Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke

Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke

<p>Abstract</p> <p>Background</p> <p>5HT<sub>1A </sub>agonists have previously been shown to promote recovery in animal models of stroke using ex vivo outcome measures which have raised the hopes for a potential clinical implementation. The purpose of this s...

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Main Authors: Modo Michel M, McCreary Andrew, Bernanos Michel, Lowe Andrew S, Beech John S, Ashioti Maria, Williams Steve CR
Format: Article
Language:English
Published: BMC 2009-07-01
Series:BMC Neuroscience
Online Access:http://www.biomedcentral.com/1471-2202/10/82
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spelling doaj-6d08c5db430548fc83e46e868efa5b912020-11-25T00:19:07ZengBMCBMC Neuroscience1471-22022009-07-011018210.1186/1471-2202-10-82Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic strokeModo Michel MMcCreary AndrewBernanos MichelLowe Andrew SBeech John SAshioti MariaWilliams Steve CR<p>Abstract</p> <p>Background</p> <p>5HT<sub>1A </sub>agonists have previously been shown to promote recovery in animal models of stroke using ex vivo outcome measures which have raised the hopes for a potential clinical implementation. The purpose of this study was to evaluate the potential neuroprotective properties of a novel 5HT<sub>1A </sub>agonist DU123015 in 2 different models of transient focal ischaemic stroke of varying severities using both in vivo neuroimaging and behavioural techniques as primary outcome measures. For these studies, the NMDA receptor antagonist MK-801 was also utilized as a positive control to further assess the effectiveness of the stroke models and techniques used.</p> <p>Results</p> <p>In contrast to MK-801, no significant therapeutic effect of DU123015 on lesion volume in either the distal MCAo or intraluminal thread model of stroke was found. MK-801 significantly reduced lesion volume in both models; the mild distal MCAo condition (60 min ischaemia) and the intraluminal thread model, although it had no significant impact upon the lesion size in the severe distal MCAo condition (120 min ischaemia). These therapeutic effects on lesion size were mirrored on a behavioural test for sensory neglect and neurological deficit score in the intraluminal thread model.</p> <p>Conclusion</p> <p>This study highlights the need for a thorough experimental design to test novel neuroprotective compounds in experimental stroke investigations incorporating: a positive reference compound, different models of focal ischaemia, varying the duration of ischaemia, and objective in vivo assessments within a single study. This procedure will help us to minimise the translation of less efficacious compounds.</p> http://www.biomedcentral.com/1471-2202/10/82
collection DOAJ
language English
format Article
sources DOAJ
author Modo Michel M
McCreary Andrew
Bernanos Michel
Lowe Andrew S
Beech John S
Ashioti Maria
Williams Steve CR
spellingShingle Modo Michel M
McCreary Andrew
Bernanos Michel
Lowe Andrew S
Beech John S
Ashioti Maria
Williams Steve CR
Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
BMC Neuroscience
author_facet Modo Michel M
McCreary Andrew
Bernanos Michel
Lowe Andrew S
Beech John S
Ashioti Maria
Williams Steve CR
author_sort Modo Michel M
title Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
title_short Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
title_full Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
title_fullStr Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
title_full_unstemmed Neither in vivo MRI nor behavioural assessment indicate therapeutic efficacy for a novel 5HT<sub>1A </sub>agonist in rat models of ischaemic stroke
title_sort neither in vivo mri nor behavioural assessment indicate therapeutic efficacy for a novel 5ht<sub>1a </sub>agonist in rat models of ischaemic stroke
publisher BMC
series BMC Neuroscience
issn 1471-2202
publishDate 2009-07-01
description <p>Abstract</p> <p>Background</p> <p>5HT<sub>1A </sub>agonists have previously been shown to promote recovery in animal models of stroke using ex vivo outcome measures which have raised the hopes for a potential clinical implementation. The purpose of this study was to evaluate the potential neuroprotective properties of a novel 5HT<sub>1A </sub>agonist DU123015 in 2 different models of transient focal ischaemic stroke of varying severities using both in vivo neuroimaging and behavioural techniques as primary outcome measures. For these studies, the NMDA receptor antagonist MK-801 was also utilized as a positive control to further assess the effectiveness of the stroke models and techniques used.</p> <p>Results</p> <p>In contrast to MK-801, no significant therapeutic effect of DU123015 on lesion volume in either the distal MCAo or intraluminal thread model of stroke was found. MK-801 significantly reduced lesion volume in both models; the mild distal MCAo condition (60 min ischaemia) and the intraluminal thread model, although it had no significant impact upon the lesion size in the severe distal MCAo condition (120 min ischaemia). These therapeutic effects on lesion size were mirrored on a behavioural test for sensory neglect and neurological deficit score in the intraluminal thread model.</p> <p>Conclusion</p> <p>This study highlights the need for a thorough experimental design to test novel neuroprotective compounds in experimental stroke investigations incorporating: a positive reference compound, different models of focal ischaemia, varying the duration of ischaemia, and objective in vivo assessments within a single study. This procedure will help us to minimise the translation of less efficacious compounds.</p>
url http://www.biomedcentral.com/1471-2202/10/82
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