Tracking vaginal, anal and oral infection in a mouse papillomavirus infection model

Hu, Jiafen; Budgeon, Lynn R.; Cladel, Nancy M.; Balogh, Karla K.; Myers, Roland L.; Cooper, Timothy K.; Christensen, Neil D.

doi:10.1099/jgv.0.000295

Cited by 41 publications

(125 citation statements)

References 66 publications

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“…While we studied skin disease here, MmuPV1 also replicates at oral, anal, and vaginal sites, suggesting how this model might be further improved (80). Using mice with persistent benign MmuPV1 papillomas, we demonstrate immune-directed clearance through vaccination with a naked DNA, hCRT-mE6mE7mL2, administered with electroporation.…”

Section: Discussionmentioning

confidence: 99%

Spontaneous and Vaccine-Induced Clearance of Mus Musculus Papillomavirus 1 Infection

Jiang

Wang

Peng

et al. 2017

J Virol

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Mus musculus papillomavirus 1 (MmuPV1/MusPV1) induces persistent papillomas in immunodeficient mice but not in common laboratory strains. To facilitate the study of immune control, we sought an outbred and immunocompetent laboratory mouse strain in which persistent papillomas could be established. We found that challenge of SKH1 mice (Crl:SKH1-Hrhr) with MmuPV1 by scarification on their tail resulted in three clinical outcomes: (i) persistent (>2-month) papillomas (∼20%); (ii) transient papillomas that spontaneously regress, typically within 2 months (∼15%); and (iii) no visible papillomas and viral clearance (∼65%). SKH1 mice with persistent papillomas were treated by using a candidate preventive/therapeutic naked-DNA vaccine that expresses human calreticulin (hCRT) fused in frame to MmuPV1 E6 (mE6) and mE7 early proteins and residues 11 to 200 of the late protein L2 (hCRTmE6/mE7/mL2). Three intramuscular DNA vaccinations were delivered biweekly via in vivo electroporation, and both humoral and CD8 T cell responses were mapped and measured. Previously persistent papillomas disappeared within 2 months after the final vaccination. Coincident virologic clearance was confirmed by in situ hybridization and a failure of disease to recur after CD3 T cell depletion. Vaccination induced strong mE6 and mE7 CD8+ T cell responses in all mice, although they were significantly weaker in mice that initially presented with persistent warts than in those that spontaneously cleared their infection. A human papillomavirus 16 (HPV16)-targeted version of the DNA vaccine also induced L2 antibodies and protected mice from vaginal challenge with an HPV16 pseudovirus. Thus, MmuPV1 challenge of SKH1 mice is a promising model of spontaneous and immunotherapy-directed clearances of HPV-related disease.IMPORTANCE High-risk-type human papillomaviruses (hrHPVs) cause 5% of all cancer cases worldwide, notably cervical, anogenital, and oropharyngeal cancers. Since preventative HPV vaccines have not been widely used in many countries and do not impact existing infections, there is considerable interest in the development of therapeutic vaccines to address existing disease and infections. The strict tropism of HPV requires the use of animal papillomavirus models for therapeutic vaccine development. However, MmuPV1 failed to grow in common laboratory strains of mice with an intact immune system. We show that MmuPV1 challenge of the outbred immunocompetent SKH1 strain produces both transient and persistent papillomas and that vaccination of the mice with a DNA expressing an MmuPV1 E6E7L2 fusion with calreticulin can rapidly clear persistent papillomas. Furthermore, an HPV16-targeted version of the DNA can protect against vaginal challenge with HPV16, suggesting the promise of this approach to both prevent and treat papillomavirus-related disease.

