BRD4
螺母
染色质
异位表达
细胞生物学
癌症研究
化学
生物
溴尿嘧啶
DNA
遗传学
组蛋白
物理
基因
声学
作者
Artyom A. Alekseyenko,Erica M. Walsh,Barry M. Zee,Tibor Pakozdi,Peter Hsi,Madeleine E. Lemieux,Paola Dal Cin,Tan A. Ince,Peter V. Kharchenko,Mitzi I. Kuroda,Christopher A. French
标识
DOI:10.1073/pnas.1702086114
摘要
Significance Chromatin factors generally act within large, multisubunit complexes; thus, identifying both their normal and aberrant interactors in cancer should provide important information regarding potential targets for therapeutic intervention. Here, we apply this principle to analysis of BRD4–NUT, a fusion oncoprotein that drives an aggressive subtype of squamous cell cancer. We identify ZNF532 as a prominent BRD4–NUT–interacting protein in an established NUT midline carcinoma patient cell line, and independently discover ZNF532 fused directly to NUT in a newly analyzed patient. Like BRD4–NUT, ZNF532–NUT forms unusually large (100-kb to 1-Mb) domains of hyperactive chromatin, including at the MYC locus, and drives self-reinforcing regulatory loops that are likely to be a powerful strategy for the growth advantage of cancer cells.
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