β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort

β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort

Many malignancies that occur in high excess in kidney transplant recipients (KTRs) are due to viruses that thrive in the setting of immunosuppression. Keratinocyte carcinoma (KC), the most frequently occurring cancer type in KTR, has been associated with skin infection by human papillomavirus (HPV)...

Full description

Bibliographic Details
Main Authors: Cinzia Borgogna, Carlotta Olivero, Simone Lanfredini, Federica Calati, Marco De Andrea, Elisa Zavattaro, Paola Savoia, Elena Trisolini, Renzo Boldorini, Girish K. Patel, Marisa Gariglio
Format: Article
Language:English
Published: Frontiers Media S.A. 2018-02-01
Series:Frontiers in Microbiology
Subjects:
β-HPV
skin cancer
xenograft
carcinogenesis
organ transplant recipients
Online Access:http://journal.frontiersin.org/article/10.3389/fmicb.2018.00117/full
id doaj-86b1d25b933e444fb3045d410e727d4f
record_format Article
collection DOAJ
language English
format Article
sources DOAJ
author Cinzia Borgogna
Carlotta Olivero
Carlotta Olivero
Simone Lanfredini
Federica Calati
Marco De Andrea
Marco De Andrea
Elisa Zavattaro
Paola Savoia
Elena Trisolini
Renzo Boldorini
Girish K. Patel
Marisa Gariglio
spellingShingle Cinzia Borgogna
Carlotta Olivero
Carlotta Olivero
Simone Lanfredini
Federica Calati
Marco De Andrea
Marco De Andrea
Elisa Zavattaro
Paola Savoia
Elena Trisolini
Renzo Boldorini
Girish K. Patel
Marisa Gariglio
β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
Frontiers in Microbiology
β-HPV
skin cancer
xenograft
carcinogenesis
organ transplant recipients
author_facet Cinzia Borgogna
Carlotta Olivero
Carlotta Olivero
Simone Lanfredini
Federica Calati
Marco De Andrea
Marco De Andrea
Elisa Zavattaro
Paola Savoia
Elena Trisolini
Renzo Boldorini
Girish K. Patel
Marisa Gariglio
author_sort Cinzia Borgogna
title β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
title_short β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
title_full β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
title_fullStr β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
title_full_unstemmed β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient Cohort
title_sort β-hpv infection correlates with early stages of carcinogenesis in skin tumors and patient-derived xenografts from a kidney transplant recipient cohort
publisher Frontiers Media S.A.
series Frontiers in Microbiology
issn 1664-302X
publishDate 2018-02-01
description Many malignancies that occur in high excess in kidney transplant recipients (KTRs) are due to viruses that thrive in the setting of immunosuppression. Keratinocyte carcinoma (KC), the most frequently occurring cancer type in KTR, has been associated with skin infection by human papillomavirus (HPV) from the beta genus. In this report, we extend our previous investigation aimed at identifying the presence of active β-HPV infection in skin tumors from KTRs through detection of viral protein expression. Using a combination of antibodies raised against the E4 and L1 proteins of the β-genotypes, we were able to visualize infection in five tumors [one keratoacanthoma (KA), three actinic keratoses (AKs), and one seborrheic keratoses (SKs)] that were all removed from two patients who had been both transplanted twice, had developed multiple KCs, and presented with a long history of immunosuppression (>30 years). These infected tissues displayed intraepidermal hyperplasia and increased expression of the ΔNp63 protein, which extended into the upper epithelial layers. In addition, using a xenograft model system in nude mice displaying a humanized stromal bed in the site of grafting, we successfully engrafted three AKs, two of which were derived from the aforementioned KTRs and displayed β-HPV infection in the original tumor. Of note, one AK-derived xenograft, along with its ensuing lymph node metastasis, was diagnosed as squamous cell carcinoma (SCC). In the latter, both β-HPV infection and ΔNp63 expression were no longer detectable. Although the overall success rate of engrafting was very low, the results of this study show for the first time that β-HPV+ and ΔNp63+ intraepidermal hyperplasia can indeed progress to an aggressive SCC able to metastasize. Consistent with a series of reports attributing a causative role of β-HPV at early stages of skin carcinogenesis through ΔNp63 induction and increased keratinocytes stemness, here we provide in vivo evidence that these events are also occurring in the affected skin of KTRs. Due to these β-HPV-driven molecular pathways, the nascent tumor cell is able to acquire a high enough number of carcinogenic insults that its proliferation and survival will eventually become independent of viral gene expression.
topic β-HPV
skin cancer
xenograft
carcinogenesis
organ transplant recipients
url http://journal.frontiersin.org/article/10.3389/fmicb.2018.00117/full
