Your search keyword '"Thomas Scheidemantel"' showing total 3 results

1. Safety, efficacy, and tolerability of memantine for cognitive and adaptive outcome measures in adolescents and young adults with Down syndrome: a randomised, double-blind, placebo-controlled phase 2 trial

Author

Alberto C S Costa, Ana C Brandão, Richard Boada, Veridiana L Barrionuevo, Hudson G Taylor, Elizabeth Roth, Melissa R Stasko, Mark W Johnson, Fernanda F Assir, Maria P Roberto, Patrícia Salmona, Guilherme Abreu-Silveira, Ilya Bederman, Erin Prendergast, Anke Hüls, Sarina Abrishamcar, Zan Mustacchi, Thomas Scheidemantel, Nancy J Roizen, and Stephen Ruedrich

Subjects

Male, Young Adult, Cognition, Treatment Outcome, Adolescent, Double-Blind Method, Memantine, Humans, Female, Neurology (clinical), Down Syndrome

Abstract

Down syndrome is a chromosomal disorder with considerable neurodevelopmental impact and neurodegenerative morbidity. In a pilot trial in young adults with Down syndrome, memantine (a drug approved for Alzheimer's disease) showed a significant effect on a secondary measure of episodic memory. We aimed to test whether memantine would improve episodic memory in adolescents and young adults with Down syndrome.We did a randomised, double-blind, placebo-controlled phase 2 trial with a parallel design, stratified by age and sex. Participants (aged 15-32 years) with either trisomy 21 or complete unbalanced translocation of chromosome 21 and in general good health were recruited from the community at one site in Brazil and another in the USA. Participants were randomly assigned (1:1) to receive either memantine (20 mg/day orally) or placebo for 16 weeks. Computer-generated randomisation tables for both sites (allocating a placebo or drug label to each member of a unique pair of participants) were centrally produced by an independent statistician and were shared only with investigational pharmacists at participating sites until unblinding of the study. Participants and investigators were masked to treatment assignments. Neuropsychological assessments were done at baseline (T1) and week 16 (T2). The primary outcome measure was change from baseline to week 16 in the California Verbal Learning Test-second edition short-form (CVLT-II-sf) total free recall score, assessed in the per-protocol population (ie, participants who completed 16 weeks of treatment and had neuropsychological assessments at T1 and T2). Linear mixed effect models were fit to data from the per-protocol population. Safety and tolerability were monitored and analysed in all participants who started treatment. Steady-state concentrations in plasma of memantine were measured at the end of the trial. This study is registered at ClinicalTrials.gov, number NCT02304302.From May 13, 2015, to July 22, 2020, 185 participants with Down syndrome were assessed for eligibility and 160 (86%) were randomly assigned either memantine (n=81) or placebo (n=79). All participants received their allocated treatment. Linear mixed effect models were fit to data from 149 (81%) participants, 73 in the memantine group and 76 in the placebo group, after 11 people (eight in the memantine group and three in the placebo group) discontinued due to COVID-19 restrictions, illness of their caregiver, adverse events, or low compliance. The primary outcome measure did not differ between groups (CVLT-II-sf total free recall score, change from baseline 0·34 points [95% CI -0·98 to 1·67], p=0·61). Memantine was well tolerated, with infrequent mild-to-moderate adverse events, the most common being viral upper respiratory infection (nine [11%] participants in the memantine group and 12 [15%] in the placebo group) and transient dizziness (eight [10%] in the memantine group and six [8%] in the placebo group). No serious adverse events were observed. Amounts of memantine in plasma were substantially lower than those considered therapeutic for Alzheimer's disease.Memantine was well tolerated, but cognition-enhancing effects were not recorded with a 20 mg/day dose in adolescents and young adults with Down syndrome. Exploratory analyses point to a need for future work.Alana Foundation.For the Portuguese translation of the abstract see Supplementary Materials section.

