Invasive cancer and spontaneous regression two weeks after papillomavirus infection

Author:

Bilger AndreaORCID,Ward-Shaw Ella T.,Lee Denis L.,King Renee E.ORCID,Newton Michael A.ORCID,Buehler Darya,Matkowskyj Kristina A.ORCID,Sundberg John P.ORCID,Hu Rong,Lambert Paul F.ORCID

Abstract

AbstractDevelopment of invasive cancer in mammals is thought to require months or years after initial events such as mutation or viral infection. Rarely, invasive cancers regress spontaneously. We show that cancers can develop and regress on a timescale of weeks, not months or years. Invasive squamous cell carcinomas developed in normal adult, immune-competent mice as soon as 2 weeks after infection with mouse papillomavirus MmuPV1. Tumor development, regression or persistence was tissue- and strain-dependent. Cancers in infected mice developed rapidly at sites also prone to papillomavirus-induced tumors and cancers in humans – the throat, anus, and skin – and their frequency was increased in mice constitutively expressing the papillomavirus E5 oncogene, which MmuPV1 lacks. Cancers and dysplasia in the throat and anus regressed completely within 4-8 weeks of infection; however, skin lesions in the ear persisted. T-cell depletion in the mouse showed that regression of throat and anal tumors requires T cells. We conclude that papillomavirus infection suffices for rapid onset of invasive cancer, and persistence of lesions depends on factors including tissue type and host immunity. The speed of these events should promote rapid progress in the study of viral cancer development, persistence, and regression.Summary Graphic

Publisher

Cold Spring Harbor Laboratory

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