Breast cancer-specific gene 1 interacts with the mitotic checkpoint kinase BubR1

23 October 2003

journal article
Published by Springer Nature in Oncogene

Vol. 22 (48) , 7593-7599
https://doi.org/10.1038/sj.onc.1206880

Abstract

The abnormal expression of breast cancer-specific gene 1 (BCSG1) in malignant mammary epithelial cells is highly associated with the development and progression of breast cancer. A series of in vitro and in vivo studies performed in our laboratory and others have demonstrated that BCSG1 expression significantly stimulates proliferation, invasion, and metastasis of breast cancer cells. However, currently little is known about how BCSG1 exerts its oncogenic functions. To elucidate the cellular mechanisms underlying the effects of BCSG1 in breast cancer cells, we used a yeast two-hybrid system to screen for proteins that could associate with BCSG1. Through this screening, we identified the mitotic checkpoint protein BubR1 as a novel binding partner of BCSG1. The specific association of BCSG1 with BubR1 in breast cancer cells was demonstrated by immunoprecipitation and GST pull-down assays. Intriguingly, experiments conducted in four different cell lines all showed that exogenous expressions of BCSG1 consistently reduce the cellular levels of the BubR1 protein without affecting BubR1 mRNA expression. The tendency of endogenous BCSG1 expression coinciding with lower BubR1 protein levels was also observed in seven out of eight breast cancer cell lines. We further showed that the reducing effect of BCSG1 on BubR1 protein expression could be prevented by treating BCSG1-transfected cells with MG-132, a selective 26S proteasome inhibitor, implying that the proteasome machinery may be involved in the BCSG1-induced reduction of the BubR1 protein. Accompanied with a reduction of BubR1 protein level, BCSG1 expression resulted in multinucleation of breast cancer cells upon treatment with spindle inhibitor nocodazole, indicating an impaired mitotic checkpoint. Taken together, our novel findings suggest that BCSG1 may accelerate the progression of breast cancer at least in part by compromising the mitotic checkpoint control through inactivation of BubR1.

Keywords

This publication has 28 references indexed in Scilit:

Mad2 and BubR1 Function in a Single Checkpoint Pathway that Responds to a Loss of Tension
Molecular Biology of the Cell, 2002
γ-Synuclein Promotes Cancer Cell Survival and Inhibits Stress- and Chemotherapy Drug-induced Apoptosis by Modulating MAPK Pathways
Journal of Biological Chemistry, 2002
BubR1 is essential for kinetochore localization of other spindle checkpoint proteins and its phosphorylation requires Mad1
The Journal of cell biology, 2002
Checkpoint Protein BubR1 Acts Synergistically with Mad2 to Inhibit Anaphase-promoting Complex
Molecular Biology of the Cell, 2002
A new view of the spindle checkpoint
The Journal of cell biology, 2001
Checkpoint inhibition of the APC/C in HeLa cells is mediated by a complex of BUBR1, BUB3, CDC20, and MAD2
The Journal of cell biology, 2001
Molecular mechanisms for aberrant expression of the human breast cancer specific gene 1 in breast cancer cells: control of transcription by DNA methylation and intronic sequences
Oncogene, 2001
Gamma synuclein: Subcellular localization in neuronal and non‐neuronal cells and effect on signal transduction
Cell Motility, 2001
The Anaphase-Promoting Complex: New Subunits and Regulators
Annual Review of Biochemistry, 1999
The Mouse Mitotic Checkpoint Gene Bub1b, a Novel Bub1 Family Member, Is Expressed in a Cell Cycle-Dependent Manner
Genomics, 1999