DIFFERENTIAL ANTIAPOPTOTIC EFFECT OF ERYTHROPOIETIN ON UNDIFFERENTIATED AND RETINOIC ACID-DIFFERENTIATED SH-SY5Y CELLS

WENKER SHIRLEY; CHAMORRO MARÍA E.; VOTA DAIANA; CALLERO MARIANA; VITTORI DANIELA; NESSE ALCIRA

JOURNAL OF CELLULAR BIOCHEMISTRY

WILEY-LISS, DIV JOHN WILEY & SONS INC

Año: 2010 vol. 110 p. 151 - 161

0730-2312

Erythropoietin (Epo) is known to have significant roles in tissues outside the hematopoietic system. In this work, we investigated the function of Epo in neuronal cells subjected to differentiation. Treatment of SH-SY5Y cells with all-trans retinoic acid (atRA) generated differentiated neuron-like cells, observed by increased expression of neuronal markers and morphological changes. Exposure of undifferentiated cells to proapoptotic stimuli such as staurosporine, TNF-α or hypoxia, significantly increased programmed cell death, which was prevented by previous treatment with Epo. In contrast, atRA-differentiated cultures showed cell resistance to apoptosis. No additional effect of Epo was detected in previously differentiated cells. The inhibition of the PI3K/Akt pathway by Ly294002 abrogated the protective effects induced by either Epo or atRA. The effect of atRA was mediated by an increased expression of Bcl-2 whereas the Epo treatment upregulated not only Bcl-2 but also Bcl- xL. This upregulation by Epo was not detected in atRA-differentiated cells, thus confirming the lack of the protective effect of this hormone. As expected, assays with AG490, an inhibitor of Jak2, blocked the Epo action only in undifferentiated cells. This reduced neuroprotective function of Epo on SH-SY5Y differentiated cells could be explained at least in part by downregulation of the Epo receptor expression which was observed in atRA-differentiated cells. This study shows differential cellular protection induced by Epo at two stages of SH-SY5Y differentiation. The results allow us to suggest that this differential cell behavior can be ascribed to the interaction between atRA and the sgnaling pathways mediated by Epo.