Ionizing radiation activates expression of FOXO3a, Fas ligand, and Bim, and induces cell apoptosis

Artigo Acesso aberto

Ionizing radiation activates expression of FOXO3a, Fas ligand, and Bim, and induces cell apoptosis

2006; Spandidos Publishing; Linguagem: Inglês

10.3892/ijo.29.3.643

ISSN

1019-6439

Autores

Jer-Yen Yang, Weiya Xia, Mickey C.‐T. Hu,

Tópico(s)

Heat shock proteins research

Resumo

Genotoxic stress such as ionizing radiation can induce DNA damage and promote cell-cycle arrest or apoptosis through either a p53-dependent or -independent pathway. Recently, members of the FOXO Forkhead transcription factor family have been implicated in playing a role in both DNA repair and apoptosis in mammalian cells that promoted us to examine the role of FOXO transcription factors in ionizing radiation-induced apoptosis. Here, we show that ionizing radiation can promote FOXO3a (FKHRL1) transcriptional activity and protein expression level, and induce nuclear translocation of FOXO3a in Saos2, a p53-null osteosarcoma cell line. Ionizing radiation stimulates expression of apoptosis-inducing proteins such as Fas ligand and the Bcl-2 interacting mediator of cell death (Bim) leading to cellular apoptosis. The observed upregulation of proapoptotic genes and apoptosis in cells without p53 in response to ionizing radiation suggests a novel p53-independent mechanism underlying ionizing radiation-induced apoptosis in cancer cells.

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Ionizing radiation activates expression of FOXO3a, Fas ligand, and Bim, and induces cell apoptosis