Evidence supports both exogenous and endogenous reactive oxidative species (ROS) as factors involved in pathologic steps in AMD.
12,17 –20 We therefore determined the effect of H
2O
2 on CCR3 expression level in CECs. We previously reported that 600 μM H
2O
2 caused a significant and selective upregulation of the VEGF
189 splice variant in RPE.
14 However, in CECs, there was no change in the expression levels of VEGF splice variants, VEGF
121, VEGF
165, and VEGF
189.
14 To determine the effect of H
2O
2 on CCR3 expression in CECs, a dose–response experiment was performed with H
2O
2 at 100, 300, or 600 μM concentrations. After incubation for 24 hours, CCR3 expression in CECs was found to be increased 4-fold from control at the 300 μM concentration (
Fig. 2C). In cultured RPE, H
2O
2 exposure also caused a significant increase in CCR3 mRNA compared with control, although the expression levels remained 10-fold less than that of CCR3 (data not shown). When RPE were exposed to 300 μM H
2O
2, there was a significant 15-fold increase in expression of all three CCR3 ligands (CCl11, CCl24, and CCl26;
Fig. 2D), whereas CEC expression of all three ligands was unchanged from control after exposure to 300 μM H
2O
2 (data not shown). Therefore, age and oxidative stress appeared to upregulate CCR3 in both CECs and RPE, and induce increased CCR3 ligand production only in RPE cells.