Published

2021

2. Hippocampal subfield volume differences are independent of age in teenagers and young adults with Down syndrome

Author

Anne Birnbaum, Katherine A. Koenig, Melissa R. Stasko, Emma Lissemore, Se-Hong Oh, Nancy J. Roizen, Stephen Ruedrich, H. G. Taylor, James B. Leverenz, Thomas Scheidemantel, Elizabeth Roth, and Alberto C.S. Costa

Subjects

Down syndrome, Epidemiology, business.industry, Health Policy, Anatomy, Hippocampal formation, medicine.disease, Temporal lobe, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Neuroimaging, medicine, Neurology (clinical), Geriatrics and Gerontology, Young adult, business, Volume (compression)

Published

2020

3. Cross-Sectional Exploration of Plasma Biomarkers of Alzheimer’s Disease in Down Syndrome: Early Data from the Longitudinal Investigation for Enhancing Down Syndrome Research (LIFE-DSR) Study

Author

Kristi Wilmes, Jason Woodward, Carolyn Revta, Tatiana Foroud, Kavita Krell, Priya S. Kishnani, James Hendrix, H. Diana Rosas, Hampus Hillerstrom, Amy Talboy, Kelley Faber, Casey L. Evans, Jennifer Mason, Frederick A. Schmitt, Jennifer A. Zimmer, Jessie Nicodemus-Johnson, Sarah J. Hart, Anna J. Esbensen, Howard Feldman, Jeffrey L. Dage, Cesar Ochoa-Lubinoff, Amy Torres, Melissa R. Stasko, David C. Airey, Anna D. Burke, Stephanie L. Santoro, Suzanne Hendrix, Ira T. Lott, Elizabeth Head, Angela Britton, Brian G. Skotko, Kelsey Haugen, Alberto C.S. Costa, Brian Chicoine, Duvia Lara Ledesma, Kim Schafer, Florence Lai, Jacqueline Chen, Ronelyn Chavez, Margaret B. Pulsifer, Nicholas K. Proctor, George T. Capone, William C. Mobley, Thomas Scheidemantel, Tracie C. Rosser, and Eric Doran

Subjects

Oncology, Aging, Longitudinal study, Down syndrome, Down syndrome research, Disease, Neurodegenerative, Alzheimer's Disease, 0302 clinical medicine, 2.1 Biological and endogenous factors, Aetiology, amyloid β peptide, screening and diagnosis, 0303 health sciences, education.field_of_study, medicine.diagnostic_test, blood biomarkers, General Medicine, peptide, Detection, neurofilament light chain, glial fibrillary acidic protein, Neurological, Medicine, Biomarker (medicine), Alzheimer’s disease, Natural history study, medicine.medical_specialty, Intellectual and Developmental Disabilities (IDD), Clinical Sciences, Population, Article, s disease, 03 medical and health sciences, Mental status examination, phosphorylated tau protein, amyloid &#946, Internal medicine, Acquired Cognitive Impairment, medicine, Alzheimer&#8217, education, 030304 developmental biology, business.industry, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), medicine.disease, Brain Disorders, 4.1 Discovery and preclinical testing of markers and technologies, Dementia, business, 030217 neurology & neurosurgery

Abstract

With improved healthcare, the Down syndrome (DS) population is both growing and aging rapidly. However, with longevity comes a very high risk of Alzheimer’s disease (AD). The LIFE-DSR study (NCT04149197) is a longitudinal natural history study recruiting 270 adults with DS over the age of 25. The study is designed to characterize trajectories of change in DS-associated AD (DS-AD). The current study reports its cross-sectional analysis of the first 90 subjects enrolled. Plasma biomarkers phosphorylated tau protein (p-tau), neurofilament light chain (NfL), amyloid β peptides (Aβ1-40, Aβ1-42), and glial fibrillary acidic protein (GFAP) were undertaken with previously published methods. The clinical data from the baseline visit include demographics as well as the cognitive measures under the Severe Impairment Battery (SIB) and Down Syndrome Mental Status Examination (DS-MSE). Biomarker distributions are described with strong statistical associations observed with participant age. The biomarker data contributes to understanding DS-AD across the spectrum of disease. Collectively, the biomarker data show evidence of DS-AD progression beginning at approximately 40 years of age. Exploring these data across the full LIFE-DSR longitudinal study population will be an important resource in understanding the onset, progression, and clinical profiles of DS-AD pathophysiology.

Published

2021