Article

CIP2A is a target of bortezomib in human triple negative breast cancer cells.

Institute of Biopharmaceutical Sciences, National Yang-Ming University, No, 155 Sec, 2 Li-Nong Street, Taipei 112, Taiwan. .
Breast cancer research: BCR (impact factor: 5.24). 04/2012; 14(2):R68. DOI:10.1186/bcr3175 pp.R68
Source: PubMed

ABSTRACT Triple negative breast cancer (TNBC) is very aggressive and currently has no specific therapeutic targets, such as hormone receptors or human epidermal growth factor receptor type 2 (HER2); therefore, prognosis is poor. Bortezomib, a proteasome inhibitor, may exert efficacy in TNBC through its multiple cellular effects. Here, we tested the efficacy of bortezomib and examined the drug mechanism in breast cancer cells.
Five breast cancer cell lines: TNBC HCC-1937, MDA-MB-231, and MDA-MB-468; HER2-overexpressing MDA-MB-453; and estrogen receptor positive MCF-7 were used for in vitro studies. Apoptosis was examined by both flow cytometry and Western Blot. Signal transduction pathways in cells were assessed by Western Blot. Gene silencing was done by small interfering RNA (siRNA). In vivo efficacy of bortezomib was tested in nude mice with breast cancer xenografts. Immunohistochemical study was performed on tumor tissues from patients with TNBC.
Bortezomib induced significant apoptosis, which was independent of its proteasome inhibition, in the three TNBC cell lines, but not in MDA-MB-453 or MCF-7 cells. Furthermore, cancerous inhibitor of protein phosphatase 2A (CIP2A), a cellular inhibitor of protein phosphatase 2A (PP2A), mediated the apoptotic effect of bortezomib. We showed that bortezomib inhibited CIP2A in association with p-Akt downregulation in a dose- and time-dependent manner in all sensitive TNBC cells, whereas no alterations in CIP2A expression and p-Akt were noted in bortezomib-resistant cells. Overexpression of CIP2A upregulated p-Akt and protected MDA-MB-231 and MDA-MB-468 cells from bortezomib-induced apoptosis, whereas silencing CIP2A by siRNA overcame the resistance to bortezomib-induced apoptosis in MCF-7 cells. In addition, bortezomib downregulated CIP2A mRNA but did not affect the degradation of CIP2A protein. Furthermore, bortezomib exerted in vivo antitumor activity in HCC-1937 xenografted tumors, but not in MCF-7 tumors. Bortezomib downregulated CIP2A expression in the HCC-1937 tumors but not in the MCF-7 tumors. Importantly, CIP2A expression is readily detectable in tumor samples from TNBC patients.
CIP2A is a major determinant mediating bortezomib-induced apoptosis in TNBC cells. CIP2A may thus be a potential therapeutic target in TNBC.

0 0
 · 
0 Bookmarks
 · 
65 Views
Data provided are for informational purposes only. Although carefully collected, accuracy cannot be guaranteed. The impact factor represents a rough estimation of the journal's impact factor and does not reflect the actual current impact factor. Publisher conditions are provided by RoMEO. Differing provisions from the publisher's actual policy or licence agreement may be applicable.

Keywords

Bortezomib downregulated CIP2A expression
 
bortezomib downregulated CIP2A mRNA
 
Bortezomib induced significant apoptosis
 
bortezomib inhibited CIP2A
 
bortezomib-induced apoptosis
 
breast cancer xenografts
 
CIP2A upregulated p-Akt
 
estrogen receptor positive MCF-7
 
HCC-1937 xenografted tumors
 
hormone receptors
 
human epidermal growth factor receptor type 2
 
Immunohistochemical study
 
major determinant mediating bortezomib-induced apoptosis
 
multiple cellular effects
 
p-Akt downregulation
 
potential therapeutic target
 
protein phosphatase 2A
 
specific therapeutic targets
 
TNBC patients
 
vivo antitumor activity