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Dive into the research topics where Karen Kotkow is active.

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Featured researches published by Karen Kotkow.


Nature | 2008

A paracrine requirement for hedgehog signalling in cancer

Robert L. Yauch; Stephen E. Gould; Suzie J. Scales; Tracy Tang; Hua Tian; Christina P. Ahn; Derek Marshall; Ling Fu; Thomas Januario; Dara Y. Kallop; Michelle Nannini-Pepe; Karen Kotkow; James C. Marsters; Lee L. Rubin; Frederic J. de Sauvage

Ligand-dependent activation of the hedgehog (Hh) signalling pathway has been associated with tumorigenesis in a number of human tissues. Here we show that, although previous reports have described a cell-autonomous role for Hh signalling in these tumours, Hh ligands fail to activate signalling in tumour epithelial cells. In contrast, our data support ligand-dependent activation of the Hh pathway in the stromal microenvironment. Specific inhibition of Hh signalling using small molecule inhibitors, a neutralizing anti-Hh antibody or genetic deletion of smoothened (Smo) in the mouse stroma results in growth inhibition in xenograft tumour models. Taken together, these studies demonstrate a paracrine requirement for Hh ligand signalling in the tumorigenesis of Hh-expressing cancers and have important implications for the development of Hh pathway antagonists in cancer.


Bioorganic & Medicinal Chemistry Letters | 2009

GDC―0449―A potent inhibitor of the hedgehog pathway

Kirk Robarge; Shirley A. Brunton; Georgette Castanedo; Yong Cui; Michael S. Dina; Richard Goldsmith; Stephen E. Gould; Oivin Guichert; Janet Gunzner; Jason S. Halladay; Wei Jia; Cyrus Khojasteh; Michael F. T. Koehler; Karen Kotkow; Hank La; Rebecca L. LaLonde; Kevin Lau; Leslie Lee; Derek Marshall; James C. Marsters; Lesley J. Murray; Changgeng Qian; Lee L. Rubin; Laurent Salphati; Mark S. Stanley; John H.A. Stibbard; Daniel P. Sutherlin; Savita Ubhayaker; Shumei Wang; Susan Wong

SAR for a wide variety of heterocyclic replacements for a benzimidazole led to the discovery of functionalized 2-pyridyl amides as novel inhibitors of the hedgehog pathway. The 2-pyridyl amides were optimized for potency, PK, and drug-like properties by modifications to the amide portion of the molecule resulting in 31 (GDC-0449). Amide 31 produced complete tumor regression at doses as low as 12.5mg/kg BID in a medulloblastoma allograft mouse model that is wholly dependent on the Hh pathway for growth and is currently in human clinical trials, where it is initially being evaluated for the treatment of BCC.


Clinical Cancer Research | 2011

Targeting Superficial or Nodular Basal Cell Carcinoma with Topically Formulated Small Molecule Inhibitor of Smoothened

Tracy Tang; Jean Y. Tang; Dongwei Li; Mike Reich Reich; Christopher A. Callahan; Ling Fu; Robert L. Yauch; Frank Wang; Karen Kotkow; Kris S. Chang; Elana Shpall; Angela Ruoha Wu; Lee L. Rubin; James C. Marsters; Ervin H. Epstein; Ivor Caro; Frederic J. de Sauvage

Purpose: Inappropriate activation of the Hedgehog (Hh) signaling pathway in skin is critical for the development of basal cell carcinomas (BCC). We have investigated the anti-BCC efficacy of topically-applied CUR61414, an inhibitor of the Hh signal transduction molecule Smoothened. Experimental Design: In preclinical studies, we used a depilatory model to evaluate the ability of topical formulations of CUR61414 to repress Hh responsive cells found at the base of hair follicles in normal skin. We also tested the in vivo effects of topical CUR61414 on murine BCCs developed in Ptch1 +/− K14-CreER2 p53 fl/fl mice. In a phase I clinical study, we evaluated the safety, tolerability, and efficacy of a multidose regimen of CUR61414 (0.09%, 0.35%, 1.1%, and 3.1%) applied topically to human superficial or nodular BCCs for up to 28 days. Results: In mice, topical CUR61414 significantly inhibited skin Hh signaling, blocked the induction of hair follicle anagen, and shrank existing BCCs. However, we observed no clinical activity of this formulation in human superficial or nodular BCCs in a phase I clinical study. Conclusions: Our data highlight some of the challenges of translating preclinical experience into successful human results for a topical anticancer agent. Clin Cancer Res; 17(10); 3378–87. ©2011 AACR.


Human Reproduction | 2004

Temporal gene expression during differentiation of human embryonic stem cells and embryoid bodies

Tamar Dvash; Yoav Mayshar; Henia Darr; Michael McElhaney; Douglas Barker; Ofra Yanuka; Karen Kotkow; Lee L. Rubin; Nissim Benvenisty; Rachel Eiges


Archive | 2001

Hedgehog antagonists, methods and uses related thereto

Henryk Dudek; Irina Karavanov; Carmen Pepicelli; Karen Kotkow; Lee L. Rubin


Archive | 2004

Stem cell-based methods for identifying and characterizing agents

Lee L. Rubin; Karen Kotkow; Cheng-Jung Lai


Cancer Research | 2008

A paracrine requirement for Hedgehog signaling in cancer

Robert L. Yauch; Stephen E. Gould; Derek Marshall; Tracy Tang; Hua Tian; Suzie J. Scales; Ling Fu; Karen Kotkow; Jim Marsters; Lee L. Rubin; Frederic J. de Sauvage


Archive | 2010

Methods of inhibiting unwanted cell proliferation using hedgehog antagonists

Henryk Dudek; Irina Karavanov; Carmen Pepicelli; Karen Kotkow; Lee L. Rubin


Archive | 2010

Methods of treating pancreatic or liver cancer using hedgehog antagonists

Henryk Dudek; Irina Karavanov; Carmen Pepicelli; Karen Kotkow; Lee L. Rubin


Bioorganic & Medicinal Chemistry Letters | 2010

Corrigendum to “GDC-0449—A potent inhibitor of the hedgehog pathway” [Bioorg. Med. Chem. Lett. 19 (2009) 5576]

Kirk Robarge; Shirley A. Brunton; Georgette Castanedo; Yong Cui; Michael S. Dina; Richard Goldsmith; Stephen E. Gould; Oivin Guichert; Janet Gunzner; Jason S. Halladay; Wei Jia; Cyrus Khojasteh; Michael F. T. Koehler; Karen Kotkow; Hank La; Rebecca L. LaLonde; Kevin Lau; Leslie Lee; Derek Marshall; James C. Marsters; Lesley J. Murray; Changgeng Qian; Lee L. Rubin; Laurent Salphati; Mark S. Stanley; John H.A. Stibbard; Daniel P. Sutherlin; Savita Ubhayaker; Shumei Wang; Susan Wong

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