Abstract

Centrosome amplification, the acquisition of three or more centrosomes, results in defective spindles, multipolar mitosis and aneuploidy. Aneuploidy generates a plethora of genetic alterations that culminates in cancer initiation and promotion. Centrosome amplification is present in most human tumors, including 80-90% human breast cancers and precursor mammary lesions. How that centrosome amplification arises is based on correlative evidence;for example, human breast cancers over-expressing Her2 (30% of all human cancers) have high frequencies of centrosome amplification. In addition, many altered gene products involved in human cancers result in centrosome amplification and chromosome instability in cell culture. Our published results showed that Ras induced centrosome amplification through the MAPK pathway in cultured cells. Our preliminary data showed that Ras, but not c-Myc induces centrosome amplification in precursor mammary lesions. Expression assays showed that human and mouse mammary epithelial cells expressing Her2, or Ras display ectopically expressed cyclin D1 and Nek2. Down-regulation of cyclinD1, Cdk4 and Nek-2 prevent Her2 and Ras- dependent centrosome amplification. We propose the following hypothesis: The Her2/Ras pathway trigger centrosome amplification and mammary tumor initiation by through a classical pathway involving Cdk4 phosphorylation of NPM, and through an alternative pathway involving ectopically-expressed Nek2.
In specific aim 1 we will distinguish between a classical and an alternative pathway to centrosome amplification.
In specific aim 2 we will assess how the alternative pathway impinges on centrosome amplification.
Specific aim 3 will address how interfering with the classical pathway in vivo prevents centrosome amplification in pre-malignancy and suppresses mammary tumorigenesis.

Public Health Relevance

Because most human cancers harbor centrosome amplification, identifying oncogene-deregulated centrosomal targets mediating centrosome amplification will provide the groundwork to patient treatment with existing or developing inhibitors specific to those mediators, including Cdk4, NPM and Nek2. Those inhibitors will prevent the centrosome amplification and aneuploidy responsible for tumor initiation and progression to malignancy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA151521-03
Application #
8245131
Study Section
Molecular Oncogenesis Study Section (MONC)
Program Officer
Hildesheim, Jeffrey
Project Start
2010-07-01
Project End
2015-04-30
Budget Start
2012-05-01
Budget End
2013-04-30
Support Year
3
Fiscal Year
2012
Total Cost
$310,316
Indirect Cost
$109,041

  Institution

Name
Emory University
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
066469933
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

King, Jamie L; Zhang, Baotong; Li, Yixiang et al. (2018) TTK promotes mesenchymal signaling via multiple mechanisms in triple negative breast cancer. Oncogenesis 7:69
Lee, Miyoung; Oprea-Ilies, Gabriela; Saavedra, Harold I (2015) Silencing of E2F3 suppresses tumor growth of Her2+ breast cancer cells by restricting mitosis. Oncotarget 6:37316-34
Lee, Mi-Young; Moreno, Carlos S; Saavedra, Harold I (2014) E2F activators signal and maintain centrosome amplification in breast cancer cells. Mol Cell Biol 34:2581-99
Brown, David I; Lassègue, Bernard; Lee, Minyoung et al. (2014) Poldip2 knockout results in perinatal lethality, reduced cellular growth and increased autophagy of mouse embryonic fibroblasts. PLoS One 9:e96657
Lee, Mi-Young; Marina, Mihaela; King, Jamie L et al. (2014) Differential expression of centrosome regulators in Her2+ breast cancer cells versus non-tumorigenic MCF10A cells. Cell Div 9:3
Marina, Mihaela; Saavedra, Harold I (2014) Nek2 and Plk4: prognostic markers, drivers of breast tumorigenesis and drug resistance. Front Biosci (Landmark Ed) 19:352-65
Hagen, Katie R; Zeng, Xiangbin; Lee, Mi-Young et al. (2013) Silencing CDK4 radiosensitizes breast cancer cells by promoting apoptosis. Cell Div 8:10
Harrison Pitner, Mary Kathryn; Saavedra, Harold I (2013) Cdk4 and nek2 signal binucleation and centrosome amplification in a her2+ breast cancer model. PLoS One 8:e65971
Harrison, Mary K; Adon, Arsene M; Saavedra, Harold I (2011) The G1 phase Cdks regulate the centrosome cycle and mediate oncogene-dependent centrosome amplification. Cell Div 6:2
Adon, Arsene M; Zeng, Xiangbin; Harrison, Mary K et al. (2010) Cdk2 and Cdk4 regulate the centrosome cycle and are critical mediators of centrosome amplification in p53-null cells. Mol Cell Biol 30:694-710

Showing the most recent 10 out of 11 publications