Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models

Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models

Abstract Background The gene desert on human chromosomal band 8q24 harbors multiple genetic variants associated with common cancers, including breast cancer. The locus, including the gene desert and its flanking genes, MYC, PVT1 and FAM84B, is also frequently amplified in human breast cancer. We gen...

Full description

Bibliographic Details
Main Authors: Collin Homer-Bouthiette, Yang Zhao, Lauren B. Shunkwiler, Benjamine Van Peel, Elizabeth Garrett-Mayer, Rachael C. Baird, Anna I. Rissman, Stephen T. Guest, Stephen P. Ethier, Manorama C. John, Patricia A. Powers, Jill D. Haag, Michael N. Gould, Bart M. G. Smits
Format: Article
Language:English
Published: BMC 2018-12-01
Series:BMC Cancer
Subjects:
Breast cancer susceptibility
Noncoding
SNP
Risk
GWAS
Murine
Online Access:http://link.springer.com/article/10.1186/s12885-018-5109-8
id doaj-b21bf55990924a71bc092663c943b4b4
record_format Article
collection DOAJ
language English
format Article
sources DOAJ
author Collin Homer-Bouthiette
Yang Zhao
Lauren B. Shunkwiler
Benjamine Van Peel
Elizabeth Garrett-Mayer
Rachael C. Baird
Anna I. Rissman
Stephen T. Guest
Stephen P. Ethier
Manorama C. John
Patricia A. Powers
Jill D. Haag
Michael N. Gould
Bart M. G. Smits
spellingShingle Collin Homer-Bouthiette
Yang Zhao
Lauren B. Shunkwiler
Benjamine Van Peel
Elizabeth Garrett-Mayer
Rachael C. Baird
Anna I. Rissman
Stephen T. Guest
Stephen P. Ethier
Manorama C. John
Patricia A. Powers
Jill D. Haag
Michael N. Gould
Bart M. G. Smits
Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
BMC Cancer
Breast cancer susceptibility
Noncoding
SNP
Risk
GWAS
Murine
author_facet Collin Homer-Bouthiette
Yang Zhao
Lauren B. Shunkwiler
Benjamine Van Peel
Elizabeth Garrett-Mayer
Rachael C. Baird
Anna I. Rissman
Stephen T. Guest
Stephen P. Ethier
Manorama C. John
Patricia A. Powers
Jill D. Haag
Michael N. Gould
Bart M. G. Smits
author_sort Collin Homer-Bouthiette
title Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
title_short Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
title_full Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
title_fullStr Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
title_full_unstemmed Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
title_sort deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer models
publisher BMC
series BMC Cancer
issn 1471-2407
publishDate 2018-12-01
description Abstract Background The gene desert on human chromosomal band 8q24 harbors multiple genetic variants associated with common cancers, including breast cancer. The locus, including the gene desert and its flanking genes, MYC, PVT1 and FAM84B, is also frequently amplified in human breast cancer. We generated a megadeletion (MD) mouse model lacking 430-Kb of sequence orthologous to the breast cancer-associated region in the gene desert. The goals were to examine the effect of the deletion on mammary cancer development and on transcript level regulation of the candidate genes within the locus. Methods The MD allele was engineered using the MICER system in embryonic stem cells and bred onto 3 well-characterized transgenic models for breast cancer, namely MMTV-PyVT, MMTV-neu and C3(1)-TAg. Mammary tumor growth, latency, multiplicity and metastasis were compared between homozygous MD and wild type mice carrying the transgenes. A reciprocal mammary gland transplantation assay was conducted to distinguish mammary cell-autonomous from non-mammary cell-autonomous anti-cancer effects. Gene expression analysis was done using quantitative real-time PCR. Chromatin interactions were evaluated by 3C. Gene-specific patient outcome data were analysed using the METABRIC and TCGA data sets through the cBioPortal website. Results Mice homozygous for the MD allele are viable, fertile, lactate sufficiently to nourish their pups, but maintain a 10% lower body weight mainly due to decreased adiposity. The deletion interferes with mammary tumorigenesis in mouse models for luminal and basal breast cancer. In the MMTV-PyVT model the mammary cancer-reducing effects of the allele are mammary cell-autonomous. We found organ-specific effects on transcript level regulation, with Myc and Fam84b being downregulated in mammary gland, prostate and mammary tumor samples. Through analysis using the METABRIC and TCGA datasets, we provide evidence that MYC and FAM84B are frequently co-amplified in breast cancer, but in contrast with MYC, FAM84B is frequently overexpressed in the luminal subtype, whereas MYC activity affect basal breast cancer outcomes. Conclusion Deletion of a breast cancer-associated non-protein coding region affects mammary cancer development in 3 transgenic mouse models. We propose Myc as a candidate susceptibility gene, regulated by the gene desert locus, and a potential role for Fam84b in modifying breast cancer development.
topic Breast cancer susceptibility
Noncoding
SNP
Risk
GWAS
Murine
