CFTR modulates programmed cell death by decreasing intracellular pH in Chinese hamster lung fibroblasts

Abstract

To study the potential influence of cystic fibrosis conductance regulator (CFTR) on intracellular pH regulation during apoptosis induction, we used PS120 Chinese hamster lung fibroblasts devoid of the Na+/H+ exchanger (NHE1 isoform) transfected with constructs, allowing the expression of CFTR and/or NHE1. Kinetics of lovastatin-induced apoptosis were measured by orcein staining, double staining with Hoechst-33258, propidium iodide, DNA fragmentation, and annexin V labeling. In PS120 control cells, the percentage of apoptotic cells after 40 h of lovastatin treatment was 23 ± 3%, whereas in PS120 CFTR-transfected cells, this percentage was 40 ± 4%. In PS120 NHE1 cells, the transfection with CFTR did not modify the percentage of apoptotic cells after 40 h (control: 19 ± 3%, n = 8; CFTR: 17 ± 1%, n = 8), indicating that blocking intracellular acidification by overexpressing the Na+/H+ exchanger inhibited the enhancement of apoptosis induced by CFTR. In all cell lines, the initial pH values were identical (pH = 7.46 ± 0.04, n = 9), and treatment with lovastatin led to intracellular acidification. However, the pH value after 40 h was lower in PS120 CFTR-transfected cells (pH = 6.85 ± 0.02, n= 10) than in PS120 cells (pH = 7.15 ± 0.03, n = 10). To further investigate the origin of this increased intracellular acidification observed in CFTR-transfected cells, the activity of the DIDS-inhibitable Cl−/HCO[Formula: see text] exchanger was studied. 8-Bromoadenosine 3′,5′-cyclic monophosphate incubation resulted in Cl−/HCO[Formula: see text] exchanger activation in PS120 CFTR-transfected cells but had no effect on PS120 cells. Together, our results suggest that CFTR can enhance apoptosis in Chinese hamster lung fibroblasts, probably due to the modulation of the Cl−/HCO[Formula: see text] exchanger, resulting in a more efficient intracellular acidification.