Cellular senescence in the glaucomatous outflow pathway.
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Journal: 2006/April - Experimental Gerontology
ISSN: 0531-5565
Abstract:
The mechanisms responsible for the progressive malfunction of the trabecular meshwork (TM)-Schlemm's canal (SC) conventional outflow pathway tissue in primary open angle glaucoma (POAG) are still not fully understood. To determine whether POAG is characterized by an accumulation of senescent cells, similar to what has been described in other diseases, we have compared the levels of the senescence marker senescence-associated-beta-galactosidase (SA-beta-gal) in the outflow pathway cells of POAG and age-matched control donors. POAG donors demonstrated a statistically significant fourfold increase in the percentage of SA-beta-gal positive cells. These results suggest a potential role for cellular senescence in the pathophysiology of the outflow pathway.
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Exp Gerontol 40(8-9): 745-748
PMID: 16051457

Cellular senescence in the glaucomatous outflow pathway

Department of Ophthalmology, Duke University, Erwin Road, Box 3802, Durham, NC 27710, USA
Paloma B. Liton: ude.ekud.seton@100notil; Pratap Challa: ude.ekud.cm@100llahc; Sandra Stinnett: ude.ekud.cm@100nnits; Coralia Luna: ude.seton.cm@3000anul; David L. Epstein: ude.ekud.cm@100etspe
Corresponding author. Tel.: +1-919-681-5995; fax: +1-919-684-8983, ude.ekud@zelaznog.ordep (P. Gonzalez)
Paloma B. Liton: ude.ekud.seton@100notil; Pratap Challa: ude.ekud.cm@100llahc; Sandra Stinnett: ude.ekud.cm@100nnits; Coralia Luna: ude.seton.cm@3000anul; David L. Epstein: ude.ekud.cm@100etspe
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Abstract

The mechanisms responsible for the progressive malfunction of the trabecular meshwork (TM)–Schlemm’s canal (SC) conventional outflow pathway tissue in primary open angle glaucoma (POAG) are still not fully understood. To determine whether POAG is characterized by an accumulation of senescent cells, similar to what has been described in other diseases, we have compared the levels of the senescence marker senescence-associated-β-galactosidase (SA-β-gal) in the outflow pathway cells of POAG and age-matched control donors. POAG donors demonstrated a statistically significant fourfold increase in the percentage of SA-β-gal positive cells. These results suggest a potential role for cellular senescence in the pathophysiology of the outflow pathway.

Keywords: Trabecular meshwork, Senescence, POAG, Glaucoma, Senescence-associated-β-galactosidase
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