work_keys_str_mv AT cinziaborgogna bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT carlottaolivero bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT carlottaolivero bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT simonelanfredini bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT federicacalati bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT marcodeandrea bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT marcodeandrea bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT elisazavattaro bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT paolasavoia bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT elenatrisolini bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT renzoboldorini bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT girishkpatel bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
AT marisagariglio bhpvinfectioncorrelateswithearlystagesofcarcinogenesisinskintumorsandpatientderivedxenograftsfromakidneytransplantrecipientcohort
_version_ 1725618653024485376
spelling doaj-86b1d25b933e444fb3045d410e727d4f2020-11-24T23:07:22ZengFrontiers Media S.A.Frontiers in Microbiology1664-302X2018-02-01910.3389/fmicb.2018.00117330215β-HPV Infection Correlates with Early Stages of Carcinogenesis in Skin Tumors and Patient-Derived Xenografts from a Kidney Transplant Recipient CohortCinzia Borgogna0Carlotta Olivero1Carlotta Olivero2Simone Lanfredini3Federica Calati4Marco De Andrea5Marco De Andrea6Elisa Zavattaro7Paola Savoia8Elena Trisolini9Renzo Boldorini10Girish K. Patel11Marisa Gariglio12Virology Unit, Department of Translational Medicine, Novara Medical School, University of Eastern Piedmont, Novara, ItalyVirology Unit, Department of Translational Medicine, Novara Medical School, University of Eastern Piedmont, Novara, ItalySchool of Biosciences, European Cancer Stem Cell Research Institute, Cardiff University, Cardiff, United KingdomSchool of Biosciences, European Cancer Stem Cell Research Institute, Cardiff University, Cardiff, United KingdomVirology Unit, Department of Translational Medicine, Novara Medical School, University of Eastern Piedmont, Novara, ItalyVirology Unit, Department of Translational Medicine, Novara Medical School, University of Eastern Piedmont, Novara, ItalyVirology Unit, Department of Public Health and Pediatric Sciences, Turin Medical School, University of Turin, Turin, ItalyDermatology Unit, Department of Health Sciences, Novara Medical School, Novara, ItalyDermatology Unit, Department of Health Sciences, Novara Medical School, Novara, ItalyPathology Unit, Department of Health Sciences, Novara Medical School, Novara, ItalyPathology Unit, Department of Health Sciences, Novara Medical School, Novara, ItalySchool of Biosciences, European Cancer Stem Cell Research Institute, Cardiff University, Cardiff, United KingdomVirology Unit, Department of Translational Medicine, Novara Medical School, University of Eastern Piedmont, Novara, ItalyMany malignancies that occur in high excess in kidney transplant recipients (KTRs) are due to viruses that thrive in the setting of immunosuppression. Keratinocyte carcinoma (KC), the most frequently occurring cancer type in KTR, has been associated with skin infection by human papillomavirus (HPV) from the beta genus. In this report, we extend our previous investigation aimed at identifying the presence of active β-HPV infection in skin tumors from KTRs through detection of viral protein expression. Using a combination of antibodies raised against the E4 and L1 proteins of the β-genotypes, we were able to visualize infection in five tumors [one keratoacanthoma (KA), three actinic keratoses (AKs), and one seborrheic keratoses (SKs)] that were all removed from two patients who had been both transplanted twice, had developed multiple KCs, and presented with a long history of immunosuppression (>30 years). These infected tissues displayed intraepidermal hyperplasia and increased expression of the ΔNp63 protein, which extended into the upper epithelial layers. In addition, using a xenograft model system in nude mice displaying a humanized stromal bed in the site of grafting, we successfully engrafted three AKs, two of which were derived from the aforementioned KTRs and displayed β-HPV infection in the original tumor. Of note, one AK-derived xenograft, along with its ensuing lymph node metastasis, was diagnosed as squamous cell carcinoma (SCC). In the latter, both β-HPV infection and ΔNp63 expression were no longer detectable. Although the overall success rate of engrafting was very low, the results of this study show for the first time that β-HPV+ and ΔNp63+ intraepidermal hyperplasia can indeed progress to an aggressive SCC able to metastasize. Consistent with a series of reports attributing a causative role of β-HPV at early stages of skin carcinogenesis through ΔNp63 induction and increased keratinocytes stemness, here we provide in vivo evidence that these events are also occurring in the affected skin of KTRs. Due to these β-HPV-driven molecular pathways, the nascent tumor cell is able to acquire a high enough number of carcinogenic insults that its proliferation and survival will eventually become independent of viral gene expression.http://journal.frontiersin.org/article/10.3389/fmicb.2018.00117/fullβ-HPVskin cancerxenograftcarcinogenesisorgan transplant recipients

Similar Items