Publication: Potential options for managing LOX+ ER− breast cancer patients
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Date
2016
Published Version
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Impact Journals LLC
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Citation
Han, Yong, Shenyi Lian, Xingran Cui, Kexin Meng, Balázs Győrffy, Tao Jin, and Dongsheng Huang. 2016. “Potential options for managing LOX+ ER− breast cancer patients.” Oncotarget 7 (22): 32893-32901. doi:10.18632/oncotarget.9073. http://dx.doi.org/10.18632/oncotarget.9073.
Research Data
Abstract
Overexpression of lysyl oxidase (LOX) is often observed in estrogen receptor negative (ER–) breast cancer patients with bone metastasis. In the present bioinformatics study, we observed that LOX is a prognostic factor for poor progression free survival in patients with ER– breast cancer. LOX overexpression was positively correlated with resistance to radiation, doxorubin and mitoxantrone, but negatively correlated with resistance to bisphosphonate, PARP1 inhibitors, cisplatin, trabectedin and gemcitabine. LOX overexpression was also associated with EMT and stemness of cancer cells, which leads to chemotherapeutic resistance and poor outcome in ER– patients. Although we suggest several therapeutic interventions that may help in the management of LOX+ ER– breast cancer patients, experiments to validate the function of LOX in ER– breast cancer are still needed.
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Keywords
LOX, estrogen recepter, EMT, chemoresistance, bisphosphonates
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