David Stern, Ph.D.

David Stern, Ph.D.
Professor of Pathology
Director, Graduate Studies, Department of Pathology, Yale University
Co-Program Director of the Breast Cancer Research Program at the Yale Comprehensive Cancer Center

B.S. Massachusetts Institute of Technology, 1976
Ph.D. University of California, San Diego, CA, Salk Institute 1983
Postdoctoral, Whitehead Institute for Biomedical Research, Massachusetts Institute of Technology

Research Interests

Human carcinogenesis is driven by gene alterations that deregulate cell proliferation, and others that disrupt checkpoint controls. Much of the work my laboratory is devoted to a major human oncogene, the neu/ErbB2/HER-2 receptor tyrosine kinase, which is now a validated therapeutic target in breast cancer. We also study DNA damage checkpoint pathways which are important in cancer causation, since their failure triggers genomic instability. These same pathways determine responses to genotoxic cancer therapeutics. For more information and publications see http://myprofile.cos.com/sternd61.

Representative Publications

Jackson-Fisher, A.J., Bellinger, G., Ramabhadran, R., Morris, J.K., Lee, K.-F., and D.F. Stern. 2004. ErbB2 is Required for Ductal Morphogenesis of the Mammary Gland. Proc.Natl.Acad.Sci USA 101:17138-43 .

Xu, X., Lee, J., and D.F. Stern. 2004. Microcephalin is required for the DNA damage-induced intra-S and G2/M checkpoints. J. Biol.Chem. 279:34091-34094.

*DiGiovanna, M.P. * Stern, D.F., Edgerton , S., Whalen , S.G., Moore II , D., and A.D. Thor. 2005. ErbB-2 Activation, Epidermal Growth Factor Receptor Expression and Prognosis in Breast Cancer Patients. Journal of Clinical Oncology 23:1152-60.

*authors contributed equally to this work

Li, Jia., and D.F. Stern. 2005. Regulation of Chk2 by DNA-dependent protein kinase. J. Biol. Chem. 280:12041-50.


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