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首页> 外文期刊>Nature cell biology >A non-canonical SWI/SNF complex is a synthetic lethal target in cancers driven by BAF complex perturbation
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A non-canonical SWI/SNF complex is a synthetic lethal target in cancers driven by BAF complex perturbation

机译:非规范的SWI / SNF复合物是由BAF复杂扰动驱动的癌症中的合成致死靶

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摘要

Mammalian SWI/SNF chromatin remodelling complexes exist in three distinct, final-form assemblies: canonical BAF (cBAF), PBAF and a newly characterized non-canonical complex (ncBAF). However, their complex-specific targeting on chromatin, functions and roles in disease remain largely undefined. Here, we comprehensively mapped complex assemblies on chromatin and found that ncBAF complexes uniquely localize to CTCF sites and promoters. We identified ncBAF subunits as synthetic lethal targets specific to synovial sarcoma and malignant rhabdoid tumours, which both exhibit cBAF complex (SMARCB1 subunit) perturbation. Chemical and biological depletion of the ncBAF subunit, BRD9, rapidly attenuates synovial sarcoma and malignant rhabdoid tumour cell proliferation. Importantly, in cBAF-perturbed cancers, ncBAF complexes maintain gene expression at retained CTCF-promoter sites and function in a manner distinct from fusion oncoprotein-bound complexes. Together, these findings unmask the unique targeting and functional roles of ncBAF complexes and present new cancer-specific therapeutic targets.
机译:哺乳动物SWI / SNF染色质重塑复合物存在于三个不同的最终形式的组件中:规范BAF(CBAF),PBAF和新表征的非规范复合物(NCBAF)。然而,它们对染色质,功能和作用的复杂靶向靶向仍然很大程度上是未定义的。在这里,我们全面映射了染色质的复杂组件,发现NCBAF复合物唯一地定位于CTCF位点和启动子。我们将NCBAF亚基确定为特异于滑膜肉瘤和恶性Rhabdoid肿瘤的合成致死靶标,这两种表现出CBAF复合物(SMARCB1亚基)扰动。 NCBAF亚基,BRD9的化学和生物耗竭,迅速衰减滑膜肉瘤和恶性Rhabdoid肿瘤细胞增殖。重要的是,在CBAF扰动的癌症中,NCBAF复合物在保留的CTCF-启动子位点保持基因表达,并以不同于融合癌蛋白结合复合物的方式起作用。这些研究结果在一起取消了NCBAF复合物的独特靶向和功能作用,并呈现了新的癌症特异性治疗目标。

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