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Publication
Featured researches published by Verlyn G. Schaefer.
Molecular and Cellular Endocrinology | 2002
Wiweka Kaszubska; H. Douglas Falls; Verlyn G. Schaefer; Deanna Haasch; Leigh Frost; Paul Hessler; Paul E. Kroeger; David White; Michael R. Jirousek; James M. Trevillyan
Protein tyrosine phosphatase 1B (PTP1B) has recently been implicated in the regulation of body weight. A surprising phenotype of PTP1B-deficient mice is their resistance to diet-induced obesity. Since leptin is one of the primary hormones involved in the regulation of body weight and energy homeostasis, we investigated whether PTP1B affects leptin receptor (lepR) signaling directly. A mouse hypothalamic cell line, GT1-7, was established as a suitable cell model for the study of leptin signaling. Stimulation of GT1-7 cells by leptin caused tyrosine phosphorylation of endogenous STAT3 and activation of a STAT-dependent luciferase reporter gene. Over-expression of PTP1B in GT1-7 cells resulted in a dose-dependent decrease in endogenous JAK2 and STAT3 tyrosine phosphorylation compared with cells transfected with lepR alone. Consistent with inhibition of JAK-STAT signaling, PTP1B over-expression caused a dose-dependent decrease in leptin-induced, STAT-dependent luciferase reporter gene activation in GT1-7 cells. Furthermore, over-expression of PTP1B led to a decrease in mRNA accumulation of suppressor-of-cytokine-signalling-3 (SOCS3) and c-fos, genes that are acutely induced by leptin. Using gene microarray analysis, we confirmed that PTP1B reduces the level of gene expression of SOCS3 and showed that the expression level of other leptin-regulated genes was affected. Genes up-regulated by leptin were decreased in cells over-expressing PTP1B. Conversely, the expression of genes down-regulated by leptin was enhanced by PTP1B over-expression in GT1-7 cells. Our findings indicate that PTP1B is a negative regulator of leptin signaling and suggest that PTP1B inhibitors might be efficacious in the treatment of obesity by increasing leptin sensitivity.
Journal of Medicinal Chemistry | 2001
Gui-Dong Zhu; David L. Arendsen; Indrani W. Gunawardana; Steven A. Boyd; Andrew O. Stewart; Dennis G. Fry; Barbara L. Cool; Lemma Kifle; Verlyn G. Schaefer; Joseph L. Meuth; Kennan C. Marsh; Anita J. Kempf-Grote; Patrick D. Kilgannon; W. Michael Gallatin; Gregory F. Okasinski
Journal of Organic Chemistry | 2002
Gui-Dong Zhu; Verlyn G. Schaefer; Steven A. Boyd; Gregory F. Okasinski
Archive | 1994
Gregory F. Okasinski; Peter J. DeVries; Barry S. Mellovitz; Joseph L. Meuth; Verlyn G. Schaefer
Journal of Medicinal Chemistry | 2006
Michael D. Serby; Hongyu Zhao; Bruce G. Szczepankiewicz; Christi Kosogof; Zhili Xin; Bo Liu; Mei Liu; Lissa T. Nelson; Wiweka Kaszubska; H. Douglas Falls; Verlyn G. Schaefer; Eugene N. Bush; Robin Shapiro; Brian A. Droz; Victoria Knourek-Segel; Thomas A. Fey; Michael E. Brune; David W. A. Beno; Theresa M. Turner; Christine A. Collins; Peer B. Jacobson; Hing L. Sham; Gang Liu
Bioorganic & Medicinal Chemistry Letters | 2004
Bo Liu; Gang Liu; Zhili Xin; Michael D. Serby; Hongyu Zhao; Verlyn G. Schaefer; H. Douglas Falls; Wiweka Kaszubska; Christine A. Collins; Hing L. Sham
Journal of Medicinal Chemistry | 2004
Hongyu Zhao; Zhili Xin; Gang Liu; Verlyn G. Schaefer; H. Douglas Falls; Wiweka Kaszubska; Christine Collins; Hing L. Sham
Journal of Molecular Endocrinology | 2006
H. Douglas Falls; Brian D. Dayton; Dennis G. Fry; Christopher A. Ogiela; Verlyn G. Schaefer; Sevan Brodjian; Regina M. Reilly; Christine A. Collins; Wiweka Kaszubska
Bioorganic & Medicinal Chemistry Letters | 2005
Zhili Xin; Hongyu Zhao; Michael D. Serby; Bo Liu; Verlyn G. Schaefer; Douglas H. Falls; Wiweka Kaszubska; Christine A. Colins; Hing L. Sham; Gang Liu
Protein Expression and Purification | 2000
Wiweka Kaszubska; Haiying Zhang; Robert L. Patterson; Thomas S. Suhar; Marie E. Uchic; Robert W. Dickinson; Verlyn G. Schaefer; Deanna Haasch; Richard S. Janis; Peter J. DeVries; Gregory F. Okasinski; Joseph L. Meuth