Photoreceptor Cell Death Mechanisms in Inherited Retinal Degeneration
(2008) In Molecular Neurobiology 38(3). p.253-269- Abstract
- Photoreceptor cell death is the major hallmark of a group of human inherited retinal degenerations commonly referred to as retinitis pigmentosa (RP). Although the causative genetic mutations are often known, the mechanisms leading to photoreceptor degeneration remain poorly defined. Previous research work has focused on apoptosis, but recent evidence suggests that photoreceptor cell death may result primarily from non-apoptotic mechanisms independently of AP1 or p53 transcription factor activity, Bcl proteins, caspases, or cytochrome c release. This review briefly describes some animal models used for studies of retinal degeneration, with particular focus on the rd1 mouse. After outlining the major features of different cell death... (More)
- Photoreceptor cell death is the major hallmark of a group of human inherited retinal degenerations commonly referred to as retinitis pigmentosa (RP). Although the causative genetic mutations are often known, the mechanisms leading to photoreceptor degeneration remain poorly defined. Previous research work has focused on apoptosis, but recent evidence suggests that photoreceptor cell death may result primarily from non-apoptotic mechanisms independently of AP1 or p53 transcription factor activity, Bcl proteins, caspases, or cytochrome c release. This review briefly describes some animal models used for studies of retinal degeneration, with particular focus on the rd1 mouse. After outlining the major features of different cell death mechanisms in general, we then compare them with results obtained in retinal degeneration models, where photoreceptor cell death appears to be governed by, among other things, changes in cyclic nucleotide metabolism, downregulation of the transcription factor CREB, and excessive activation of calpain and PARP. Based on recent experimental evidence, we propose a putative non-apoptotic molecular pathway for photoreceptor cell death in the rd1 retina. The notion that inherited photoreceptor cell death is driven by non-apoptotic mechanisms may provide new ideas for future treatment of RP. (Less)
Please use this url to cite or link to this publication:
https://lup.lub.lu.se/record/1415765
- author
- Sancho-Pelluz, J. ; Arango-Gonzalez, B. ; Kustermann, S. ; Romero, F. J. ; van Veen, Theo LU ; Zrenner, E. ; Ekström, Per LU and Paquet-Durand, F.
- organization
- publishing date
- 2008
- type
- Contribution to journal
- publication status
- published
- subject
- keywords
- Retina, rd1, PARP, CREB, Oxidative stress, Calpain, cGMP, AIF, Calcium, rd2, rds, APOPTOSIS-INDUCING FACTOR, ROD CGMP-PHOSPHODIESTERASE, ENDOPLASMIC-RETICULUM STRESS, ELEMENT-BINDING PROTEIN, CAMP EARLY, REPRESSOR, RD1 MOUSE RETINA, MEDIATED PROGRAMMED NECROSIS, CALCIUM-CHANNEL BLOCKER, NITRIC-OXIDE SYNTHASE, D-CIS-DILTIAZEM
- in
- Molecular Neurobiology
- volume
- 38
- issue
- 3
- pages
- 253 - 269
- publisher
- Humana Press
- external identifiers
-
- wos:000261598100004
- scopus:59049100857
- pmid:18982459
- ISSN
- 1559-1182
- DOI
- 10.1007/s12035-008-8045-9
- language
- English
- LU publication?
- yes
- id
- f2ab4d45-ad23-41e4-a819-ad50a4bb4636 (old id 1415765)
- date added to LUP
- 2016-04-01 14:01:01
- date last changed
- 2022-03-29 18:44:57
@article{f2ab4d45-ad23-41e4-a819-ad50a4bb4636,
abstract = {{Photoreceptor cell death is the major hallmark of a group of human inherited retinal degenerations commonly referred to as retinitis pigmentosa (RP). Although the causative genetic mutations are often known, the mechanisms leading to photoreceptor degeneration remain poorly defined. Previous research work has focused on apoptosis, but recent evidence suggests that photoreceptor cell death may result primarily from non-apoptotic mechanisms independently of AP1 or p53 transcription factor activity, Bcl proteins, caspases, or cytochrome c release. This review briefly describes some animal models used for studies of retinal degeneration, with particular focus on the rd1 mouse. After outlining the major features of different cell death mechanisms in general, we then compare them with results obtained in retinal degeneration models, where photoreceptor cell death appears to be governed by, among other things, changes in cyclic nucleotide metabolism, downregulation of the transcription factor CREB, and excessive activation of calpain and PARP. Based on recent experimental evidence, we propose a putative non-apoptotic molecular pathway for photoreceptor cell death in the rd1 retina. The notion that inherited photoreceptor cell death is driven by non-apoptotic mechanisms may provide new ideas for future treatment of RP.}},
author = {{Sancho-Pelluz, J. and Arango-Gonzalez, B. and Kustermann, S. and Romero, F. J. and van Veen, Theo and Zrenner, E. and Ekström, Per and Paquet-Durand, F.}},
issn = {{1559-1182}},
keywords = {{Retina; rd1; PARP; CREB; Oxidative stress; Calpain; cGMP; AIF; Calcium; rd2; rds; APOPTOSIS-INDUCING FACTOR; ROD CGMP-PHOSPHODIESTERASE; ENDOPLASMIC-RETICULUM STRESS; ELEMENT-BINDING PROTEIN; CAMP EARLY; REPRESSOR; RD1 MOUSE RETINA; MEDIATED PROGRAMMED NECROSIS; CALCIUM-CHANNEL BLOCKER; NITRIC-OXIDE SYNTHASE; D-CIS-DILTIAZEM}},
language = {{eng}},
number = {{3}},
pages = {{253--269}},
publisher = {{Humana Press}},
series = {{Molecular Neurobiology}},
title = {{Photoreceptor Cell Death Mechanisms in Inherited Retinal Degeneration}},
url = {{http://dx.doi.org/10.1007/s12035-008-8045-9}},
doi = {{10.1007/s12035-008-8045-9}},
volume = {{38}},
year = {{2008}},
}