HFE variants and the expression of iron-related proteins in breast cancer-associated lymphocytes and macrophages

A Waheed; A Waheed; A Walsh; Alexandra Rêma; Ana Rosa; B Halliwell; B Manger; Berta Martins da Silva; BK Abraham; Carlos Lopes; DB Kell; DM Paulnock; E Nemeth; E Nemeth; F D’Alessio; G Porto; Graça Porto; HJH Fenton; J Waalen; JA Lebron; JL Babitt; JL Babitt; JN Feder; JN Feder; JN Feder; JW Eaton; K Miyazono; Luciana Leite; M Kelley; M Vujic Spasic; NC Andrews; O Marques; O Marques; Oriana Marques; P Aguilar-Martinez; Paula Faustino; PJ Schmidt; S Duijn van; SG Gray; SY Lee; SY Lee; T Ganz; T Goswami

research

HFE variants and the expression of iron-related proteins in breast cancer-associated lymphocytes and macrophages

Authors: A Waheed
A Waheed
A Walsh
Alexandra Rêma
Ana Rosa
B Halliwell
B Manger
Berta Martins da Silva
BK Abraham
Carlos Lopes
DB Kell
DM Paulnock
E Nemeth
E Nemeth
F D’Alessio
G Porto
Graça Porto
HJH Fenton
J Waalen
JA Lebron
JL Babitt
JL Babitt
JN Feder
JN Feder
JN Feder
JW Eaton
K Miyazono
Luciana Leite
M Kelley
M Vujic Spasic
NC Andrews
O Marques
O Marques
Oriana Marques
P Aguilar-Martinez
Paula Faustino
PJ Schmidt
S Duijn van
SG Gray
SY Lee
SY Lee
T Ganz
T Goswami
Publication date: 27 December 2016
Publisher: 'Springer Science and Business Media LLC'
Doi

Abstract

Disponível em: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5264664/The association of HFE (High Iron FE) major variants with breast cancer risk and behavior has been a matter of discussion for a long time. However, their impact on the expression of iron-related proteins in the breast cancer tissue has never been addressed. In the present study, hepcidin, ferroportin 1, transferrin receptor 1 (TfR1), and ferritin expressions, as well as tissue iron deposition were evaluated in a collection of samples from breast cancers patients and analyzed according to the patients’ HFE genotype. Within the group of patients with invasive carcinoma, those carrying the p.Cys282Tyr variant in heterozygosity presented a higher expression of hepcidin in lymphocytes and macrophages than wild-type or p.His63Asp carriers. An increased expression of TfR1 was also observed in all the cell types analyzed but only in p.Cys282Tyr/p.His63Asp compound heterozygous patients. A differential impact of the two HFE variants was further noticed with the observation of a significantly higher percentage of p.Cys282Tyr heterozygous patients presenting tissue iron deposition in comparison to p.His63Asp heterozygous. In the present cohort, no significant associations were found between HFE variants and classical clinicopathological markers of breast cancer behavior and prognosis. Although limited by a low sampling size, our results provide a new possible explanation for the previously reported impact of HFE major variants on breast cancer progression, i.e., not by influencing systemic iron homeostasis but rather by differentially modulating the local cellular expression of iron-related proteins and tissue iron deposition.OM is a recipient of the PhD grant SFRH/BD/2011/78184 from Fundação para a Ciência e Tecnologia (FCT). The authors also acknowledge financial support from ICBAS/AI&NSUMIB and by national funds through FCT and Ministério da Educação e Ciência (MEC) and when applicable co-funded by FEDER funds within the partnership agreement PT2020 related with the research unit number 4293.info:eu-repo/semantics/publishedVersio