Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer

Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer

Abstract Background Oestrogen receptor-positive (ER+) breast cancer is commonly treated using endocrine therapies such as aromatase inhibitors which block synthesis of oestradiol, but the influence of this therapy on the immune composition of breast tumours has not been fully explored. Previous find...

Full description

Bibliographic Details
Main Authors: Jody Hazlett, Virginia Niemi, Aziz Aiderus, Katelyn Powell, Lyn Wise, Roslyn Kemp, Anita K. Dunbier
Format: Article
Language:English
Published: BMC 2021-10-01
Series:Breast Cancer Research
Subjects:
Non-steroidal anti-inflammatory drugs
Oestrogen receptor
Breast cancer
Endocrine therapy
Online Access:https://doi.org/10.1186/s13058-021-01472-1
id doaj-1bf3059867b54fb0bf092fe3619971c0
record_format Article
spelling doaj-1bf3059867b54fb0bf092fe3619971c02021-10-10T11:12:49ZengBMCBreast Cancer Research1465-542X2021-10-0123111510.1186/s13058-021-01472-1Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancerJody Hazlett0Virginia Niemi1Aziz Aiderus2Katelyn Powell3Lyn Wise4Roslyn Kemp5Anita K. Dunbier6Department of Biochemistry, University of OtagoDepartment of Microbiology and Immunology, University of OtagoDepartment of Biochemistry, University of OtagoDepartment of Biochemistry, University of OtagoDepartment of Pharmacology and Toxicology, University of OtagoDepartment of Microbiology and Immunology, University of OtagoDepartment of Biochemistry, University of OtagoAbstract Background Oestrogen receptor-positive (ER+) breast cancer is commonly treated using endocrine therapies such as aromatase inhibitors which block synthesis of oestradiol, but the influence of this therapy on the immune composition of breast tumours has not been fully explored. Previous findings suggest that tumour infiltrating lymphocytes and immune-related gene expression may be altered by treatment with aromatase inhibitors. However, whether these changes are a direct result of impacts on the host immune system or mediated through tumour cells is not known. We aimed to investigate the effect of oestrogen deprivation on the expression of chemokines and immune infiltration in vitro and in an ER+ immunocompetent mouse model. Methods RT-qPCR and a bead-based Bioplex system were used to investigate the expression of chemokines in MCF-7 breast cancer cells deprived of oestrogen. A migration assay and flow cytometry were used to measure the migration of human peripheral blood mononuclear cells (PBMCs) to MCF-7 cells grown without the main biologically active oestrogen, oestradiol. Using flow cytometry and immunohistochemistry, we examined the immune cell infiltrate into tumours created by injecting SSM3 ER+ breast cancer cells into wild-type, immunocompetent 129/SvEv mice. Results This study demonstrates that oestrogen deprivation increases breast cancer secretion of TNF, CCL5, IL-6, IL-8, and CCL22 and alters total human peripheral blood mononuclear cell migration in an in vitro assay. Oestrogen deprivation of breast cancer cells increases migration of CD4+ T cells and decreases migration of CD11c+ and CD14+ PBMC towards cancer cells. PBMC migration towards breast cancer cells can be reduced by treatment with the non-steroidal anti-inflammatory drugs, aspirin and celecoxib. Treatment with endocrine therapy using the aromatase inhibitor letrozole increases CD4+ T cell infiltration into ER+ breast cancer tumours in immune competent mice. Conclusions These results suggest that anti-oestrogen treatment of ER+ breast cancer cells can alter cytokine production and immune cells in the area surrounding the cancer cells. These findings may have implications for the combination and timing of anti-oestrogen therapies with other therapies.https://doi.org/10.1186/s13058-021-01472-1Non-steroidal anti-inflammatory drugsOestrogen receptorBreast cancerEndocrine therapy
collection DOAJ
language English
format Article
sources DOAJ
author Jody Hazlett
Virginia Niemi
Aziz Aiderus
Katelyn Powell
Lyn Wise
Roslyn Kemp
Anita K. Dunbier
spellingShingle Jody Hazlett
Virginia Niemi
Aziz Aiderus
Katelyn Powell
Lyn Wise
Roslyn Kemp
Anita K. Dunbier
Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
Breast Cancer Research
Non-steroidal anti-inflammatory drugs
Oestrogen receptor
Breast cancer
Endocrine therapy
author_facet Jody Hazlett
Virginia Niemi
Aziz Aiderus
Katelyn Powell
Lyn Wise
Roslyn Kemp
Anita K. Dunbier
author_sort Jody Hazlett
title Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
title_short Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
title_full Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
title_fullStr Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
title_full_unstemmed Oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
title_sort oestrogen deprivation induces chemokine production and immune cell recruitment in in vitro and in vivo models of oestrogen receptor-positive breast cancer
publisher BMC
series Breast Cancer Research
issn 1465-542X
publishDate 2021-10-01
description Abstract Background Oestrogen receptor-positive (ER+) breast cancer is commonly treated using endocrine therapies such as aromatase inhibitors which block synthesis of oestradiol, but the influence of this therapy on the immune composition of breast tumours has not been fully explored. Previous findings suggest that tumour infiltrating lymphocytes and immune-related gene expression may be altered by treatment with aromatase inhibitors. However, whether these changes are a direct result of impacts on the host immune system or mediated through tumour cells is not known. We aimed to investigate the effect of oestrogen deprivation on the expression of chemokines and immune infiltration in vitro and in an ER+ immunocompetent mouse model. Methods RT-qPCR and a bead-based Bioplex system were used to investigate the expression of chemokines in MCF-7 breast cancer cells deprived of oestrogen. A migration assay and flow cytometry were used to measure the migration of human peripheral blood mononuclear cells (PBMCs) to MCF-7 cells grown without the main biologically active oestrogen, oestradiol. Using flow cytometry and immunohistochemistry, we examined the immune cell infiltrate into tumours created by injecting SSM3 ER+ breast cancer cells into wild-type, immunocompetent 129/SvEv mice. Results This study demonstrates that oestrogen deprivation increases breast cancer secretion of TNF, CCL5, IL-6, IL-8, and CCL22 and alters total human peripheral blood mononuclear cell migration in an in vitro assay. Oestrogen deprivation of breast cancer cells increases migration of CD4+ T cells and decreases migration of CD11c+ and CD14+ PBMC towards cancer cells. PBMC migration towards breast cancer cells can be reduced by treatment with the non-steroidal anti-inflammatory drugs, aspirin and celecoxib. Treatment with endocrine therapy using the aromatase inhibitor letrozole increases CD4+ T cell infiltration into ER+ breast cancer tumours in immune competent mice. Conclusions These results suggest that anti-oestrogen treatment of ER+ breast cancer cells can alter cytokine production and immune cells in the area surrounding the cancer cells. These findings may have implications for the combination and timing of anti-oestrogen therapies with other therapies.
topic Non-steroidal anti-inflammatory drugs
Oestrogen receptor
Breast cancer
Endocrine therapy
url https://doi.org/10.1186/s13058-021-01472-1
work_keys_str_mv AT jodyhazlett oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT virginianiemi oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT azizaiderus oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT katelynpowell oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT lynwise oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT roslynkemp oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
AT anitakdunbier oestrogendeprivationinduceschemokineproductionandimmunecellrecruitmentininvitroandinvivomodelsofoestrogenreceptorpositivebreastcancer
_version_ 1716829882966605824

Similar Items