Inactivating CUX1 mutations promote tumorigenesis

失活 CUX1 突变促进肿瘤发生

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作者：Chi C Wong, Inigo Martincorena, Alistair G Rust, Mamunur Rashid, Constantine Alifrangis, Ludmil B Alexandrov, Jessamy C Tiffen, Christina Kober; Chronic Myeloid Disorders Working Group of the International Cancer Genome Consortium; Anthony R Green, Charles E Massie, Jyoti Nangalia, Stella Lempidaki,

期刊：

Nature Genetics

影响因子：

31.700

时间：

2014

起止号：

2014 Jan;46(1):33-8.

doi：

10.1038/ng.2846

方法学：

研究方向：

肿瘤

Abstract

A major challenge in cancer genetics is to determine which low-frequency somatic mutations are drivers of tumorigenesis. Here we interrogate the genomes of 7,651 diverse human cancers and find inactivating mutations in the homeodomain transcription factor gene CUX1 (cut-like homeobox 1) in ~1-5% of various tumors. Meta-analysis of CUX1 mutational status in 2,519 cases of myeloid malignancies reveals disruptive mutations associated with poor survival, highlighting the clinical significance of CUX1 loss. In parallel, we validate CUX1 as a bona fide tumor suppressor using mouse transposon-mediated insertional mutagenesis and Drosophila cancer models. We demonstrate that CUX1 deficiency activates phosphoinositide 3-kinase (PI3K) signaling through direct transcriptional downregulation of the PI3K inhibitor PIK3IP1 (phosphoinositide-3-kinase interacting protein 1), leading to increased tumor growth and susceptibility to PI3K-AKT inhibition. Thus, our complementary approaches identify CUX1 as a pan-driver of tumorigenesis and uncover a potential strategy for treating CUX1-mutant tumors.

Inactivating CUX1 mutations promote tumorigenesis

失活 CUX1 突变促进肿瘤发生

Abstract

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