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Section: Discussionmentioning

confidence: 99%

Spontaneous and Vaccine-Induced Clearance of Mus Musculus Papillomavirus 1 Infection

Jiang

Wang

Peng

et al. 2017

J Virol

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“…Conceptrol (Ortho Options, over the counter) as previously described . Tongues 519 were withdrawn using a sterile forceps and microneedles were used to wound the ventral surface 520 of the tongues (Cladel et al, 2016;Hu et al, 2015). Twenty-four hours after wounding, eight 521 female and six male Hsd: Nu athymic mice were again anesthetized and challenged with 522 infectious MmuPV1 virions (1×10 8 viral DNA equivalents) via the tail vein.…”

Section: Analyses 512mentioning

confidence: 99%

Papillomavirus can be transmitted through the blood and produce infections in blood recipients: Evidence from two animal models

Cladel

Jiang

et al. 2019

Preprint

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Human papillomavirus (HPV) infections are commonly thought to be strictly sexually transmitted. However, studies have demonstrated the presence of HPV in cancers of many non-sexual internal organs, raising the question as to how the viruses gain access to these sites. A possible connection between blood transfusion and HPV-associated disease has not received much attention. We show, in two animal models, that blood infected with papillomavirus yields infections at permissive sites. Furthermore, we demonstrate that blood from actively infected mice can transmit the infection to naïve animals. Finally, we report papillomavirus infections in the stomach tissues of animals infected via the blood. Stomach tissues are not known to be permissive for papillomavirus infection, although the literature suggests that HPVs may be associated with a subset of gastric cancers. These results indicate that the human blood supply, which is not screened for papillomaviruses, could be a potential source of HPV infection and subsequent cancers.SUMMARYHuman papillomaviruses cause 5% of human cancers. Currently, blood banks do not screen for these viruses. We demonstrate that blood transfused from papillomavirus-infected animals produces infections in recipients. Public health implications are significant if the same is true for humans.DefinitionsLocal papillomavirus infection: An infection initiated by the direct application of virus or viral DNA to the site of infectionIntravenous (IV) papillomavirus infection: An infection resulting from blood-borne delivery of virus or viral DNA to the site of infection.

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“…The virus can infect both cutaneous and mucosal epithelium (Cladel, Budgeon et al, 2013a; Cladel, Budgeon et al, 2015a;Hu, Budgeon et al, 2015)…”

Section: Preclinical Models (In Vivo)mentioning

confidence: 99%

“…Experiments have shown that back, muzzle and tail skin are susceptible sites and led the initial investigators to conclude that this virus shows a cutaneous tropism (Ingle, Ghim et al, 2011). However, additional studies demonstrated that secondary infections could be found in mucosal tissues of the vaginal, anal and oral cavities (Cladel, Budgeon et al, 2013a;Cladel, Budgeon et al, 2015b) and that infections could be experimentally induced at these sites with ease (Cladel, Budgeon et al, 2015a; Hu, Budgeon et al, 2015). More recent studies in our lab with several strains of mice with varying levels of immune deficiency have indicated that there are unknown mechanisms of altered tissue tropism in which vaginal sites in two strains show active and persistent infections whereas direct infection of tail skin showed no signs of clinical disease.…”

Section: Preclinical Models (In Vivo)mentioning

confidence: 99%

Recent advances in preclinical model systems for papillomaviruses

et al. 2017

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Preclinical model systems to study multiple features of the papillomavirus life cycle have greatly aided our understanding of Human Papillomavirus (HPV) biology, disease progression and treatments. The challenge to studying HPV in hosts is that HPV along with most PVs are both species and tissue restricted. Thus, fundamental properties of HPV viral proteins can be assessed in specialized cell culture systems but host responses that involve innate immunity and host restriction factors requires preclinical surrogate models. Fortunately, there are several well-characterized and new animal models of papillomavirus infections that are available to the PV research community. Old models that continue to have value include canine, bovine and rabbit PV models and new rodent models are in place to better assess host-virus interactions. Questions arise as to the strengths and weaknesses of animal PV models for HPV disease and how accurately these preclinical models predict malignant progression, vaccine efficacy and therapeutic control of HPV-associated disease. In this review, we examine current preclinical models and highlight the strengths and weaknesses of the various models as well as provide an update on new opportunities to study the numerous unknowns that persist in the HPV research field.

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Tracking vaginal, anal and oral infection in a mouse papillomavirus infection model

Cited by 41 publications

References 66 publications

Spontaneous and Vaccine-Induced Clearance of Mus Musculus Papillomavirus 1 Infection

Spontaneous and Vaccine-Induced Clearance of Mus Musculus Papillomavirus 1 Infection

Papillomavirus can be transmitted through the blood and produce infections in blood recipients: Evidence from two animal models

Recent advances in preclinical model systems for papillomaviruses

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