMSE ranges from 0 to 30 [21];…”

Section: Designing Clinical Trials On Autosomal Dominant Alzheimer DImentioning

confidence: 99%

“…In the API trial, the proposed cognitive composite is also equally weighted among the following individual tests over multiple cognitive domains [23]: Consortium to Establish a Registry for Alzheimer's Disease (CERAD) Word List Recall, CERAD Boston Naming Test (high frequency items), MMSE Orientation to Time, CERAD Constructional Praxis, and Raven's Progressive Matrices (Set A) [24-27]. It is reported that the proposed composite is more sensitive than using the entire CERAD battery [23]. Whereas each of the proposed cognitive composite score weighs multiple tests equally, and has performed reasonably well, it remains unknown whether they provide the optimum power for designing RCTs on early stage AD.…”

Section: Introductionmentioning

confidence: 99%

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Linear combinations of multiple outcome measures to improve the power of efficacy analysis – application to clinical trials on early-stage Alzheimer's disease

Xiong

Luo

Morris

et al. 2017

Biostatistics & Epidemiology

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Modern clinical trials on Alzheimer disease (AD) focus on the early symptomatic stage or even the preclinical stage. Subtle disease progression at the early stages, however, poses a major challenge in designing such clinical trials. We propose a multivariate mixed model on repeated measures to model the disease progression over time on multiple efficacy outcomes, and derive the optimum weights to combine multiple outcome measures by minimizing the sample sizes to adequately power the clinical trials. A cross-validation simulation study is conducted to assess the accuracy for the estimated weights as well as the improvement in reducing the sample sizes for such trials. The proposed methodology is applied to the multiple cognitive tests from the ongoing observational study of the Dominantly Inherited Alzheimer Network (DIAN) to power future clinical trials in the DIAN with a cognitive endpoint. Our results show that the optimum weights to combine multiple outcome measures can be accurately estimated, and that compared to the individual outcomes, the combined efficacy outcome with these weights significantly reduces the sample size required to adequately power clinical trials. When applied to the clinical trial in the DIAN, the estimated linear combination of six cognitive tests can adequately power the clinical trial.

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“…time-to-AD conversion, may not be suitable for these early trials (1). While several groups are developing new composite cognitive tests that could serve as surrogate outcome measures by detecting subtle cognitive changes in normal people (2, 15), there is a need for longitudinal brain imaging techniques that can correlate with temporal changes in these new tests and provide additional objective measures of neuropathological changes in brain. In particular, within-individual longitudinal comparisons of imaging data may improve these evaluations by controlling for between subject variability.…”

Section: Introductionmentioning

confidence: 99%

Longitudinal Positron Emission Tomography in Preventive Alzheimer's Disease Drug Trials, Critical Barriers from Imaging Science Perspective

Shokouhi¹,

Campbell²,

Brill³

et al. 2016

Brain Pathology

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Recent Alzheimer’s trials have recruited cognitively normal people at risk for Alzheimer’s dementia. Due to the lack of clinical symptoms in normal population, conventional clinical outcome measures are not suitable for these early trials. While several groups are developing new composite cognitive tests that could serve as potential outcome measures by detecting subtle cognitive changes in normal people, there is a need for longitudinal brain imaging techniques that can correlate with temporal changes in these new tests and provide additional objective measures of neuropathological changes in brain. Positron emission tomography (PET) is a nuclear medicine imaging procedure based on the measurement of annihilation photons after positron emission from radiolabeled molecules that allow tracking of biological processes in body, including the brain. PET is a well-established in vivo imaging modality in Alzheimer’s disease diagnosis and research due to its capability of detecting abnormalities in three major hallmarks of this disease. These include 1) amyloid beta plaques, 2) neurofibrillary tau tangles and 3) decrease in neuronal activity due to loss of nerve cell connection and death. While semi-quantitative PET imaging techniques are commonly used to set discrete cut-points to stratify abnormal levels of amyloid accumulation and neurodegeneration, they are sub-optimal for detecting subtle longitudinal changes. In this study, we have identified and discussed four critical barriers in conventional longitudinal PET imaging that may be particularly relevant for early Alzheimer’s disease studies. These include within and across subject heterogeneity of AD-affected brain regions, PET intensity normalization, neuronal compensations in early disease stages and cerebrovascular amyloid deposition.

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The Alzheimer’s Prevention Initiative Composite Cognitive Test Score

Cited by 71 publications

References 39 publications

An empirically derived composite cognitive test score with improved power to track and evaluate treatments for preclinical Alzheimer's disease

An empirically derived composite cognitive test score with improved power to track and evaluate treatments for preclinical Alzheimer's disease

Linear combinations of multiple outcome measures to improve the power of efficacy analysis – application to clinical trials on early-stage Alzheimer's disease

Longitudinal Positron Emission Tomography in Preventive Alzheimer's Disease Drug Trials, Critical Barriers from Imaging Science Perspective

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