Fibroblasts regulate the transcriptional signature of human papillomavirus-positive keratinocytes

Claire D James; Rachel L Lewis; Austin J Witt; Christiane Carter; Nabiha M Rais; Xu Wang; Molly L Bristol

doi:10.1016/j.tvr.2024.200302

Fibroblasts regulate the transcriptional signature of human papillomavirus-positive keratinocytes

Tumour Virus Res. 2024 Dec 10:19:200302. doi: 10.1016/j.tvr.2024.200302. Online ahead of print.

Authors

Claire D James¹, Rachel L Lewis¹, Austin J Witt¹, Christiane Carter², Nabiha M Rais¹, Xu Wang¹, Molly L Bristol³

Affiliations

¹ Philips Institute for Oral Health Research, School of Dentistry, Virginia Commonwealth University (VCU), Richmond, VA, USA.
² VCU Massey Bioinformatics Shared Resource, Richmond, VA, USA.
³ Philips Institute for Oral Health Research, School of Dentistry, Virginia Commonwealth University (VCU), Richmond, VA, USA; VCU Massey Comprehensive Cancer Center, Richmond, VA, USA. Electronic address: [email protected].

Abstract

Persistent human papillomavirus (HPV) infection is necessary but insufficient for viral oncogenesis. Additional contributing co-factors, such as immune evasion and viral integration have been implicated in HPV-induced cancer progression. It is widely accepted that HPV + keratinocytes require co-culture with fibroblasts to maintain viral DNA as episomes. How fibroblasts regulate viral episome maintenance is a critical knowledge gap. Here we present comprehensive RNA sequencing and proteomic analysis demonstrating that coculture with fibroblasts is supportive of the viral life cycle, and is confirmatory of previous observations. Novel observations suggest that errors in "cross-talk" between fibroblasts and infected keratinocytes may regulate HPV integration and drive oncogenic progression. Our co-culture models offer new insights into HPV-related transformation mechanisms.

Keywords: EMT; Fibroblasts; Human papillomavirus; Microenvironment; Oropharyngeal cancer; Stroma; Transcriptional reprogramming.