Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways

Abstract Background Human papillomavirus (HPV) infection causes around 90% of cervical cancer cases, and cervical cancer is a leading cause of female mortality worldwide. HPV-derived oncoprotein E7 participates in cervical carcinogenesis by inducing aberrant host DNA methylation. However, the target...

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Main Authors: Nopphamon Na Rangsee, Pattamawadee Yanatatsaneejit, Trairak Pisitkun, Poorichaya Somparn, Pornrutsami Jintaridth, Supachai Topanurak
Format: Article
Language:English
Published: BMC 2020-02-01
Series:Infectious Agents and Cancer
Subjects:
Online Access:https://doi.org/10.1186/s13027-020-0271-4
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spelling doaj-e86bf0b03c9049ea9be9c708b8d4b5132021-02-07T12:10:23ZengBMCInfectious Agents and Cancer1750-93782020-02-0115111810.1186/s13027-020-0271-4Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathwaysNopphamon Na Rangsee0Pattamawadee Yanatatsaneejit1Trairak Pisitkun2Poorichaya Somparn3Pornrutsami Jintaridth4Supachai Topanurak5Department of Molecular Tropical Medicine and Genetics, Faculty of Tropical Medicine, Mahidol UniversityDepartment of Botany, Faculty of Science, Chulalongkorn UniversityCenter of Excellence in Systems Biology, Faculty of Medicine, Chulalongkorn UniversityCenter of Excellence in Systems Biology, Faculty of Medicine, Chulalongkorn UniversityDepartment of Tropical Nutrition and Food Science, Faculty of Tropical Medicine, Mahidol UniversityDepartment of Molecular Tropical Medicine and Genetics, Faculty of Tropical Medicine, Mahidol UniversityAbstract Background Human papillomavirus (HPV) infection causes around 90% of cervical cancer cases, and cervical cancer is a leading cause of female mortality worldwide. HPV-derived oncoprotein E7 participates in cervical carcinogenesis by inducing aberrant host DNA methylation. However, the targeting specificity of E7 methylation of host genes is not fully understood but is important in the down-regulation of crucial proteins of the hallmark cancer pathways. In this study, we aim to link E7-driven aberrations in the host proteome to corresponding gene promoter hypermethylation events in the hope of providing novel therapeutic targets and biomarkers to indicate the progression of cervical cancer. Methods HEK293 cells were transfected with pcDNA3.1-E7 plasmid and empty vector and subjected to mass spectrometry-based proteomic analysis. Down-regulated proteins (where relative abundance was determined significant by paired T-test) relevant to cancer pathways were selected as gene candidates for mRNA transcript abundance measurement by qPCR and expression compared with that in SiHa cells (HPV type 16 positive). Methylation Specific PCR was used to determine promoter hypermethylation in genes downregulated in both SiHa and transfected HEK293 cell lines. The FunRich and STRING databases were used for identification of potential regulatory transcription factors and the proteins interacting with transcription factor gene candidates, respectively. Results Approximately 400 proteins totally were identified in proteomics analysis. The transcripts of six genes involved in the host immune response and cell proliferation (PTMS, C1QBP, BCAP31, CDKN2A, ZMYM6 and HIST1H1D) were down-regulated, corresponding to proteomic results. Methylation assays showed four gene promoters (PTMS, C1QBP, BCAP31 and CDKN2A) were hypermethylated with 61, 55.5, 70 and 78% increased methylation, respectively. Those four genes can be regulated by the GA-binding protein alpha chain, specificity protein 1 and ETS-like protein-1 transcription factors, as identified from FunRich database predictions. Conclusions HPV E7 altered the HEK293 proteome, particularly with respect to proteins involved in cell proliferation and host immunity. Down-regulation of these proteins appears to be partly mediated via host DNA methylation. E7 possibly complexes with the transcription factors of its targeting genes and DNMT1, allowing methylation of specific target gene promoters.https://doi.org/10.1186/s13027-020-0271-4DNA methylationEpigeneticsProteomicsCervical cancerHuman papilloma virusViral oncoproteins
collection DOAJ
language English
format Article
sources DOAJ
author Nopphamon Na Rangsee
Pattamawadee Yanatatsaneejit
Trairak Pisitkun
Poorichaya Somparn
Pornrutsami Jintaridth
Supachai Topanurak
spellingShingle Nopphamon Na Rangsee
Pattamawadee Yanatatsaneejit
Trairak Pisitkun
Poorichaya Somparn
Pornrutsami Jintaridth
Supachai Topanurak
Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
Infectious Agents and Cancer
DNA methylation
Epigenetics
Proteomics
Cervical cancer
Human papilloma virus
Viral oncoproteins
author_facet Nopphamon Na Rangsee
Pattamawadee Yanatatsaneejit
Trairak Pisitkun
Poorichaya Somparn
Pornrutsami Jintaridth
Supachai Topanurak
author_sort Nopphamon Na Rangsee
title Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
title_short Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
title_full Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
title_fullStr Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
title_full_unstemmed Host proteome linked to HPV E7-mediated specific gene hypermethylation in cancer pathways
title_sort host proteome linked to hpv e7-mediated specific gene hypermethylation in cancer pathways
publisher BMC
series Infectious Agents and Cancer
issn 1750-9378
publishDate 2020-02-01
description Abstract Background Human papillomavirus (HPV) infection causes around 90% of cervical cancer cases, and cervical cancer is a leading cause of female mortality worldwide. HPV-derived oncoprotein E7 participates in cervical carcinogenesis by inducing aberrant host DNA methylation. However, the targeting specificity of E7 methylation of host genes is not fully understood but is important in the down-regulation of crucial proteins of the hallmark cancer pathways. In this study, we aim to link E7-driven aberrations in the host proteome to corresponding gene promoter hypermethylation events in the hope of providing novel therapeutic targets and biomarkers to indicate the progression of cervical cancer. Methods HEK293 cells were transfected with pcDNA3.1-E7 plasmid and empty vector and subjected to mass spectrometry-based proteomic analysis. Down-regulated proteins (where relative abundance was determined significant by paired T-test) relevant to cancer pathways were selected as gene candidates for mRNA transcript abundance measurement by qPCR and expression compared with that in SiHa cells (HPV type 16 positive). Methylation Specific PCR was used to determine promoter hypermethylation in genes downregulated in both SiHa and transfected HEK293 cell lines. The FunRich and STRING databases were used for identification of potential regulatory transcription factors and the proteins interacting with transcription factor gene candidates, respectively. Results Approximately 400 proteins totally were identified in proteomics analysis. The transcripts of six genes involved in the host immune response and cell proliferation (PTMS, C1QBP, BCAP31, CDKN2A, ZMYM6 and HIST1H1D) were down-regulated, corresponding to proteomic results. Methylation assays showed four gene promoters (PTMS, C1QBP, BCAP31 and CDKN2A) were hypermethylated with 61, 55.5, 70 and 78% increased methylation, respectively. Those four genes can be regulated by the GA-binding protein alpha chain, specificity protein 1 and ETS-like protein-1 transcription factors, as identified from FunRich database predictions. Conclusions HPV E7 altered the HEK293 proteome, particularly with respect to proteins involved in cell proliferation and host immunity. Down-regulation of these proteins appears to be partly mediated via host DNA methylation. E7 possibly complexes with the transcription factors of its targeting genes and DNMT1, allowing methylation of specific target gene promoters.
topic DNA methylation
Epigenetics
Proteomics
Cervical cancer
Human papilloma virus
Viral oncoproteins
url https://doi.org/10.1186/s13027-020-0271-4
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