Disruption of neuronal function by soluble hyperphosphorylated tau in a Drosophila model of tauopathy
Disruption of neuronal function by soluble hyperphosphorylated tau in a Drosophila model of tauopathy
Axonal microtubules are essential for transport of materials to the synapse. Compromised microtubules
and synaptic loss have been demonstrated in AD (Alzheimer’s disease), which is believed to contribute to cognitive dysfunction before neuronal death in the early stages of the disease.
The mechanism by which hyperphosphorylated tau, the building block of neurofibrillary tangles, one of the pathological hallmarks of AD, disrupts neuronal and synaptic function is unclear. There is a theory that hyperphosphorylated tau does not bind effectively to microtubules and is no longer able to function in stabilizing them, thus axonal transport can no longer proceed efficiently.
This leads to synaptic dysfunction. We have tested this theory in a Drosophila model of tauopathies in which we expressed human tau (h-tau). Using this model, we
have tested all aspects of this hypothesis and have demonstrated that axonal transport does become
compromised in the presence of hyperphosphorylated h-tau and this leads to synaptic and behavioural defects.
We are currently investigating the mechanism by which hyperphosphorylated h-tau mediates this effect and are preliminary data indicate that this entails phospho tau-mediated affects that are predicted by the tau–microtubule hypothesis, as well as novel effects.
These deleterious effects of h-tau occur in the
absence of tau filaments and before neuronal death. This sequence of pathogenic events may constitute the mechanism by which abnormal tau disrupts neuronal and synaptic function and contributes to cognitive impairment before neuronal death in the early stages of tauopathies such as AD.
Alzheimer’s disease, axonal transport, lithium, microtubule, neurofibrillary tangle, synapse.
564-570
Cowan, Catherine M.
9dd8dfb6-bfa9-4388-b386-8e98e188b22a
Chee, Francis
a21a1cbf-388a-4a2d-a484-f3e527b6b576
Shepherd, David
11aa6858-d19c-4450-82ff-11dff9dcd9c4
Mudher, Amritpal
ce0ccb35-ac49-4b6c-92b4-8dd5e78ac119
April 2010
Cowan, Catherine M.
9dd8dfb6-bfa9-4388-b386-8e98e188b22a
Chee, Francis
a21a1cbf-388a-4a2d-a484-f3e527b6b576
Shepherd, David
11aa6858-d19c-4450-82ff-11dff9dcd9c4
Mudher, Amritpal
ce0ccb35-ac49-4b6c-92b4-8dd5e78ac119
Cowan, Catherine M., Chee, Francis, Shepherd, David and Mudher, Amritpal
(2010)
Disruption of neuronal function by soluble hyperphosphorylated tau in a Drosophila model of tauopathy.
Biochemical Society Transactions, 38, part 2, .
(doi:10.1042/BST0380564).
Abstract
Axonal microtubules are essential for transport of materials to the synapse. Compromised microtubules
and synaptic loss have been demonstrated in AD (Alzheimer’s disease), which is believed to contribute to cognitive dysfunction before neuronal death in the early stages of the disease.
The mechanism by which hyperphosphorylated tau, the building block of neurofibrillary tangles, one of the pathological hallmarks of AD, disrupts neuronal and synaptic function is unclear. There is a theory that hyperphosphorylated tau does not bind effectively to microtubules and is no longer able to function in stabilizing them, thus axonal transport can no longer proceed efficiently.
This leads to synaptic dysfunction. We have tested this theory in a Drosophila model of tauopathies in which we expressed human tau (h-tau). Using this model, we
have tested all aspects of this hypothesis and have demonstrated that axonal transport does become
compromised in the presence of hyperphosphorylated h-tau and this leads to synaptic and behavioural defects.
We are currently investigating the mechanism by which hyperphosphorylated h-tau mediates this effect and are preliminary data indicate that this entails phospho tau-mediated affects that are predicted by the tau–microtubule hypothesis, as well as novel effects.
These deleterious effects of h-tau occur in the
absence of tau filaments and before neuronal death. This sequence of pathogenic events may constitute the mechanism by which abnormal tau disrupts neuronal and synaptic function and contributes to cognitive impairment before neuronal death in the early stages of tauopathies such as AD.
Text
Cowan_and_Mudher_2010.pdf
- Version of Record
Restricted to Repository staff only
Request a copy
More information
e-pub ahead of print date: 1 April 2010
Published date: April 2010
Keywords:
Alzheimer’s disease, axonal transport, lithium, microtubule, neurofibrillary tangle, synapse.
Identifiers
Local EPrints ID: 143781
URI: http://eprints.soton.ac.uk/id/eprint/143781
ISSN: 0300-5127
PURE UUID: ffbd68f1-cd28-426d-a616-cdccd29226ed
Catalogue record
Date deposited: 13 Apr 2010 08:35
Last modified: 14 Mar 2024 00:44
Export record
Altmetrics
Contributors
Author:
Catherine M. Cowan
Author:
Francis Chee
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics