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Therapeutic Opportunities of Targeting Canonical and Noncanonical PcG/TrxG Functions in Acute Myeloid Leukemia
Annual Review of Genomics and Human Genetics ( IF 7.7 ) Pub Date : 2021-08-31 , DOI: 10.1146/annurev-genom-111120-102443
Bernd B Zeisig 1, 2 , Chi Wai Eric So 1, 2
Affiliation  

Transcriptional deregulation is a key driver of acute myeloid leukemia (AML), a heterogeneous blood cancer with poor survival rates. Polycomb group (PcG) and Trithorax group (TrxG) genes, originally identified in Drosophila melanogaster several decades ago as master regulators of cellular identity and epigenetic memory, not only are important in mammalian development but also play a key role in AML disease biology. In addition to their classical canonical antagonistic transcriptional functions, noncanonical synergistic and nontranscriptional functions of PcG and TrxG are emerging. Here, we review the biochemical properties of major mammalian PcG and TrxG complexes and their roles in AML disease biology, including disease maintenance as well as drug resistance. We summarize current efforts on targeting PcG and TrxG for treatment of AML and propose rational synthetic lethality and drug-induced antagonistic pleiotropy options involving PcG and TrxG as potential new therapeutic avenues for treatment of AML.

中文翻译:



急性髓系白血病中针对经典和非经典 PcG/TrxG 功能的治疗机会



转录失调是急性髓系白血病(AML)的关键驱动因素,急性髓系白血病是一种生存率较低的异质性血癌。 Polycomb 组 (PcG) 和 Trithorax 组 (TrxG) 基因最初在几十年前在果蝇中被鉴定为细胞身份和表观遗传记忆的主要调节因子,不仅在哺乳动物发育中很重要,而且在 AML 疾病生物学中也发挥着关键作用。除了经典的经典拮抗转录功能外,PcG 和 TrxG 的非经典协同和非转录功能也正在出现。在这里,我们回顾了主要哺乳动物 PcG 和 TrxG 复合物的生化特性及其在 AML 疾病生物学中的作用,包括疾病维持和耐药性。我们总结了目前针对 PcG 和 TrxG 治疗 AML 的努力,并提出了涉及 PcG 和 TrxG 的合理合成致死性和药物诱导的拮抗多效性选择,作为治疗 AML 的潜在新治疗途径。

更新日期:2021-09-01
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