A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design

BACKGROUND: The rise of direct-to-consumer genetic testing has enabled many to learn of their possible increased risk for rare diseases, some of which may be suitable for gene-targeted therapies. However, recruiting a large and representative population for rare diseases or genetically defined sub-p...

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Autores principales: Schneider, Ruth B., Myers, Taylor L., Rowbotham, Helen M., Luff, Marie K., Amodeo, Katherine, Sharma, Saloni, Wilson, Renee, Jensen-Roberts, Stella, Auinger, Peggy, McDermott, Michael P., Alcalay, Roy N., Biglan, Kevin, Kinel, Daniel, Tanner, Caroline, Winter-Evans, Reni, Augustine, Erika F., Cannon, Paul, Holloway, Robert G., Dorsey, E. Ray
Formato: Online Artículo Texto
Lenguaje:English
Publicado: IOS Press 2020
Materias:
Research Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7505001/
https://www.ncbi.nlm.nih.gov/pubmed/32568109
http://dx.doi.org/10.3233/JPD-202019
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author Schneider, Ruth B.
Myers, Taylor L.
Rowbotham, Helen M.
Luff, Marie K.
Amodeo, Katherine
Sharma, Saloni
Wilson, Renee
Jensen-Roberts, Stella
Auinger, Peggy
McDermott, Michael P.
Alcalay, Roy N.
Biglan, Kevin
Kinel, Daniel
Tanner, Caroline
Winter-Evans, Reni
Augustine, Erika F.
Cannon, Paul
Holloway, Robert G.
Dorsey, E. Ray
author_facet Schneider, Ruth B.
Myers, Taylor L.
Rowbotham, Helen M.
Luff, Marie K.
Amodeo, Katherine
Sharma, Saloni
Wilson, Renee
Jensen-Roberts, Stella
Auinger, Peggy
McDermott, Michael P.
Alcalay, Roy N.
Biglan, Kevin
Kinel, Daniel
Tanner, Caroline
Winter-Evans, Reni
Augustine, Erika F.
Cannon, Paul
Holloway, Robert G.
Dorsey, E. Ray
author_sort Schneider, Ruth B.
collection PubMed
description BACKGROUND: The rise of direct-to-consumer genetic testing has enabled many to learn of their possible increased risk for rare diseases, some of which may be suitable for gene-targeted therapies. However, recruiting a large and representative population for rare diseases or genetically defined sub-populations of common diseases is slow, difficult, and expensive. OBJECTIVE: To assess the feasibility of recruiting and retaining a cohort of individuals who carry a genetic mutation linked to Parkinson’s disease (G2019S variant of LRRK2); to characterize this cohort relative to the characteristics of traditional, in-person studies; and to evaluate this model’s ability to create an engaged study cohort interested in future clinical trials of gene-directed therapies. METHODS: This single-site,3-year national longitudinal observational study will recruit between 250 to 350 LRRK2 carriers without Parkinson’s disease and approximately 50 with the condition. Participants must have undergone genetic testing by the personal genetics company, 23andMe, Inc., have knowledge of their carrier status, and consent to be contacted for research studies. All participants undergo standardized assessments, including video-based cognitive and motor examination, and complete patient-reported outcomes on an annual basis. RESULTS: 263 individuals living in 33 states have enrolled. The cohort has a mean (SD) age of 56.0 (15.9) years, 59% are female, and 76% are of Ashkenazi Jewish descent. 233 have completed the baseline visit: 47 with self-reported Parkinson’s disease and 186 without. CONCLUSIONS: This study establishes a promising model for developing a geographically dispersed and well-characterized cohort ready for participation in future clinical trials of gene-directed therapies.
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spelling pubmed-75050012020-10-06 A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design Schneider, Ruth B. Myers, Taylor L. Rowbotham, Helen M. Luff, Marie K. Amodeo, Katherine Sharma, Saloni Wilson, Renee Jensen-Roberts, Stella Auinger, Peggy McDermott, Michael P. Alcalay, Roy N. Biglan, Kevin Kinel, Daniel Tanner, Caroline Winter-Evans, Reni Augustine, Erika F. Cannon, Paul Holloway, Robert G. Dorsey, E. Ray J Parkinsons Dis Research Report BACKGROUND: The rise of direct-to-consumer genetic testing has enabled many to learn of their possible increased risk for rare diseases, some of which may be suitable for gene-targeted therapies. However, recruiting a large and representative population for rare diseases or genetically defined sub-populations of common diseases is slow, difficult, and expensive. OBJECTIVE: To assess the feasibility of recruiting and retaining a cohort of individuals who carry a genetic mutation linked to Parkinson’s disease (G2019S variant of LRRK2); to characterize this cohort relative to the characteristics of traditional, in-person studies; and to evaluate this model’s ability to create an engaged study cohort interested in future clinical trials of gene-directed therapies. METHODS: This single-site,3-year national longitudinal observational study will recruit between 250 to 350 LRRK2 carriers without Parkinson’s disease and approximately 50 with the condition. Participants must have undergone genetic testing by the personal genetics company, 23andMe, Inc., have knowledge of their carrier status, and consent to be contacted for research studies. All participants undergo standardized assessments, including video-based cognitive and motor examination, and complete patient-reported outcomes on an annual basis. RESULTS: 263 individuals living in 33 states have enrolled. The cohort has a mean (SD) age of 56.0 (15.9) years, 59% are female, and 76% are of Ashkenazi Jewish descent. 233 have completed the baseline visit: 47 with self-reported Parkinson’s disease and 186 without. CONCLUSIONS: This study establishes a promising model for developing a geographically dispersed and well-characterized cohort ready for participation in future clinical trials of gene-directed therapies. IOS Press 2020-07-28 /pmc/articles/PMC7505001/ /pubmed/32568109 http://dx.doi.org/10.3233/JPD-202019 Text en © 2020 – IOS Press and the authors. All rights reserved https://creativecommons.org/licenses/by-nc/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution Non-Commercial (CC BY-NC 4.0) License (https://creativecommons.org/licenses/by-nc/4.0/) , which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Report
Schneider, Ruth B.
Myers, Taylor L.
Rowbotham, Helen M.
Luff, Marie K.
Amodeo, Katherine
Sharma, Saloni
Wilson, Renee
Jensen-Roberts, Stella
Auinger, Peggy
McDermott, Michael P.
Alcalay, Roy N.
Biglan, Kevin
Kinel, Daniel
Tanner, Caroline
Winter-Evans, Reni
Augustine, Erika F.
Cannon, Paul
Holloway, Robert G.
Dorsey, E. Ray
A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title_full A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title_fullStr A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title_full_unstemmed A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title_short A Virtual Cohort Study of Individuals at Genetic Risk for Parkinson’s Disease: Study Protocol and Design
title_sort virtual cohort study of individuals at genetic risk for parkinson’s disease: study protocol and design
topic Research Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7505001/
https://www.ncbi.nlm.nih.gov/pubmed/32568109
http://dx.doi.org/10.3233/JPD-202019
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