Stephen R. Hammes, M.D., Ph.D.

Dr. Hammes received his B.A. in chemistry from Cornell University in 1985, where he worked with Dr. Barbara Baird studying the IgE receptor. Dr. Hammes then entered the MD/PhD program at Duke. For his PhD, Dr. Hammes studied retroviral gene regulation with Dr. Warner Greene. He then traveled to San Francisco, where he completed an internship and residency in General Medicine, followed by a fellowship in Endocrinology. For his postdoctoral research, Dr. Hammes again chose an alternative direction, working with a cardiologist rather than an endocrinologist. He trained with Dr. Shaun Coughlin, where he studied G protein-coupled receptors.

In 1999, Dr. Hammes left UCSF to become faculty at the UT Southwestern Medical Center in Dallas, where he started an entirely new research program, choosing to study transcription-independent, or nongenomic, steroid signaling. Specifically, Dr. Hammes studied steroid-triggered maturation (meiotic progression) of oocytes, one of the few physiologically relevant steroid-triggered processes that is generally accepted to be nongenomic. Dr. Hammes has recently expanded his work to study ovarian development and function, with a focus on diseases of androgen excess such as polycystic ovarian syndrome. He also studies hormone-sensitive cancers such as prostate cancer and the rare disease lymphangioleiomyomatosis.

Finally, in 2009 Dr. Hammes moved back to Upstate New York, where he is the Louis S. Wolk Professor of Biomedical Research and the Chief of the Division of Endocrinology at the University of Rochester Medical Center.

Research

The Hammes laboratory studies steroid signaling and steroid production, with a focus on how steroids regulate fertility as well as how steroid promote hormone-sensitive cancer such as breast and prostate cancer.

With regard to steroid signaling, the Hammes laboratory pioneered research related to rapid, extranuclear, or "nongenomic," steroid effects, demonstrating that these rapid responses that initiate at or near the membrane of cells are critical for the subsequent steroid-mediated nuclear effects on transcription. The Hammes laboratory demonstrated that extranuclear androgen signaling via classical androgen receptors located outside of the nucleus initiate rapid activation of G protein and kinase signals that modulate normal fertility in males and females, as well as prostate cancer progression in response to androgens.

The Hammes laboratory was also one of the first to use genetic mouse models to demonstrate that androgen signaling in granulosa cells of the ovary (both nuclear and extranuclear effects) is critical for normal follicle development and subsequent ovulation. Too much androgen signaling, as seen in the disease polycystic ovary syndrome, leads to excessive and unregulated follicle growth.

The Hammes laboratory has also been studying androgen effects on prostate cancer, demonstrating that these same signaling extranuclear and nuclear pathways work together to regulate prostate cancer growth. The laboratory has also recently taken an interest in inflammation and its effects on prostate cancer progression.

Finally, the Hammes laboratory studies a rare lung disease found almost exclusively in women called lymphangioleiomyomatosis, or LAM. The laboratory has developed a mouse model for this disease, and is currently examining the roles of estrogen as well as inflammation in progression of this devastating disorder.

Credentials

Faculty Appointments

Associate Chair/Academic Affairs - Department of Medicine, Endocrine/Metabolism (SMD)
Chief - Department of Medicine, Endocrine/Metabolism (SMD)
Louis S. Wolk Distinguished Professorship in Medicine - Department of Medicine, Endocrine/Metabolism (SMD)
Professor - Department of Medicine, Endocrine/Metabolism (SMD) - Primary
Professor - Department of Pharmacology and Physiology (SMD)

Specialties

Endocrinology, Diabetes and Metabolism - American Board of Internal Medicine
Internal Medicine

Education

1985
BA | Cornell University
Chemistry

1992
MD | Duke University Sch Medicine
Medicine

1992
PhD | Duke University
Microbiology

Post-doctoral Training & Residency

01/01/1993 - 06/30/1993
Research in at Duke University Medical Center

07/01/1993 - 06/30/1994
Internship in Internal Medicine at University of California, San Francisco Medical Center

07/01/1994 - 06/30/1995
Residency in Internal Medicine at University of California, San Francisco Medical Center

07/01/1995 - 06/30/1999
Fellowship in Internal Medicine: Endocrinology, Diabetes, and Metabolism at University of California, San Francisco Medical Center

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Publications

Journal Articles

6/28/2017
Ma X, Hayes E, Biswas A, Seger C, Prizant H, Hammes SR, Sen A. "Androgens Regulate Ovarian Gene Expression Through Modulation of Ezh2 Expression and Activity." Endocrinology.. 2017 Jun 28; Epub 2017 Jun 28.

6/15/2017
Miedlich SU, Taya M, Young MR, Hammes SR. "Paxillin and embryonic PolyAdenylation Binding Protein (ePABP) engage to regulate androgen-dependent Xenopus laevis oocyte maturation - A model of kinase-dependent regulation of protein expression." Molecular and cellular endocrinology.. 2017 Jun 15; 448:87-97. Epub 2017 Mar 28.

6/2017
Lu C, Lee HS, Pappas GP, Dilling DF, Burger CD, Shifren A, Veeraraghavan S, Chapman JT, Parambil J, Ruoss SJ, Young LR, Hammes SR, Kopras EJ, Roads T, Krischer JP, McCormack FX, . "A Phase II Clinical Trial of an Aromatase Inhibitor for Postmenopausal Women with Lymphangioleiomyomatosis." Annals of the American Thoracic Society.. 2017 Jun 0; 14(6):919-928.

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Videos

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