Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits

Synaptic dysfunction and loss caused by age-dependent accumulation of synaptotoxic beta amyloid (Abeta) 1–42 oligomers is proposed to underlie cognitive decline in Alzheimer's disease (AD). Alterations in membrane trafficking induced by Abeta oligomers mediates reduction in neuronal surface rec...

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Autores principales: Izzo, Nicholas J., Staniszewski, Agnes, To, Lillian, Fa, Mauro, Teich, Andrew F., Saeed, Faisal, Wostein, Harrison, Walko, Thomas, Vaswani, Anisha, Wardius, Meghan, Syed, Zanobia, Ravenscroft, Jessica, Mozzoni, Kelsie, Silky, Colleen, Rehak, Courtney, Yurko, Raymond, Finn, Patricia, Look, Gary, Rishton, Gilbert, Safferstein, Hank, Miller, Miles, Johanson, Conrad, Stopa, Edward, Windisch, Manfred, Hutter-Paier, Birgit, Shamloo, Mehrdad, Arancio, Ottavio, LeVine, Harry, Catalano, Susan M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4229098/
https://www.ncbi.nlm.nih.gov/pubmed/25390368
http://dx.doi.org/10.1371/journal.pone.0111898
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author Izzo, Nicholas J.
Staniszewski, Agnes
To, Lillian
Fa, Mauro
Teich, Andrew F.
Saeed, Faisal
Wostein, Harrison
Walko, Thomas
Vaswani, Anisha
Wardius, Meghan
Syed, Zanobia
Ravenscroft, Jessica
Mozzoni, Kelsie
Silky, Colleen
Rehak, Courtney
Yurko, Raymond
Finn, Patricia
Look, Gary
Rishton, Gilbert
Safferstein, Hank
Miller, Miles
Johanson, Conrad
Stopa, Edward
Windisch, Manfred
Hutter-Paier, Birgit
Shamloo, Mehrdad
Arancio, Ottavio
LeVine, Harry
Catalano, Susan M.
author_facet Izzo, Nicholas J.
Staniszewski, Agnes
To, Lillian
Fa, Mauro
Teich, Andrew F.
Saeed, Faisal
Wostein, Harrison
Walko, Thomas
Vaswani, Anisha
Wardius, Meghan
Syed, Zanobia
Ravenscroft, Jessica
Mozzoni, Kelsie
Silky, Colleen
Rehak, Courtney
Yurko, Raymond
Finn, Patricia
Look, Gary
Rishton, Gilbert
Safferstein, Hank
Miller, Miles
Johanson, Conrad
Stopa, Edward
Windisch, Manfred
Hutter-Paier, Birgit
Shamloo, Mehrdad
Arancio, Ottavio
LeVine, Harry
Catalano, Susan M.
author_sort Izzo, Nicholas J.
collection PubMed
description Synaptic dysfunction and loss caused by age-dependent accumulation of synaptotoxic beta amyloid (Abeta) 1–42 oligomers is proposed to underlie cognitive decline in Alzheimer's disease (AD). Alterations in membrane trafficking induced by Abeta oligomers mediates reduction in neuronal surface receptor expression that is the basis for inhibition of electrophysiological measures of synaptic plasticity and thus learning and memory. We have utilized phenotypic screens in mature, in vitro cultures of rat brain cells to identify small molecules which block or prevent the binding and effects of Abeta oligomers. Synthetic Abeta oligomers bind saturably to a single site on neuronal synapses and induce deficits in membrane trafficking in neuronal cultures with an EC(50) that corresponds to its binding affinity. The therapeutic lead compounds we have found are pharmacological antagonists of Abeta oligomers, reducing the binding of Abeta oligomers to neurons in vitro, preventing spine loss in neurons and preventing and treating oligomer-induced deficits in membrane trafficking. These molecules are highly brain penetrant and prevent and restore cognitive deficits in mouse models of Alzheimer's disease. Counter-screening these compounds against a broad panel of potential CNS targets revealed they are highly potent and specific ligands of the sigma-2/PGRMC1 receptor. Brain concentrations of the compounds corresponding to greater than 80% receptor occupancy at the sigma-2/PGRMC1 receptor restore cognitive function in transgenic hAPP Swe/Ldn mice. These studies demonstrate that synthetic and human-derived Abeta oligomers act as pharmacologically-behaved ligands at neuronal receptors - i.e. they exhibit saturable binding to a target, they exert a functional effect related to their binding and their displacement by small molecule antagonists blocks their functional effect. The first-in-class small molecule receptor antagonists described here restore memory to normal in multiple AD models and sustain improvement long-term, representing a novel mechanism of action for disease-modifying Alzheimer's therapeutics.
