Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice

See Mercado and Hetz (doi:10.1093/brain/awx107) for a scientific commentary on this article. Signalling through the PERK/eIF2α-P branch of the unfolded protein response plays a critical role in controlling protein synthesis rates in cells. This pathway is overactivated in brains of patient...

Descripción completa

Detalles Bibliográficos
Autores principales: Halliday, Mark, Radford, Helois, Zents, Karlijn A. M., Molloy, Collin, Moreno, Julie A., Verity, Nicholas C., Smith, Ewan, Ortori, Catharine A., Barrett, David A., Bushell, Martin, Mallucci, Giovanna R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2017
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5445255/
https://www.ncbi.nlm.nih.gov/pubmed/28430857
http://dx.doi.org/10.1093/brain/awx074
_version_ 1783238845706272768
author Halliday, Mark
Radford, Helois
Zents, Karlijn A. M.
Molloy, Collin
Moreno, Julie A.
Verity, Nicholas C.
Smith, Ewan
Ortori, Catharine A.
Barrett, David A.
Bushell, Martin
Mallucci, Giovanna R.
author_facet Halliday, Mark
Radford, Helois
Zents, Karlijn A. M.
Molloy, Collin
Moreno, Julie A.
Verity, Nicholas C.
Smith, Ewan
Ortori, Catharine A.
Barrett, David A.
Bushell, Martin
Mallucci, Giovanna R.
author_sort Halliday, Mark
collection PubMed
description See Mercado and Hetz (doi:10.1093/brain/awx107) for a scientific commentary on this article. Signalling through the PERK/eIF2α-P branch of the unfolded protein response plays a critical role in controlling protein synthesis rates in cells. This pathway is overactivated in brains of patients with Alzheimer’s disease and related disorders and has recently emerged as a promising therapeutic target for these currently untreatable conditions. Thus, in mouse models of neurodegenerative disease, prolonged overactivation of PERK/eIF2α-P signalling causes sustained attenuation of protein synthesis, leading to memory impairment and neuronal loss. Re-establishing translation rates by inhibition of eIF2α-P activity, genetically or pharmacologically, restores memory and prevents neurodegeneration and extends survival. However, the experimental compounds used preclinically are unsuitable for use in humans, due to associated toxicity or poor pharmacokinetic properties. To discover compounds that have anti-eIF2α-P activity suitable for clinical use, we performed phenotypic screens on a NINDS small molecule library of 1040 drugs. We identified two compounds, trazodone hydrochloride and dibenzoylmethane, which reversed eIF2α-P-mediated translational attenuation in vitro and in vivo. Both drugs were markedly neuroprotective in two mouse models of neurodegeneration, using clinically relevant doses over a prolonged period of time, without systemic toxicity. Thus, in prion-diseased mice, both trazodone and dibenzoylmethane treatment restored memory deficits, abrogated development of neurological signs, prevented neurodegeneration and significantly prolonged survival. In tauopathy-frontotemporal dementia mice, both drugs were neuroprotective, rescued memory deficits and reduced hippocampal atrophy. Further, trazodone reduced p-tau burden. These compounds therefore represent potential new disease-modifying treatments for dementia. Trazodone in particular, a licensed drug, should now be tested in clinical trials in patients.
format Online
Article
Text
id pubmed-5445255
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-54452552017-05-31 Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice Halliday, Mark Radford, Helois Zents, Karlijn A. M. Molloy, Collin Moreno, Julie A. Verity, Nicholas C. Smith, Ewan Ortori, Catharine A. Barrett, David A. Bushell, Martin Mallucci, Giovanna R. Brain Original Articles See Mercado and Hetz (doi:10.1093/brain/awx107) for a scientific commentary on this article. Signalling through the PERK/eIF2α-P branch of the unfolded protein response plays a critical role in controlling protein synthesis rates in cells. This pathway is overactivated in brains of patients with Alzheimer’s disease and related disorders and has recently emerged as a promising therapeutic target for these currently untreatable conditions. Thus, in mouse models of neurodegenerative disease, prolonged overactivation of PERK/eIF2α-P signalling causes sustained attenuation of protein synthesis, leading to memory impairment and neuronal loss. Re-establishing translation rates by inhibition of eIF2α-P activity, genetically or pharmacologically, restores memory and prevents neurodegeneration and extends survival. However, the experimental compounds used preclinically are unsuitable for use in humans, due to associated toxicity or poor pharmacokinetic properties. To discover compounds that have anti-eIF2α-P activity suitable for clinical use, we performed phenotypic screens on a NINDS small molecule library of 1040 drugs. We identified two compounds, trazodone hydrochloride and dibenzoylmethane, which reversed eIF2α-P-mediated translational attenuation in vitro and in vivo. Both drugs were markedly neuroprotective in two mouse models of neurodegeneration, using clinically relevant doses over a prolonged period of time, without systemic toxicity. Thus, in prion-diseased mice, both trazodone and dibenzoylmethane treatment restored memory deficits, abrogated development of neurological signs, prevented neurodegeneration and significantly prolonged survival. In tauopathy-frontotemporal dementia mice, both drugs were neuroprotective, rescued memory deficits and reduced hippocampal atrophy. Further, trazodone reduced p-tau burden. These compounds therefore represent potential new disease-modifying treatments for dementia. Trazodone in particular, a licensed drug, should now be tested in clinical trials in patients. Oxford University Press 2017-06 2017-04-19 /pmc/articles/PMC5445255/ /pubmed/28430857 http://dx.doi.org/10.1093/brain/awx074 Text en © The Author (2017). Published by Oxford University Press on behalf of the Guarantors of Brain. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Articles
Halliday, Mark
Radford, Helois
Zents, Karlijn A. M.
Molloy, Collin
Moreno, Julie A.
Verity, Nicholas C.
Smith, Ewan
Ortori, Catharine A.
Barrett, David A.
Bushell, Martin
Mallucci, Giovanna R.
Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title_full Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title_fullStr Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title_full_unstemmed Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title_short Repurposed drugs targeting eIF2α-P-mediated translational repression prevent neurodegeneration in mice
title_sort repurposed drugs targeting eif2α-p-mediated translational repression prevent neurodegeneration in mice
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5445255/
https://www.ncbi.nlm.nih.gov/pubmed/28430857
http://dx.doi.org/10.1093/brain/awx074
work_keys_str_mv AT hallidaymark repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT radfordhelois repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT zentskarlijnam repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT molloycollin repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT morenojuliea repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT veritynicholasc repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT smithewan repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT ortoricatharinea repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT barrettdavida repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT bushellmartin repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice
AT malluccigiovannar repurposeddrugstargetingeif2alphapmediatedtranslationalrepressionpreventneurodegenerationinmice

Ejemplares similares