Design and Optimization of Potent and Orally Bioavailable Tetrahydronaphthalene Raf Inhibitors

Alexandra E. Gould,Ruth Adams,Sharmila Adhikari,Kathleen Aertgeerts,Roushan Afroze,Christopher Blackburn,Emily F. Calderwood,Ryan Chau,Jouhara Chouitar,Matthew O. Duffey,Dylan England,Cheryl A. Farrer,Nancy Forsyth,Khristofer Garcia,Jeffery Gaulin,Paul D. Greenspan,Ribo Guo,Sean Harrison,Shih-Chung Huang,Natalia Iartchouk,Dave Janowick,Mi-Sook Kim,Bheemashankar Kulkarni,Steven P. Langston,Jane X. Liu,Li-Ting Ma,Saurabh Menon,Hirotake Mizutani,Erin Paske,Christelle C. Renou,Mansoureh Rezaei,R. Scott Rowland,Michael D. Sintchak,Michael D. Smith,Stephen G. Stroud,Ming Tregay,Yuan Tian,Ole P. Veiby,Tricia J. Vos,Stepan Vyskocil,Juliet Williams,Tianlin Xu,Johnny Yang,Jason Yano,Hongbo Zeng,Dong Mei Zhang,Qin Zhang,Katherine M. Galvin

Design and Optimization of Potent and Orally Bioavailable Tetrahydronaphthalene Raf Inhibitors

2011

Inhibition of mutant B-Raf signaling, through either direct inhibition of the enzyme or inhibition of MEK, the direct substrate of Raf, has been demonstrated preclinically to inhibit tumor growth. Very recently, treatment of B-Raf mutant melanoma patients with a selective B-Raf inhibitor has resulted in promising preliminary evidence of antitumor activity. This article describes the design and optimization of tetrahydronaphthalene-derived compounds as potent inhibitors of the Raf pathway in vitro and in vivo. These compounds possess good pharmacokinetic properties in rodents and inhibit B-Raf mutant tumor growth in mouse xenograft models.

Keywords:

Substrate (chemistry)
Enzyme
Melanoma
In vivo
Mutant
Biochemistry
Bioavailability
Biology
Pharmacokinetics
In vitro
Pharmacology
antitumor activity
Chemistry

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