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Characterization of stress response in human retinal epithelial cells
Authors:Michelle Savoldelli  Roberta Gioia  Antonella Forlino  Giuliano Mazzini  Marzia Pennati  Nadia Zaffaroni  Anna Ivana Scovassi  Alicia Torriglia
Institution:1. Departement Ophtalmologie, Hotel Dieu, , Paris, France;2. Dipartimento di Biochimica, Università di Pavia, , Pavia, Italy;3. Istituto di Genetica Molecolare, CNR, , Pavia, Italy;4. Department of Experimental Oncology, Fondazione IRCCS Istituto Nazionale dei Tumori, , Milano, Italy;5. U872 eq. 17, Centre de Recherches des Cordeliers, INSERM, , Paris, France;6. Centre de Recherches des Cordeliers, Université Pierre et Marie Curie, , Paris, France;7. Centre de Recherches des Cordeliers, Université Paris Descartes, , Paris, France
Abstract:The pathogenesis of age‐related macular degeneration (AMD) involves demise of the retinal pigment epithelium and death of photoreceptors. In this article, we investigated the response of human adult retinal pigmented epithelial (ARPE‐19) cells to 5‐(N,N‐hexamethylene)amiloride (HMA), an inhibitor of Na+/H+ exchangers. We observed that ARPE‐19 cells treated with HMA are unable to activate ‘classical’ apoptosis but they succeed to activate autophagy. In the first 2 hrs of HMA exposure, autophagy is efficient in protecting cells from death. Thereafter, autophagy is impaired, as indicated by p62 accumulation, and this protective mechanism becomes the executioner of cell death. This switch in autophagy property as a function of time for a single stimulus is here shown for the first time. The activation of autophagy was observed, at a lesser extent, with etoposide, suggesting that this event might be a general response of ARPE cells to stress and the most important pathway involved in cell resistance to adverse conditions and toxic stimuli.
Keywords:Apoptosis  ARPE‐19 cells  autophagy  caspases     HMA     L‐DNase II  PARP‐1
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