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Genomic characterization of genes encoding histone acetylation modulator proteins identifies therapeutic targets for cancer treatment

机译:编码组蛋白乙酰化调节蛋白的基因的基因组鉴定确定了癌症治疗的靶标

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摘要

A growing emphasis in anticancer drug discovery efforts has been on targeting histone acetylation modulators. Here we comprehensively analyze the genomic alterations of the genes encoding histone acetylation modulator proteins (HAMPs) in the Cancer Genome Atlas cohort and observe that HAMPs have a high frequency of focal copy number alterations and recurrent mutations, whereas transcript fusions of HAMPs are relatively rare genomic events in common adult cancers. Collectively, 86.3% (63/73) of HAMPs have recurrent alterations in at least 1 cancer type and 16 HAMPs, including 9 understudied HAMPs, are identified as putative therapeutic targets across multiple cancer types. For example, the recurrent focal amplification of BRD9 is observed in 9 cancer types and genetic depletion of BRD9 inhibits tumor growth. Our systematic genomic analysis of HAMPs across a large-scale cancer specimen cohort may facilitate the identification and prioritization of potential drug targets and selection of suitable patients for precision treatment.
机译:在抗癌药物发现工作中,越来越多的重点放在靶向组蛋白乙酰化调节剂上。在这里,我们全面分析了癌症基因组图集中编码组蛋白乙酰化调节蛋白(HAMPs)的基因的基因组变化,并观察到HAMPs的焦点拷贝数变化和复发突变的发生频率很高,而HAMPs的转录本融合是相对罕见的基因组常见成人癌症中的事件。总体上,至少有1种癌症类型中86.3%(63/73)的HAMP具有复发性改变,并且将16种HAMP(包括9种研究不足的HAMP)确定为多种癌症的推定治疗靶标。例如,在9种癌症类型中观察到了BRD9的复发性局灶性扩增,并且BRD9的遗传耗竭抑制了肿瘤的生长。我们对大规模癌症样本队列中的HAMP进行系统的基因组分析,可能有助于识别和确定潜在药物靶标的优先次序,并选择合适的患者进行精确治疗。

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