GSK-3 促进 CREB 与其共激活因子的条件性结合,与 MEIS1 一起促进 HOX 介导的转录和肿瘤发生。
GSK-3 promotes conditional association of CREB and its coactivators with MEIS1 to facilitate HOX-mediated transcription and oncogenesis.
机构信息
Department of Pathology, Stanford University School of Medicine, Stanford, CA 94305, USA.
出版信息
Cancer Cell. 2010 Jun 15;17(6):597-608. doi: 10.1016/j.ccr.2010.04.024.
Abstract
Acute leukemias induced by MLL chimeric oncoproteins are among the subset of cancers distinguished by a paradoxical dependence on GSK-3 kinase activity for sustained proliferation. We demonstrate here that GSK-3 maintains the MLL leukemia stem cell transcriptional program by promoting the conditional association of CREB and its coactivators TORC and CBP with homedomain protein MEIS1, a critical component of the MLL-subordinate program, which in turn facilitates HOX-mediated transcription and transformation. This mechanism also applies to hematopoietic cells transformed by other HOX genes, including CDX2, which is highly expressed in a majority of acute myeloid leukemias, thus providing a molecular approach based on GSK-3 inhibitory strategies to target HOX-associated transcription in a broad spectrum of leukemias.
摘要
由 MLL 嵌合癌蛋白诱导的急性白血病是一类以对 GSK-3 激酶活性持续增殖的依赖性为特征的癌症亚类。我们在此证明,GSK-3 通过促进 CREB 与其共激活因子 TORC 和 CBP 与同源域蛋白 MEIS1 的条件关联来维持 MLL 白血病干细胞转录程序,MEIS1 是 MLL 下属程序的关键组成部分,这反过来又促进了 HOX 介导的转录和转化。该机制也适用于由其他 HOX 基因(包括在大多数急性髓细胞白血病中高度表达的 CDX2)转化的造血细胞,从而为基于 GSK-3 抑制策略的靶向 HOX 相关转录的分子方法提供了广泛的白血病。
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