A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug

A growing body of evidence supports the ‘calcium hypothesis’ of Alzheimer’s disease (AD), which postulates that a variety of insults might disrupt the homeostatic regulation of neuronal calcium (Ca(2+)) in the brain, resulting in the progressive symptoms that typify the disease. However, despite ong...

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Autores principales: Copenhaver, Philip F., Anekonda, Thimmappa S., Musashe, Derek, Robinson, Kristine M., Ramaker, Jenna M., Swanson, Tracy L., Wadsworth, Teri L., Kretzschmar, Doris, Woltjer, Randall L., Quinn, Joseph F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Limited 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3180227/
https://www.ncbi.nlm.nih.gov/pubmed/21596710
http://dx.doi.org/10.1242/dmm.006841
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author Copenhaver, Philip F.
Anekonda, Thimmappa S.
Musashe, Derek
Robinson, Kristine M.
Ramaker, Jenna M.
Swanson, Tracy L.
Wadsworth, Teri L.
Kretzschmar, Doris
Woltjer, Randall L.
Quinn, Joseph F.
author_facet Copenhaver, Philip F.
Anekonda, Thimmappa S.
Musashe, Derek
Robinson, Kristine M.
Ramaker, Jenna M.
Swanson, Tracy L.
Wadsworth, Teri L.
Kretzschmar, Doris
Woltjer, Randall L.
Quinn, Joseph F.
author_sort Copenhaver, Philip F.
collection PubMed
description A growing body of evidence supports the ‘calcium hypothesis’ of Alzheimer’s disease (AD), which postulates that a variety of insults might disrupt the homeostatic regulation of neuronal calcium (Ca(2+)) in the brain, resulting in the progressive symptoms that typify the disease. However, despite ongoing efforts to develop new methods for testing therapeutic compounds that might be beneficial in AD, no single bioassay permits both rapid screening and in vivo validation of candidate drugs that target specific components of the Ca(2+) regulatory machinery. To address this issue, we have integrated four distinct model systems that provide complementary information about a trial compound: the human neuroblastoma MC65 line, which provides an in vitro model of amyloid toxicity; a transgenic Drosophila model, which develops age-dependent pathologies associated with AD; the 3×TgAD transgenic mouse, which recapitulates many of the neuropathological features that typify AD; and the embryonic nervous system of Manduca, which provides a novel in vivo assay for the acute effects of amyloid peptides on neuronal motility. To demonstrate the value of this ‘translational suite’ of bioassays, we focused on a set of clinically approved dihydropyridines (DHPs), a class of well-defined inhibitors of L-type calcium channels that have been suggested to be neuroprotective in AD. Among the DHPs tested in this study, we found that isradipine reduced the neurotoxic consequences of β-amyloid accumulation in all four model systems without inducing deleterious side effects. Our results provide new evidence in support of the Ca(2+) hypothesis of AD, and indicate that isradipine represents a promising drug for translation into clinical trials. In addition, these studies also demonstrate that this continuum of bioassays (representing different levels of complexity) provides an effective means of evaluating other candidate compounds that target specific components of the Ca(2+) regulatory machinery and that therefore might be beneficial in the treatment of AD.
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spelling pubmed-31802272011-09-30 A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug Copenhaver, Philip F. Anekonda, Thimmappa S. Musashe, Derek Robinson, Kristine M. Ramaker, Jenna M. Swanson, Tracy L. Wadsworth, Teri L. Kretzschmar, Doris Woltjer, Randall L. Quinn, Joseph F. Dis Model Mech Research Article A growing body of evidence supports the ‘calcium hypothesis’ of Alzheimer’s disease (AD), which postulates that a variety of insults might disrupt the homeostatic regulation of neuronal calcium (Ca(2+)) in the brain, resulting in the progressive symptoms that typify the disease. However, despite ongoing efforts to develop new methods for testing therapeutic compounds that might be beneficial in AD, no single bioassay permits both rapid screening and in vivo validation of candidate drugs that target specific components of the Ca(2+) regulatory machinery. To address this issue, we have integrated four distinct model systems that provide complementary information about a trial compound: the human neuroblastoma MC65 line, which provides an in vitro model of amyloid toxicity; a transgenic Drosophila model, which develops age-dependent pathologies associated with AD; the 3×TgAD transgenic mouse, which recapitulates many of the neuropathological features that typify AD; and the embryonic nervous system of Manduca, which provides a novel in vivo assay for the acute effects of amyloid peptides on neuronal motility. To demonstrate the value of this ‘translational suite’ of bioassays, we focused on a set of clinically approved dihydropyridines (DHPs), a class of well-defined inhibitors of L-type calcium channels that have been suggested to be neuroprotective in AD. Among the DHPs tested in this study, we found that isradipine reduced the neurotoxic consequences of β-amyloid accumulation in all four model systems without inducing deleterious side effects. Our results provide new evidence in support of the Ca(2+) hypothesis of AD, and indicate that isradipine represents a promising drug for translation into clinical trials. In addition, these studies also demonstrate that this continuum of bioassays (representing different levels of complexity) provides an effective means of evaluating other candidate compounds that target specific components of the Ca(2+) regulatory machinery and that therefore might be beneficial in the treatment of AD. The Company of Biologists Limited 2011-09 2011-05-19 /pmc/articles/PMC3180227/ /pubmed/21596710 http://dx.doi.org/10.1242/dmm.006841 Text en © 2011. Published by The Company of Biologists Ltd This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial Share Alike License (http://creativecommons.org/licenses/by-nc-sa/3.0), which permits unrestricted non-commercial use, distribution and reproduction in any medium provided that the original work is properly cited and all further distributions of the work or adaptation are subject to the same Creative Commons License terms.
spellingShingle Research Article
Copenhaver, Philip F.
Anekonda, Thimmappa S.
Musashe, Derek
Robinson, Kristine M.
Ramaker, Jenna M.
Swanson, Tracy L.
Wadsworth, Teri L.
Kretzschmar, Doris
Woltjer, Randall L.
Quinn, Joseph F.
A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title_full A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title_fullStr A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title_full_unstemmed A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title_short A translational continuum of model systems for evaluating treatment strategies in Alzheimer’s disease: isradipine as a candidate drug
title_sort translational continuum of model systems for evaluating treatment strategies in alzheimer’s disease: isradipine as a candidate drug
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3180227/
https://www.ncbi.nlm.nih.gov/pubmed/21596710
http://dx.doi.org/10.1242/dmm.006841
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