Genomic structures and regulation patterns at HPV integration sites in cervical cancer

Author:

Porter Vanessa L.ORCID,O’Neill KieranORCID,MacLennan SigneORCID,Corbett Richard D.,Ng MichelleORCID,Culibrk LukaORCID,Hamadeh Zeid,Iden MarissaORCID,Schmidt Rachel,Tsaih Shirng-Wern,Chang GlennORCID,Fan Jeremy,Nip Ka MingORCID,Akbari VahidORCID,Chan Simon K.,Hopkins James,Moore Richard A.,Chuah Eric,Mungall Karen L.,Mungall Andrew J.ORCID,Birol InancORCID,Jones Steven J. M.ORCID,Rader Janet S.ORCID,Marra Marco A.ORCID

Abstract

AbstractHuman papillomavirus (HPV) integration has been implicated in transforming HPV infection into cancer, but its genomic consequences have been difficult to study using short-read technologies. To resolve the dysregulation associated with HPV integration, we performed long-read sequencing on 63 cervical cancer genomes. We identified six categories of integration events based on HPV-human genomic structures. Of all HPV integrants, defined as two HPV-human breakpoints bridged by an HPV sequence, 24% contained variable copies of HPV between the breakpoints, a phenomenon we termed heterologous integration. Analysis of DNA methylation within and in proximity to the HPV genome at individual integration events revealed relationships between methylation status of the integrant and its orientation and structure. Dysregulation of the human epigenome and neighboring gene expression inciswith the HPV-integrated allele was observed over megabase-ranges of the genome. By elucidating the structural, epigenetic, and allele-specific impacts of HPV integration, we provide insight into the role of integrated HPV in cervical cancer.

Publisher

Cold Spring Harbor Laboratory

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