Epm2a suppresses tumor growth in an immunocompromised host by inhibiting Wnt signaling

Artigo Acesso aberto Revisado por pares

Epm2a suppresses tumor growth in an immunocompromised host by inhibiting Wnt signaling

2006; Cell Press; Volume: 10; Issue: 3 Linguagem: Inglês

10.1016/j.ccr.2006.08.008

ISSN

1878-3686

Autores

Yin Wang, Yan Liu, Cindy Wu, Huiming Zhang, Xincheng Zheng, Zhi Zheng, Terrence L. Geiger, Gerard J. Nuovo, Yang Liu, Pan Zheng,

Tópico(s)

Genetics and Neurodevelopmental Disorders

Resumo

The genetic mechanisms responsible for increased incidence of lymphoma in immunocompromised individuals have not been fully elucidated. We show that, in a line of TCR transgenic TG-B mice, an insertional mutation in one allele of the Epm2a locus and epigenetic silencing of another led to a high rate of lymphoma with early onset. Overexpressing Epm2a suppressed the growth of established tumor cells and the development of lymphoma in the TG-B mice, while specific silencing of the locus increased tumorigenesis in the immune-deficient host. Downregulation of Epm2a expression is widespread among mouse and human lymphoma cell lines. Epm2a-encoded laforin is a phosphatase for GSK-3β and an important repressor in the Wnt signaling pathway. Inactivation of Epm2a resulted in increased Wnt signaling and tumorigenesis.

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Epm2a suppresses tumor growth in an immunocompromised host by inhibiting Wnt signaling