url http://link.springer.com/article/10.1186/s12885-018-5109-8
work_keys_str_mv AT collinhomerbouthiette deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT yangzhao deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT laurenbshunkwiler deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT benjaminevanpeel deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT elizabethgarrettmayer deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT rachaelcbaird deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT annairissman deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT stephentguest deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT stephenpethier deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT manoramacjohn deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT patriciaapowers deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT jilldhaag deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT michaelngould deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
AT bartmgsmits deletionofthemurineorthologofthe8q24genedeserthasanticancereffectsintransgenicmammarycancermodels
_version_ 1724714246117261312
spelling doaj-b21bf55990924a71bc092663c943b4b42020-11-25T02:56:06ZengBMCBMC Cancer1471-24072018-12-0118111610.1186/s12885-018-5109-8Deletion of the murine ortholog of the 8q24 gene desert has anti-cancer effects in transgenic mammary cancer modelsCollin Homer-Bouthiette0Yang Zhao1Lauren B. Shunkwiler2Benjamine Van Peel3Elizabeth Garrett-Mayer4Rachael C. Baird5Anna I. Rissman6Stephen T. Guest7Stephen P. Ethier8Manorama C. John9Patricia A. Powers10Jill D. Haag11Michael N. Gould12Bart M. G. Smits13Department of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Public Health Sciences, Medical University of South CarolinaDepartment of Oncology, McArdle Laboratory for Cancer Research, University of Wisconsin School of Medicine and Public HealthDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaDepartment of Cell and Regenerative Biology, University of Wisconsin School of Medicine and Public HealthDepartment of Cell and Regenerative Biology, University of Wisconsin School of Medicine and Public HealthDepartment of Oncology, McArdle Laboratory for Cancer Research, University of Wisconsin School of Medicine and Public HealthDepartment of Oncology, McArdle Laboratory for Cancer Research, University of Wisconsin School of Medicine and Public HealthDepartment of Pathology and Laboratory Medicine, Medical University of South CarolinaAbstract Background The gene desert on human chromosomal band 8q24 harbors multiple genetic variants associated with common cancers, including breast cancer. The locus, including the gene desert and its flanking genes, MYC, PVT1 and FAM84B, is also frequently amplified in human breast cancer. We generated a megadeletion (MD) mouse model lacking 430-Kb of sequence orthologous to the breast cancer-associated region in the gene desert. The goals were to examine the effect of the deletion on mammary cancer development and on transcript level regulation of the candidate genes within the locus. Methods The MD allele was engineered using the MICER system in embryonic stem cells and bred onto 3 well-characterized transgenic models for breast cancer, namely MMTV-PyVT, MMTV-neu and C3(1)-TAg. Mammary tumor growth, latency, multiplicity and metastasis were compared between homozygous MD and wild type mice carrying the transgenes. A reciprocal mammary gland transplantation assay was conducted to distinguish mammary cell-autonomous from non-mammary cell-autonomous anti-cancer effects. Gene expression analysis was done using quantitative real-time PCR. Chromatin interactions were evaluated by 3C. Gene-specific patient outcome data were analysed using the METABRIC and TCGA data sets through the cBioPortal website. Results Mice homozygous for the MD allele are viable, fertile, lactate sufficiently to nourish their pups, but maintain a 10% lower body weight mainly due to decreased adiposity. The deletion interferes with mammary tumorigenesis in mouse models for luminal and basal breast cancer. In the MMTV-PyVT model the mammary cancer-reducing effects of the allele are mammary cell-autonomous. We found organ-specific effects on transcript level regulation, with Myc and Fam84b being downregulated in mammary gland, prostate and mammary tumor samples. Through analysis using the METABRIC and TCGA datasets, we provide evidence that MYC and FAM84B are frequently co-amplified in breast cancer, but in contrast with MYC, FAM84B is frequently overexpressed in the luminal subtype, whereas MYC activity affect basal breast cancer outcomes. Conclusion Deletion of a breast cancer-associated non-protein coding region affects mammary cancer development in 3 transgenic mouse models. We propose Myc as a candidate susceptibility gene, regulated by the gene desert locus, and a potential role for Fam84b in modifying breast cancer development.http://link.springer.com/article/10.1186/s12885-018-5109-8Breast cancer susceptibilityNoncodingSNPRiskGWASMurine

Similar Items