Changes in signaling pathways of cell proliferation and apoptosis during NK/Ly lymphoma aging

Expression of specific proteins involved in regulation of cell proliferation and apoptosis was studied at the initial (7–8 days after tumor inoculation), median (13–14 days), and terminal (20–21 days) stages of murine NK/Ly lymphoma development. Western‐blot analysis using antibodies to MEK—ERK signaling pathway, E2F‐1/2 and c‐Myc, pSTAT1, pSTAT3, pSTAT5, anti‐apoptotic Bcl‐X L and pro‐apoptotic p53 and Rb proteins, as well as active cleaved forms of caspases‐3, −6, −7, was carried out to investigate the growth and survival status of NK/Ly cells. There was a marked increase in the expression of E2F‐1/2 transcription factors, MAPK signaling cascade and c‐Myc, which suggests intensive proliferation of lymphoma cells at terminal stage of tumor development. However, cytomorphological investigation and electrophoretic study of DNA fragmentation have shown degeneration of NK/Ly lymphoma cells and increase in their death. No expression of p53 protein or cleaved forms of caspases‐3, −6, −7 was found, which suggests a caspase‐independent type of apoptosis in these cells. Ascitic fluid collected at a terminal stage of NK/Ly lymphoma development was significantly weaker in supporting tumor cell growth than ascitic fluid collected at the initial stage of tumor development. It is suggested that uncontrolled cell proliferation at terminal stage of the NK/Ly lymphoma development causes nutrient deprivation and deficiency of specific growth factors in the ascitic fluid, due to overexpression of MEK—ERK, E2F and c‐Myc, thereby leading to the induction of apoptosis.