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Lack of p75 receptor does not protect photoreceptors from light-induced cell death

Authors :
Michael T. Matthes
Bärbel Rohrer
Louis F. Reichardt
Matthew M. LaVail
Source :
Experimental Eye Research. 76:125-129
Publication Year :
2003
Publisher :
Elsevier BV, 2003.

Abstract

Rod photoreceptors are susceptible to light-induced cell death. Previous results have suggested that the neurotrophin receptor p75 in Müller cells controls photoreceptor cell death during light-exposure by suppressing trophic factor release; and consequently, if p75 is blocked or eliminated during light-exposure, apoptosis is delayed. We explored this question by examining photoreceptor cell survival in albino p75(-/-) mice as well as their heterozygous and homozygous littermates. Photoreceptor cell death was examined in semi-thin sections by counting the remaining rows of photoreceptors. No difference in the amount of cell death was found between p75(+/+) and p75(-/-) animals, whereas the single copy of p75 in the heterozygous p75(+/-) mice provided significant neuroprotection. Cell death in the wild-type animals may indeed be mediated by p75, whereas other known apoptosis pathways may be activated in the p75(-/-) mice. The pro-apoptotic activity of the p75 receptor may have been partially suppressed in the heterozygous p75(+/-) mice by the silencing effect of the Trk receptor. Thus, our results suggest that p75 signaling does not mediate the main apoptosis pathway activated during light-damage.

Details

ISSN :
00144835
Volume :
76
Database :
OpenAIRE
Journal :
Experimental Eye Research
Accession number :
edsair.doi.dedup.....0b5a7228bfffb9696c7424d7ec7fc7d6