Sharon J. Krinsky‐McHale scite author profile

Increasingly individuals with intellectual and developmental disabilities, including Down syndrome, are being targeted for clinical trials. However, a challenge exists in effectively evaluating the outcomes of these new pharmacological interventions. Few empirically evaluated, psychometrically sound outcome measures appropriate for use in clinical trials with individuals with Down syndrome have been identified. To address this challenge, the NIH assembled leading clinicians and scientists to review existing measures and identify those that currently are appropriate for trials; those that may be appropriate after expansion of age range addition of easier items, and/or downward extension of psychometric norms; and areas where new measures need to be developed. This paper focuses on measures in the areas of cognition and behavior.

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Chapter 4 Alzheimer's Disease in Adults with Down Syndrome

Zigman¹,

Devenny²,

Krinsky‐McHale³

et al. 2008

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Changes in explicit memory associated with early dementia in adults with Down’s syndrome

Krinsky‐McHale

Devenny

Silverman

2002

J intellect Disabil Res

107

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The Alzheimer's Biomarker Consortium‐Down Syndrome: Rationale and methodology

Handen

Lott

Christian

et al. 2020

Alzheimer's & Dementia: Diagnosis, Assessment &

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Introduction Adults with Down syndrome (DS) are at exceptionally high risk for Alzheimer's disease (AD), with virtually all individuals developing key neuropathological features by age 40. Identifying biomarkers of AD progression in DS can provide valuable insights into pathogenesis and suggest targets for disease modifying treatments. Methods We describe the development of a multi‐center, longitudinal study of biomarkers of AD in DS. The protocol includes longitudinal examination of clinical, cognitive, blood and cerebrospinal fluid‐based biomarkers, magnetic resonance imaging and positron emission tomography measures (at 16‐month intervals), as well as genetic modifiers of AD risk and progression. Results Approximately 400 individuals will be enrolled in the study (more than 370 to date). The methodological approach from the administrative, clinical, neuroimaging, omics, neuropathology, and statistical cores is provided. Discussion This represents the largest U.S.‐based, multi‐site, biomarker initiative of AD in DS. Findings can inform other multidisciplinary networks studying AD in the general population.

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Cued recall in early‐stage dementia in adults with Down's syndrome

Devenny

Zimmerli

Kittler

et al. 2002

J intellect Disabil Res

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