BET抑制剂
溴尿嘧啶
医学
增强子
表观遗传学
癌症研究
白血病
融合蛋白
基因
细胞凋亡
淋巴细胞白血病
融合基因
DNA
生物
DNA损伤
基因表达调控
表型
癌基因蛋白质类
DNA甲基化
基因表达
BRD4
下调和上调
化学
作者
Aditi Chauhan,Kulwant Singh,Chandra Prakash Chaturvedi,Abhishek Kumar
标识
DOI:10.1080/10428194.2026.2614078
摘要
B-cell acute lymphoblastic leukemia harboring MEF2D-translocations represents an aggressive subtype with poor prognosis. MEF2D fusion proteins drive leukemogenesis via super enhancer mediated transcriptional dysregulation, making them promising target for epigenetic intervention. BET proteins, especially BRD4, are key regulators of oncogenic enhancer activity. Here, we explored the potential of BET protein inhibition as a targeted therapeutic strategy in MEF2D-HNRNPUL1 translocated B-ALL. Our study revealed that BET inhibitor inhibited proliferation and triggered apoptosis in leukemic cells, by targeting pre-BCR genes in addition to previously demonstrated targets, c-myc and IL-7R. A novel finding is that BET inhibitor induces DNA damage by downregulating DNA repair genes. These findings highlight that anti-leukemic activity of BET inhibitors offers a promising strategy to improve outcomes in this high-risk leukemia subtype.
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