Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.

Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.

Inhibitory factors have been implicated in the failure of remyelination in demyelinating diseases. Myelin associated inhibitors act through a common receptor called Nogo receptor (NgR) that plays critical inhibitory roles in CNS plasticity. Here we investigated the effects of abrogating NgR inhibiti...

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Main Authors: Fereshteh Pourabdolhossein, Sabah Mozafari, Ghislaine Morvan-Dubois, Javad Mirnajafi-Zadeh, Alejandra Lopez-Juarez, Jacqueline Pierre-Simons, Barbara A Demeneix, Mohammad Javan
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4153612?pdf=render
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spelling doaj-7de154ac1aa14861a2409103e12945142020-11-25T01:48:14ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0199e10637810.1371/journal.pone.0106378Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.Fereshteh PourabdolhosseinSabah MozafariGhislaine Morvan-DuboisJavad Mirnajafi-ZadehAlejandra Lopez-JuarezJacqueline Pierre-SimonsBarbara A DemeneixMohammad JavanInhibitory factors have been implicated in the failure of remyelination in demyelinating diseases. Myelin associated inhibitors act through a common receptor called Nogo receptor (NgR) that plays critical inhibitory roles in CNS plasticity. Here we investigated the effects of abrogating NgR inhibition in a non-immune model of focal demyelination in adult mouse optic chiasm.A focal area of demyelination was induced in adult mouse optic chiasm by microinjection of lysolecithin. To knock down NgR levels, siRNAs against NgR were intracerebroventricularly administered via a permanent cannula over 14 days, Functional changes were monitored by electrophysiological recording of latency of visual evoked potentials (VEPs). Histological analysis was carried out 3, 7 and 14 days post demyelination lesion. To assess the effect of NgR inhibition on precursor cell repopulation, BrdU was administered to the animals prior to the demyelination induction. Inhibition of NgR significantly restored VEPs responses following optic chiasm demyelination. These findings were confirmed histologically by myelin specific staining. siNgR application resulted in a smaller lesion size compared to control. NgR inhibition significantly increased the numbers of BrdU+/Olig2+ progenitor cells in the lesioned area and in the neurogenic zone of the third ventricle. These progenitor cells (Olig2+ or GFAP+) migrated away from this area as a function of time.Our results show that inhibition of NgR facilitate myelin repair in the demyelinated chiasm, with enhanced recruitment of proliferating cells to the lesion site. Thus, antagonizing NgR function could have therapeutic potential for demyelinating disorders such as Multiple Sclerosis.http://europepmc.org/articles/PMC4153612?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Fereshteh Pourabdolhossein
Sabah Mozafari
Ghislaine Morvan-Dubois
Javad Mirnajafi-Zadeh
Alejandra Lopez-Juarez
Jacqueline Pierre-Simons
Barbara A Demeneix
Mohammad Javan
spellingShingle Fereshteh Pourabdolhossein
Sabah Mozafari
Ghislaine Morvan-Dubois
Javad Mirnajafi-Zadeh
Alejandra Lopez-Juarez
Jacqueline Pierre-Simons
Barbara A Demeneix
Mohammad Javan
Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
PLoS ONE
author_facet Fereshteh Pourabdolhossein
Sabah Mozafari
Ghislaine Morvan-Dubois
Javad Mirnajafi-Zadeh
Alejandra Lopez-Juarez
Jacqueline Pierre-Simons
Barbara A Demeneix
Mohammad Javan
author_sort Fereshteh Pourabdolhossein
title Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
title_short Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
title_full Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
title_fullStr Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
title_full_unstemmed Nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
title_sort nogo receptor inhibition enhances functional recovery following lysolecithin-induced demyelination in mouse optic chiasm.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Inhibitory factors have been implicated in the failure of remyelination in demyelinating diseases. Myelin associated inhibitors act through a common receptor called Nogo receptor (NgR) that plays critical inhibitory roles in CNS plasticity. Here we investigated the effects of abrogating NgR inhibition in a non-immune model of focal demyelination in adult mouse optic chiasm.A focal area of demyelination was induced in adult mouse optic chiasm by microinjection of lysolecithin. To knock down NgR levels, siRNAs against NgR were intracerebroventricularly administered via a permanent cannula over 14 days, Functional changes were monitored by electrophysiological recording of latency of visual evoked potentials (VEPs). Histological analysis was carried out 3, 7 and 14 days post demyelination lesion. To assess the effect of NgR inhibition on precursor cell repopulation, BrdU was administered to the animals prior to the demyelination induction. Inhibition of NgR significantly restored VEPs responses following optic chiasm demyelination. These findings were confirmed histologically by myelin specific staining. siNgR application resulted in a smaller lesion size compared to control. NgR inhibition significantly increased the numbers of BrdU+/Olig2+ progenitor cells in the lesioned area and in the neurogenic zone of the third ventricle. These progenitor cells (Olig2+ or GFAP+) migrated away from this area as a function of time.Our results show that inhibition of NgR facilitate myelin repair in the demyelinated chiasm, with enhanced recruitment of proliferating cells to the lesion site. Thus, antagonizing NgR function could have therapeutic potential for demyelinating disorders such as Multiple Sclerosis.
url http://europepmc.org/articles/PMC4153612?pdf=render
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AT sabahmozafari nogoreceptorinhibitionenhancesfunctionalrecoveryfollowinglysolecithininduceddemyelinationinmouseopticchiasm
AT ghislainemorvandubois nogoreceptorinhibitionenhancesfunctionalrecoveryfollowinglysolecithininduceddemyelinationinmouseopticchiasm
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