Chimera RNA transcribed from integrated HPV18 genome with adjacent host genomic region promotes oncogenic gene expression through condensate formation

子宮頸がん患者由来のHeLa細胞では、宿主ゲノムにヒトパピローマウイルス18型(HPV18)が挿入されています。この論文では、挿入されたHPV18から転写されるRNAが足場となって液滴様のボディが形成されることで、がん原遺伝子c-Mycの転写が過剰活性化されていることが明らかとなりました。

Abstract: Most cervical cancers are caused by human papillomavirus (HPV) infection. In HeLa cells, the HPV18 viral genome is integrated at chromosome 8q24.21 and activates transcription of the proto-oncogene c-Myc. However, the mechanism of how the integrated HPV genome and its transcribed RNAs exhibit transcription activation function has not been fully elucidated. In this study, we found that HPV18 transcripts contain an enhancer RNA-like function to activate proximal genes including CCAT1-5L and c-Myc. We showed that the human genome-integrated HPV18 genes are activated by transcription coregulators including BRD4 and Mediator. The transcribed HPV18 RNAs form a liquid-like condensate at chromosome 8q24.21 locus, which in turn accumulates RNA polymerase II. Moreover, we focused on a relatively uncharacterized transcript from the upstream region of CCAT1, named URC. The URC RNA is transcribed as a chimera RNA with HPV18 and is composed of the 3′-untranslated region of the HPV18 transcript. We experimentally showed that the URC contributes to stabilization of HPV18 RNAs by supplying a polyadenylation site for the HPV18 transcript. Our findings suggest that integrated HPV18 at 8q24.21 locus produces HPV18-URC chimera RNA and promotes tumorigenesis through RNA-based condensate formation.

Authors: Kazuki FurugoriHidefumi SuzukiRyota AbeKeiko HoriuchiTomohiko AkiyamaTomonori HiroseAtsushi ToyodaHidehisa Takahashi

Journal: Genes to Cells, 2024

DOI: 10.1111/gtc.13121