Genome co-amplification upregulates a mitotic gene network activity that predicts outcome and response to mitotic protein inhibitors in breast cancer

Zhi Hu; Jian-Hua Mao; Christina Curtis; Ge Huang; Shenda Gu; Laura Heiser; Marc E Lenburg; James E Korkola; Nora Bayani; Shamith Samarajiwa; Jose A Seoane; Mark A Dane; Amanda Esch; Heidi S Feiler; Nicholas J Wang; Mary Ann Hardwicke; Sylvie Laquerre; Jeff Jackson; Kenneth W Wood; Barbara Weber; Paul T Spellman; Samuel Aparicio; Richard Wooster; Carlos Caldas; Joe W Gray

doi:10.1186/s13058-016-0728-y

Genome co-amplification upregulates a mitotic gene network activity that predicts outcome and response to mitotic protein inhibitors in breast cancer

Breast Cancer Res. 2016 Jul 1;18(1):70. doi: 10.1186/s13058-016-0728-y.

Authors

Zhi Hu¹, Jian-Hua Mao², Christina Curtis³, Ge Huang¹, Shenda Gu¹, Laura Heiser¹, Marc E Lenburg⁴, James E Korkola¹, Nora Bayani², Shamith Samarajiwa⁵, Jose A Seoane³, Mark A Dane¹, Amanda Esch¹, Heidi S Feiler¹, Nicholas J Wang¹, Mary Ann Hardwicke⁶, Sylvie Laquerre⁶, Jeff Jackson⁶, Kenneth W Wood⁷, Barbara Weber⁶, Paul T Spellman¹, Samuel Aparicio⁸, Richard Wooster⁶, Carlos Caldas⁹, Joe W Gray¹⁰

Affiliations

¹ Department of Biomedical Engineering, School of Medicine, Oregon Health & Science University, 3303 SW Bond Ave., CH13B, Portland, OR, 97239, USA.
² Life Sciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA, 94127, USA.
³ Department of Medicine, Division of Oncology and Department of Genetics, Stanford University School of Medicine, Stanford, CA, 94305, USA.
⁴ Department of Pathology and Laboratory Medicine, Boston University School of Medicine, Boston, MA, 02215, USA.
⁵ MRC Cancer Unit, University of Cambridge, Cambridge, CB2 0XZ, UK.
⁶ GlaxoSmithKline, Collegeville, PA, 19425, USA.
⁷ Cytokinetics, Inc., South San Francisco, CA, 94080, USA.
⁸ Molecular Oncology, BC Cancer Research Centre, Vancouver, Canada.
⁹ Cancer Research UK, Cambridge Institute, Cambridge, UK. carlos.caldas@cancer.org.uk.
¹⁰ Department of Biomedical Engineering, School of Medicine, Oregon Health & Science University, 3303 SW Bond Ave., CH13B, Portland, OR, 97239, USA. Grayjo@ohsu.edu.

Abstract

Background: High mitotic activity is associated with the genesis and progression of many cancers. Small molecule inhibitors of mitotic apparatus proteins are now being developed and evaluated clinically as anticancer agents. With clinical trials of several of these experimental compounds underway, it is important to understand the molecular mechanisms that determine high mitotic activity, identify tumor subtypes that carry molecular aberrations that confer high mitotic activity, and to develop molecular markers that distinguish which tumors will be most responsive to mitotic apparatus inhibitors.

Methods: We identified a coordinately regulated mitotic apparatus network by analyzing gene expression profiles for 53 malignant and non-malignant human breast cancer cell lines and two separate primary breast tumor datasets. We defined the mitotic network activity index (MNAI) as the sum of the transcriptional levels of the 54 coordinately regulated mitotic apparatus genes. The effect of those genes on cell growth was evaluated by small interfering RNA (siRNA).

Results: High MNAI was enriched in basal-like breast tumors and was associated with reduced survival duration and preferential sensitivity to inhibitors of the mitotic apparatus proteins, polo-like kinase, centromere associated protein E and aurora kinase designated GSK462364, GSK923295 and GSK1070916, respectively. Co-amplification of regions of chromosomes 8q24, 10p15-p12, 12p13, and 17q24-q25 was associated with the transcriptional upregulation of this network of 54 mitotic apparatus genes, and we identify transcription factors that localize to these regions and putatively regulate mitotic activity. Knockdown of the mitotic network by siRNA identified 22 genes that might be considered as additional therapeutic targets for this clinically relevant patient subgroup.

Conclusions: We define a molecular signature which may guide therapeutic approaches for tumors with high mitotic network activity.

Keywords: Breast cancer; Mitotic index; Novel therapeutics; Predictive biomarker.

MeSH terms

Aurora Kinases / antagonists & inhibitors
Aurora Kinases / genetics
Aurora Kinases / metabolism
Breast Neoplasms / drug therapy
Breast Neoplasms / genetics*
Breast Neoplasms / metabolism
Cell Cycle Proteins / antagonists & inhibitors
Cell Cycle Proteins / genetics
Cell Cycle Proteins / metabolism
Cell Line, Tumor
Cell Proliferation / drug effects
Cell Proliferation / genetics
Chromosomal Proteins, Non-Histone / antagonists & inhibitors
Chromosomal Proteins, Non-Histone / genetics
Chromosomal Proteins, Non-Histone / metabolism
Female
Gene Amplification
Gene Expression Profiling / methods
Gene Expression Regulation, Neoplastic*
Gene Regulatory Networks / drug effects
Gene Regulatory Networks / genetics*
Genome, Human / genetics*
Humans
Kaplan-Meier Estimate
Mitosis / drug effects*
Mitosis / genetics
Polo-Like Kinase 1
Prognosis
Protein Serine-Threonine Kinases / antagonists & inhibitors
Protein Serine-Threonine Kinases / genetics
Protein Serine-Threonine Kinases / metabolism
Proto-Oncogene Proteins / antagonists & inhibitors
Proto-Oncogene Proteins / genetics
Proto-Oncogene Proteins / metabolism
RNA Interference
Small Molecule Libraries / pharmacology
Treatment Outcome

Substances

Cell Cycle Proteins
Chromosomal Proteins, Non-Histone
Proto-Oncogene Proteins
Small Molecule Libraries
centromere protein E
Aurora Kinases
Protein Serine-Threonine Kinases

Abstract

MeSH terms

Substances

Grants and funding