Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease
A beta peptide accumulation is thought to be the primary event in the pathogenesis of Alzheimer's disease (AD), with downstream neurotoxic effects including the hyperphosphorylation of tau protein. Glycogen synthase kinase-3 (GSK-3) is increasingly implicated as playing a pivotal role in this a...
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ftucl:oai:eprints.ucl.ac.uk.OAI2:1302796 2024-10-13T14:05:48+00:00 Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease Sofola, O Kerr, F Rogers, I Killick, R Augustin, H Gandy, C Allen, MJ Hardy, J Lovestone, S Partridge, L 2010-09 application/pdf https://discovery.ucl.ac.uk/id/eprint/1302796/1/journal.pgen.1001087.pdf https://discovery.ucl.ac.uk/id/eprint/1302796/ eng eng PUBLIC LIBRARY SCIENCE https://discovery.ucl.ac.uk/id/eprint/1302796/1/journal.pgen.1001087.pdf https://discovery.ucl.ac.uk/id/eprint/1302796/ open PLoS Genetics , 6 (9) , Article e1001087. (2010) Glycogen-synthase kinase-3 App transgenic mice In-vivo Tau phosphorylation Protein-tau Neurofibrillary tangles Signaling pathway Memory deficits Premature death Mouse model Article 2010 ftucl 2024-09-30T07:42:09Z A beta peptide accumulation is thought to be the primary event in the pathogenesis of Alzheimer's disease (AD), with downstream neurotoxic effects including the hyperphosphorylation of tau protein. Glycogen synthase kinase-3 (GSK-3) is increasingly implicated as playing a pivotal role in this amyloid cascade. We have developed an adult-onset Drosophila model of AD, using an inducible gene expression system to express Arctic mutant A beta 42 specifically in adult neurons, to avoid developmental effects. A beta 42 accumulated with age in these flies and they displayed increased mortality together with progressive neuronal dysfunction, but in the apparent absence of neuronal loss. This fly model can thus be used to examine the role of events during adulthood and early AD aetiology. Expression of A beta 42 in adult neurons increased GSK-3 activity, and inhibition of GSK-3 (either genetically or pharmacologically by lithium treatment) rescued A beta 42 toxicity. A beta 42 pathogenesis was also reduced by removal of endogenous fly tau; but, within the limits of detection of available methods, tau phosphorylation did not appear to be altered in flies expressing A beta 42. The GSK-3-mediated effects on A beta 42 toxicity appear to be at least in part mediated by tau-independent mechanisms, because the protective effect of lithium alone was greater than that of the removal of tau alone. Finally, A beta 42 levels were reduced upon GSK-3 inhibition, pointing to a direct role of GSK-3 in the regulation of A beta 42 peptide level, in the absence of APP processing. Our study points to the need both to identify the mechanisms by which GSK-3 modulates A beta 42 levels in the fly and to determine if similar mechanisms are present in mammals, and it supports the potential therapeutic use of GSK-3 inhibitors in AD. Article in Journal/Newspaper Arctic University College London: UCL Discovery Arctic |
institution |
Open Polar |
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University College London: UCL Discovery |
op_collection_id |
ftucl |
language |
English |
topic |
Glycogen-synthase kinase-3 App transgenic mice In-vivo Tau phosphorylation Protein-tau Neurofibrillary tangles Signaling pathway Memory deficits Premature death Mouse model |
spellingShingle |
Glycogen-synthase kinase-3 App transgenic mice In-vivo Tau phosphorylation Protein-tau Neurofibrillary tangles Signaling pathway Memory deficits Premature death Mouse model Sofola, O Kerr, F Rogers, I Killick, R Augustin, H Gandy, C Allen, MJ Hardy, J Lovestone, S Partridge, L Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
topic_facet |
Glycogen-synthase kinase-3 App transgenic mice In-vivo Tau phosphorylation Protein-tau Neurofibrillary tangles Signaling pathway Memory deficits Premature death Mouse model |
description |
A beta peptide accumulation is thought to be the primary event in the pathogenesis of Alzheimer's disease (AD), with downstream neurotoxic effects including the hyperphosphorylation of tau protein. Glycogen synthase kinase-3 (GSK-3) is increasingly implicated as playing a pivotal role in this amyloid cascade. We have developed an adult-onset Drosophila model of AD, using an inducible gene expression system to express Arctic mutant A beta 42 specifically in adult neurons, to avoid developmental effects. A beta 42 accumulated with age in these flies and they displayed increased mortality together with progressive neuronal dysfunction, but in the apparent absence of neuronal loss. This fly model can thus be used to examine the role of events during adulthood and early AD aetiology. Expression of A beta 42 in adult neurons increased GSK-3 activity, and inhibition of GSK-3 (either genetically or pharmacologically by lithium treatment) rescued A beta 42 toxicity. A beta 42 pathogenesis was also reduced by removal of endogenous fly tau; but, within the limits of detection of available methods, tau phosphorylation did not appear to be altered in flies expressing A beta 42. The GSK-3-mediated effects on A beta 42 toxicity appear to be at least in part mediated by tau-independent mechanisms, because the protective effect of lithium alone was greater than that of the removal of tau alone. Finally, A beta 42 levels were reduced upon GSK-3 inhibition, pointing to a direct role of GSK-3 in the regulation of A beta 42 peptide level, in the absence of APP processing. Our study points to the need both to identify the mechanisms by which GSK-3 modulates A beta 42 levels in the fly and to determine if similar mechanisms are present in mammals, and it supports the potential therapeutic use of GSK-3 inhibitors in AD. |
format |
Article in Journal/Newspaper |
author |
Sofola, O Kerr, F Rogers, I Killick, R Augustin, H Gandy, C Allen, MJ Hardy, J Lovestone, S Partridge, L |
author_facet |
Sofola, O Kerr, F Rogers, I Killick, R Augustin, H Gandy, C Allen, MJ Hardy, J Lovestone, S Partridge, L |
author_sort |
Sofola, O |
title |
Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
title_short |
Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
title_full |
Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
title_fullStr |
Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
title_full_unstemmed |
Inhibition of GSK-3 ameliorates Aβ pathology in an adult-onset drosophila model of Alzheimer's Disease |
title_sort |
inhibition of gsk-3 ameliorates aβ pathology in an adult-onset drosophila model of alzheimer's disease |
publisher |
PUBLIC LIBRARY SCIENCE |
publishDate |
2010 |
url |
https://discovery.ucl.ac.uk/id/eprint/1302796/1/journal.pgen.1001087.pdf https://discovery.ucl.ac.uk/id/eprint/1302796/ |
geographic |
Arctic |
geographic_facet |
Arctic |
genre |
Arctic |
genre_facet |
Arctic |
op_source |
PLoS Genetics , 6 (9) , Article e1001087. (2010) |
op_relation |
https://discovery.ucl.ac.uk/id/eprint/1302796/1/journal.pgen.1001087.pdf https://discovery.ucl.ac.uk/id/eprint/1302796/ |
op_rights |
open |
_version_ |
1812811836411609088 |