Heme Oxygenase-1 Has an Antitumor Role in Breast Cancer

被引:51
作者
Ariel Gandini, Norberto [1 ]
Noelia Alonso, Eliana [1 ]
Eugenia Fermento, Maria [1 ]
Mascaro, Marilina [1 ]
Carlos Abba, Martin [2 ]
Pamela Colo, Georgina [1 ]
Arevalo, Julian [1 ,3 ]
Julia Ferronato, Maria [1 ]
Alejandra Guevara, Josefina [1 ]
Nunez, Myriam [4 ]
Pichel, Pamela [5 ]
Carlos Curino, Alejandro [1 ]
Marta Facchinetti, Maria [1 ]
机构
[1] UNS, CONICET, Inst Invest Bioquim Bahia Blanca INIBIBB, Lab Biol Canc,Dept Biol Bioquim & Farm, San Juan 670, RA-8000 Bahia Blanca, Buenos Aires, Argentina
[2] Univ Nacl La Plata, Fac Ciencias Med, CINIBA, La Plata, Buenos Aires, Argentina
[3] Hosp Interzonal Agudos Dr Jose Penna, Serv Patol, Bahia Blanca, Buenos Aires, Argentina
[4] Univ Buenos Aires, Fac Farm & Bioquim, Buenos Aires, DF, Argentina
[5] Hosp Municipal Agudos Dr Leonidas Lucero, Bahia Blanca, Buenos Aires, Argentina
关键词
heme oxygenase-1; breast; cancer; antitumor; TUMOR-GROWTH; NUCLEAR TRANSLOCATION; CONFERS RESISTANCE; CARBON-MONOXIDE; GASTRIC-CANCER; UP-REGULATION; EXPRESSION; INHIBITION; SURVIVAL; CELLS;
D O I
10.1089/ars.2018.7554
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Aims: Heme oxygenase-1 (HO-1) is an enzyme involved in cellular responses to oxidative stress and has also been shown to regulate processes related to cancer progression. In this regard, HO-1 has been shown to display a dual effect with either antitumor or protumor activity, which is also true for breast cancer (BC). In this work, we address this discrepancy regarding the role of HO-1 in BC. Results: HO-1 was detected in human BC tissues, and its protein levels correlated with reduced tumor size and longer overall survival time of patients, thus suggesting the clinical importance of HO-1 in this type of cancer. Contrariwise, nuclear localization of HO-1 correlated with higher tumor grade suggesting that the effect of HO-1 is dependent on its cellular localization. In vivo experiments showed that both pharmacological activation and genetic overexpression of HO-1 reduce the tumor burden in two different animal models of BC. Furthermore, the pharmacological and genetic activation of HO-1 in several BC cell lines reduce the cellular viability by inducing apoptosis and cell cycle arrest and decrease the cellular migration and invasion rates by modulating pathways involved in the epithelial-mesenchymal transition. Furthermore, HO-1 activation impaired in vivo the metastatic dissemination. Innovation and Conclusion: By using various BC cell lines and animal models as well as human tumor samples, we demonstrated that total HO-1 displays antitumor activities in BC. Furthermore, our study suggests that HO-1 subcellular localization may explain the differential effects observed for the protein in different tumor types.
引用
收藏
页码:2030 / 2049
页数:20
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