Involvement of Bcl-XL deamidation in E1A-mediated cisplatin sensitization of ovarian cancer cells

The adenovirus E1A protein has been shown to be involved in the potentiation of apoptosis induced by chemotherapeutic agents, yet the molecular events of E1A-mediated apoptosis are not very clear. A recent report has suggested that deamidation of the Bcl-X-L protein inhibits its antiapoptotic ability and leads to apoptosis induced by alkylating agents in Rb-deficient tumor cells. Since Rb is known to interact with E1A, which interrupts Rb's normal function, we examined Bcl-X-L deamidation and cell death induced by cisplatin in E1A transfectants. We found that the E1A transfectants became sensitive to cisplatin-induced apoptosis compared to the parental cells, SKOV3.ip1. Our data show that cisplatin treatment induced the modi. cation of Bcl-X-L in the E1A transfectants in dosage and time-dependent manner. Furthermore, phosphatase treatment had no effect on the level of Bcl-X-L modi. cation, whereas alkaline lysis buffer appeared to induce the same modi. cation of Bcl-X-L. Ectopic expression of the deamidated forms of Bcl-X-L in SKOV3.ip1 cells revealed that the modi. cation to the Bcl-X-L protein molecules was deamidation. Expression of the E1A mutant ( dl1108) which contains deletion at CR2 domain suppressed Bcl-X-L deamidation and apoptosis induced by cisplatin. We also found that expression of the nondeamidated Bcl-X-L protected E1A transfectants from apoptosis. These findings suggest that Bcl-X-L deamidation contributes to E1A-mediated cisplatin sensitization in SKOV3.ip1 cells.