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组蛋白基因处的RNA聚合酶II可预测人类癌症的预后。

RNA polymerase II at histone genes predicts outcome in human cancer.

作者信息

Henikoff Steven, Zheng Ye, Paranal Ronald M, Xu Yiling, Greene Jacob E, Henikoff Jorja G, Russell Zachary R, Szulzewsky Frank, Thirimanne H Nayanga, Kugel Sita, Holland Eric C, Ahmad Kami

机构信息

Basic Sciences Division, Fred Hutchinson Cancer Center, Seattle, WA, USA.

Howard Hughes Medical Institute, Chevy Chase, MD, USA.

出版信息

Science. 2025 Jan 2;387(6735):737-743. doi: 10.1126/science.ads2169. Epub 2025 Feb 13.

Abstract

Genome-wide hypertranscription is common in human cancer and predicts poor prognosis. To understand how hypertranscription might drive cancer, we applied our formalin-fixed paraffin-embedded (FFPE)-cleavage under targeted accessible chromatin method for mapping RNA polymerase II (RNAPII) genome-wide in FFPE sections. We demonstrate global RNAPII elevations in mouse gliomas and assorted human tumors in small clinical samples and discover regional elevations corresponding to de novo HER2 amplifications punctuated by likely selective sweeps. RNAPII occupancy at S-phase-dependent histone genes correlated with WHO grade in meningiomas, accurately predicted rapid recurrence, and corresponded to whole-arm chromosome losses. Elevated RNAPII at histone genes in meningiomas and diverse breast cancers is consistent with histone production being rate-limiting for S-phase progression and histone gene hypertranscription driving overproliferation and aneuploidy in cancer, with general implications for precision oncology.

摘要

全基因组超转录在人类癌症中很常见,并预示着预后不良。为了了解超转录如何驱动癌症,我们应用了靶向可及染色质下福尔马林固定石蜡包埋(FFPE)切割方法,在FFPE切片中对全基因组的RNA聚合酶II(RNAPII)进行定位。我们在小鼠神经胶质瘤和小临床样本中的各种人类肿瘤中证实了全局RNAPII升高,并发现了与新生HER2扩增相对应的区域升高,这些扩增由可能的选择性清除所间断。脑膜瘤中S期依赖性组蛋白基因的RNAPII占据与世界卫生组织(WHO)分级相关,准确预测了快速复发,并与整条染色体丢失相对应。脑膜瘤和多种乳腺癌中组蛋白基因处RNAPII升高与组蛋白产生是S期进展的限速因素以及组蛋白基因超转录驱动癌症中的过度增殖和非整倍体一致,这对精准肿瘤学具有普遍意义。

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