HER/ErbB Receptor Interactions and Signaling Patterns in Human Mammary Epithelial Cells

Zhang, Yi; Opresko, Lee K; Shankaran, Harish; Chrisler, William B; Wiley, H S; Resat, Haluk

doi:10.1186/1471-2121-10-78

Title: HER/ErbB Receptor Interactions and Signaling Patterns in Human Mammary Epithelial Cells

Journal Article · Sat Oct 31 00:00:00 EDT 2009 · BMC Cell Biology, 10 :Article No. 78

DOI:https://doi.org/10.1186/1471-2121-10-78· OSTI ID:970366

Zhang, Yi; Opresko, Lee K; Shankaran, Harish; Chrisler, William B; Wiley, H S; Resat, Haluk

Knowledge about signaling pathways is typically compiled based on data gathered using different cell lines. This approach implicitly assumes that cell line dependence is not important, which can be misleading because different cell lines do not always respond to a particular stimulus in the same way. The lack of coherent data collected from closely related cellular systems can be detrimental to the efforts to understand the regulation of biological processes. In this study, we report the development of a library of human mammary epithelial (HME) cell lines which express endogenous levels of the cell surface receptor EGFR/HER1, and different levels of HER2 and HER3. Using our clone library, we have quantified the interactions among the HER1-3 receptors and systematically investigated the existing hypotheses about their interaction patterns. Contrary to earlier suggestions, we find that lateral interactions with HER2 do not lead to strong transactivation between EGFR and HER3. Our study identified HER2 as the dominant dimerization partner for both EGFR and HER3, and revealed that EGFR and HER3 activations are only weakly linked in HME cells. We have also quantified the time-dependent activation patterns of the downstream effectors Erk and Akt. We found that HER3 signaling makes the strongest contribution to Akt activation and that, stimulation of either EGFR or HER3 pathways activate Erk at significant levels. Our study shows that cell libraries formed from closely related clones can be a powerful resource for pursuing the quantitative investigations that are necessary for developing a systems level understanding of cell signaling.

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Research Organization:: Pacific Northwest National Lab. (PNNL), Richland, WA (United States)

Sponsoring Organization:: USDOE

DOE Contract Number:: AC05-76RL01830

OSTI ID:: 970366

Report Number(s):: PNNL-SA-64538; 400412000; TRN: US201003%%529

Journal Information:: BMC Cell Biology, 10 :Article No. 78, Vol. 10

Country of Publication:: United States

Language:: English

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59 BASIC BIOLOGICAL SCIENCES
DIMERIZATION
REGULATIONS
STIMULATION

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