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The transcription factor GABP selectively binds and activates the mutant TERT promoter in cancer

机译:转录因子GABP在癌症中选择性结合并激活突变型TERT启动子

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摘要

Reactivation of telomerase reverse transcriptase (TERT) expression enables cells to overcome replicative senescence and escape apoptosis, fundamental steps in the initiation of human cancer. Multiple cancer types, including up to 83% of glioblastomas (GBM), harbor highly recurrent TERT promoter mutations of unknown function but specific to two nucleotide positions. We identify the functional consequence of these mutations in GBM to be recruitment of the multimeric GABP transcription factor specifically to the mutant promoter. Allelic recruitment of GABP is consistently observed across four cancer types, highlighting a shared mechanism underlying TERT reactivation. Tandem flanking native ETS motifs critically cooperate with these mutations to activate TERT, likely by facilitating GABP heterotetramer binding. GABP thus directly links TERT promoter mutations to aberrant expression in multiple cancers.
机译:端粒酶逆转录酶(TERT)表达的重新激活使细胞能够克服复制性衰老并逃脱凋亡,这是人类癌症发作的基本步骤。多种癌症类型,包括高达83%的胶质母细胞瘤(GBM),都具有功能未知但对两个核苷酸位置具有特异性的高复发性TERT启动子突变。我们确定在GBM中这些突变的功能性后果是募集了多聚GABP转录因子,专门针对突变启动子。在四种癌症类型中始终观察到GABP的等位基因募集,突显了TERT重新激活的共同机制。串联的天然ETS基序与这些突变关键地协作以激活TERT,可能是通过促进GABP异四聚体结合。因此,GABP直接将TERT启动子突变与多种癌症中的异常表达联系起来。

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