Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells

Glaucoma is characterized by a loss of retinal ganglion cells (RGC) which is associated with a decrease of visual function. Neuroprotective agents as a new therapeutic strategy could prevent the remaining neurons from apoptotic cell death. Previous studies have shown the involvement of the Cyclooxyg...

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Main Authors: Anja-Kristina Brust, Holger K. Ulbrich, Gail M. Seigel, Norbert Pfeiffer, Franz H. Grus
Format: Article
Language:English
Published: SAGE Publishing 2008-01-01
Series:Biomarker Insights
Subjects:
Online Access:http://www.la-press.com/effects-of-cyclooxygenase-inhibitors-on-apoptotic-neuroretinal-cells-a1308
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spelling doaj-6fc79bbf792648298855d44ba5878c022020-11-25T02:59:51ZengSAGE PublishingBiomarker Insights1177-27192008-01-013387402Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal CellsAnja-Kristina BrustHolger K. UlbrichGail M. SeigelNorbert PfeifferFranz H. GrusGlaucoma is characterized by a loss of retinal ganglion cells (RGC) which is associated with a decrease of visual function. Neuroprotective agents as a new therapeutic strategy could prevent the remaining neurons from apoptotic cell death. Previous studies have shown the involvement of the Cyclooxygenase (COX)-2 signalling in the apoptotic death of neurons. Herein we investigated the neuroprotective effect of COX-1/COX-2- and selective COX-2- inhibitors on apoptotic. R28, a neuroretinal cell line and determined the PGE2 levels by ELISA. Furthermore we investigated differences in protein expression in the cells after exposure to elevated pressure compared to untreated cells by ProteinChip analysis.In addition, a protein profiling study of the cells after exposure to elevated pressure was performed. The protein expression profiles were measured by SELDI-TOF (Surface Enhanced Laser Desorption/Ionization-time of flight) Protein Chips. The protein identification was performed by mass spectrometry (MS).It could be shown that COX-2 inhibition significantly prevented the cells from apoptosis and reduced the PGE2 concentrations. Selective COX-2 inhibitors were significant more potent than non-selective inhibitors or COX-1 inhibitors. We found differently expressed protein patterns in neuroretinal cells cultured at atmospheric pressure compared to those cells exposed to elevated pressure with or without celecoxib respectively. We identified three biomarkers, ubiquitin, HSP10 and NDKB, which were differently expressed in the groups. However, our data indicates a distinct neuroprotective effect of COX-2 inhibition. The local treatment with selective COX-2 inhibitors might provide an innovative strategy of therapeutic intervention for glaucoma.http://www.la-press.com/effects-of-cyclooxygenase-inhibitors-on-apoptotic-neuroretinal-cells-a1308retinal ganglion cellscyclooxygenasePGE2apoptosisneuroprotectionSeldi/Maldibiomarker neuroprotection of apoptotic neuroretinal cells
collection DOAJ
language English
format Article
sources DOAJ
author Anja-Kristina Brust
Holger K. Ulbrich
Gail M. Seigel
Norbert Pfeiffer
Franz H. Grus
spellingShingle Anja-Kristina Brust
Holger K. Ulbrich
Gail M. Seigel
Norbert Pfeiffer
Franz H. Grus
Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
Biomarker Insights
retinal ganglion cells
cyclooxygenase
PGE2
apoptosis
neuroprotection
Seldi/Maldi
biomarker neuroprotection of apoptotic neuroretinal cells
author_facet Anja-Kristina Brust
Holger K. Ulbrich
Gail M. Seigel
Norbert Pfeiffer
Franz H. Grus
author_sort Anja-Kristina Brust
title Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
title_short Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
title_full Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
title_fullStr Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
title_full_unstemmed Effects of Cyclooxygenase Inhibitors on Apoptotic Neuroretinal Cells
title_sort effects of cyclooxygenase inhibitors on apoptotic neuroretinal cells
publisher SAGE Publishing
series Biomarker Insights
issn 1177-2719
publishDate 2008-01-01
description Glaucoma is characterized by a loss of retinal ganglion cells (RGC) which is associated with a decrease of visual function. Neuroprotective agents as a new therapeutic strategy could prevent the remaining neurons from apoptotic cell death. Previous studies have shown the involvement of the Cyclooxygenase (COX)-2 signalling in the apoptotic death of neurons. Herein we investigated the neuroprotective effect of COX-1/COX-2- and selective COX-2- inhibitors on apoptotic. R28, a neuroretinal cell line and determined the PGE2 levels by ELISA. Furthermore we investigated differences in protein expression in the cells after exposure to elevated pressure compared to untreated cells by ProteinChip analysis.In addition, a protein profiling study of the cells after exposure to elevated pressure was performed. The protein expression profiles were measured by SELDI-TOF (Surface Enhanced Laser Desorption/Ionization-time of flight) Protein Chips. The protein identification was performed by mass spectrometry (MS).It could be shown that COX-2 inhibition significantly prevented the cells from apoptosis and reduced the PGE2 concentrations. Selective COX-2 inhibitors were significant more potent than non-selective inhibitors or COX-1 inhibitors. We found differently expressed protein patterns in neuroretinal cells cultured at atmospheric pressure compared to those cells exposed to elevated pressure with or without celecoxib respectively. We identified three biomarkers, ubiquitin, HSP10 and NDKB, which were differently expressed in the groups. However, our data indicates a distinct neuroprotective effect of COX-2 inhibition. The local treatment with selective COX-2 inhibitors might provide an innovative strategy of therapeutic intervention for glaucoma.
topic retinal ganglion cells
cyclooxygenase
PGE2
apoptosis
neuroprotection
Seldi/Maldi
biomarker neuroprotection of apoptotic neuroretinal cells
url http://www.la-press.com/effects-of-cyclooxygenase-inhibitors-on-apoptotic-neuroretinal-cells-a1308
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