β2-adrenoceptor signaling regulates invadopodia formation to enhance tumor cell invasion

Breast Cancer Research - Tập 17 - Trang 1-12 - 2015
Sarah J. Creed1, Caroline P. Le1, Mona Hassan1, Cindy K. Pon1, Sabine Albold1, Keefe T. Chan2,3, Matthew E. Berginski4, Zhendong Huang5, James E. Bear2, J. Robert Lane1, Michelle L. Halls1, Davide Ferrari5, Cameron J. Nowell1, Erica K. Sloan1,6,7
1Drug Discovery Biology Theme, Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, Australia
2Department of Cell & Developmental Biology and Lineberger Comprehensive Cancer Center, School of Medicine, The University of North Carolina Chapel Hill, Chapel Hill, USA
3Current address: Peter MacCallum Cancer Centre, East Melbourne, Australia
4Department of Biomedical Engineering, Duke University, Durham, USA
5Department of Mathematics and Statistics, The University of Melbourne, Parkville, Australia
6Cousins Center for PNI, UCLA Semel Institute, and Jonsson Comprehensive Cancer Center, University of California Los Angeles, Los Angeles, USA
7Division of Cancer Surgery, Peter MacCallum Cancer Centre, East Melbourne, Australia

Tóm tắt

For efficient metastatic dissemination, tumor cells form invadopodia to degrade and move through three-dimensional extracellular matrix. However, little is known about the conditions that favor invadopodia formation. Here, we investigated the effect of β-adrenoceptor signaling - which allows cells to respond to stress neurotransmitters - on the formation of invadopodia and examined the effect on tumor cell invasion. To characterize the molecular and cellular mechanisms of β-adrenergic signaling on the invasive properties of breast cancer cells, we used functional cellular assays to quantify invadopodia formation and to evaluate cell invasion in two-dimensional and three-dimensional environments. The functional significance of β-adrenergic regulation of invadopodia was investigated in an orthotopic mouse model of spontaneous breast cancer metastasis. β-adrenoceptor activation increased the frequency of invadopodia-positive tumor cells and the number of invadopodia per cell. The effects were selectively mediated by the β2-adrenoceptor subtype, which signaled through the canonical Src pathway to regulate invadopodia formation. Increased invadopodia occurred at the expense of focal adhesion formation, resulting in a switch to increased tumor cell invasion through three-dimensional extracellular matrix. β2-adrenoceptor signaling increased invasion of tumor cells from explanted primary tumors through surrounding extracellular matrix, suggesting a possible mechanism for the observed increased spontaneous tumor cell dissemination in vivo. Selective antagonism of β2-adrenoceptors blocked invadopodia formation, suggesting a pharmacological strategy to prevent tumor cell dissemination. These findings provide insight into conditions that control tumor cell invasion by identifying signaling through β2-adrenoceptors as a regulator of invadopodia formation. These findings suggest novel pharmacological strategies for intervention, by using β-blockers to target β2-adrenoceptors to limit tumor cell dissemination and metastasis.

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Breast Cancer Research

Tập 17

1-12

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