Abstract
ERBB receptor tyrosine kinases are activated by ligand-induced dimerization followed by activation and transphosphorylation of their intracellular kinase domains. A recent study by Bill and colleagues demonstrates that receptor transphosphorylation can be regulated from inside the cell by members of the cytohesin protein family. These data highlight a novel mechanism of amplification of ERBB receptor signaling output that may contribute to embryogenesis and cancer progression.
Cite
CITATION STYLE
Arteaga, C. L. (2011). ERBB receptors in cancer: signaling from the inside. Breast Cancer Research : BCR, 13(2), 304. https://doi.org/10.1186/bcr2829
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