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spelling pubmed-42290982014-11-18 Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits Izzo, Nicholas J. Staniszewski, Agnes To, Lillian Fa, Mauro Teich, Andrew F. Saeed, Faisal Wostein, Harrison Walko, Thomas Vaswani, Anisha Wardius, Meghan Syed, Zanobia Ravenscroft, Jessica Mozzoni, Kelsie Silky, Colleen Rehak, Courtney Yurko, Raymond Finn, Patricia Look, Gary Rishton, Gilbert Safferstein, Hank Miller, Miles Johanson, Conrad Stopa, Edward Windisch, Manfred Hutter-Paier, Birgit Shamloo, Mehrdad Arancio, Ottavio LeVine, Harry Catalano, Susan M. PLoS One Research Article Synaptic dysfunction and loss caused by age-dependent accumulation of synaptotoxic beta amyloid (Abeta) 1–42 oligomers is proposed to underlie cognitive decline in Alzheimer's disease (AD). Alterations in membrane trafficking induced by Abeta oligomers mediates reduction in neuronal surface receptor expression that is the basis for inhibition of electrophysiological measures of synaptic plasticity and thus learning and memory. We have utilized phenotypic screens in mature, in vitro cultures of rat brain cells to identify small molecules which block or prevent the binding and effects of Abeta oligomers. Synthetic Abeta oligomers bind saturably to a single site on neuronal synapses and induce deficits in membrane trafficking in neuronal cultures with an EC(50) that corresponds to its binding affinity. The therapeutic lead compounds we have found are pharmacological antagonists of Abeta oligomers, reducing the binding of Abeta oligomers to neurons in vitro, preventing spine loss in neurons and preventing and treating oligomer-induced deficits in membrane trafficking. These molecules are highly brain penetrant and prevent and restore cognitive deficits in mouse models of Alzheimer's disease. Counter-screening these compounds against a broad panel of potential CNS targets revealed they are highly potent and specific ligands of the sigma-2/PGRMC1 receptor. Brain concentrations of the compounds corresponding to greater than 80% receptor occupancy at the sigma-2/PGRMC1 receptor restore cognitive function in transgenic hAPP Swe/Ldn mice. These studies demonstrate that synthetic and human-derived Abeta oligomers act as pharmacologically-behaved ligands at neuronal receptors - i.e. they exhibit saturable binding to a target, they exert a functional effect related to their binding and their displacement by small molecule antagonists blocks their functional effect. The first-in-class small molecule receptor antagonists described here restore memory to normal in multiple AD models and sustain improvement long-term, representing a novel mechanism of action for disease-modifying Alzheimer's therapeutics. Public Library of Science 2014-11-12 /pmc/articles/PMC4229098/ /pubmed/25390368 http://dx.doi.org/10.1371/journal.pone.0111898 Text en © 2014 Izzo et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Izzo, Nicholas J.
Staniszewski, Agnes
To, Lillian
Fa, Mauro
Teich, Andrew F.
Saeed, Faisal
Wostein, Harrison
Walko, Thomas
Vaswani, Anisha
Wardius, Meghan
Syed, Zanobia
Ravenscroft, Jessica
Mozzoni, Kelsie
Silky, Colleen
Rehak, Courtney
Yurko, Raymond
Finn, Patricia
Look, Gary
Rishton, Gilbert
Safferstein, Hank
Miller, Miles
Johanson, Conrad
Stopa, Edward
Windisch, Manfred
Hutter-Paier, Birgit
Shamloo, Mehrdad
Arancio, Ottavio
LeVine, Harry
Catalano, Susan M.
Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title_full Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title_fullStr Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title_full_unstemmed Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title_short Alzheimer's Therapeutics Targeting Amyloid Beta 1–42 Oligomers I: Abeta 42 Oligomer Binding to Specific Neuronal Receptors Is Displaced by Drug Candidates That Improve Cognitive Deficits
title_sort alzheimer's therapeutics targeting amyloid beta 1–42 oligomers i: abeta 42 oligomer binding to specific neuronal receptors is displaced by drug candidates that improve cognitive deficits
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4229098/
https://www.ncbi.nlm.nih.gov/pubmed/25390368
http://dx.doi.org/10.1371/journal.pone.0111898
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