Transposable elements drive widespread expression of oncogenes in human cancers

转座元件驱动人类癌症中癌基因的广泛表达

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作者:Hyo Sik Jang # ,Nakul M Shah # ,Alan Y Du ,Zea Z Dailey ,Erica C Pehrsson ,Paula M Godoy ,David Zhang ,Daofeng Li ,Xiaoyun Xing ,Sungsu Kim ,David O'Donnell ,Jeffrey I Gordon ,Ting Wang

Abstract

Transposable elements (TEs) are an abundant and rich genetic resource of regulatory sequences1-3. Cryptic regulatory elements within TEs can be epigenetically reactivated in cancer to influence oncogenesis in a process termed onco-exaptation4. However, the prevalence and impact of TE onco-exaptation events across cancer types are poorly characterized. Here, we analyzed 7,769 tumors and 625 normal datasets from 15 cancer types, identifying 129 TE cryptic promoter-activation events involving 106 oncogenes across 3,864 tumors. Furthermore, we interrogated the AluJb-LIN28B candidate: the genetic deletion of the TE eliminated oncogene expression, while dynamic DNA methylation modulated promoter activity, illustrating the necessity and sufficiency of a TE for oncogene activation. Collectively, our results characterize the global profile of TE onco-exaptation and highlight this prevalent phenomenon as an important mechanism for promiscuous oncogene activation and ultimately tumorigenesis.

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