Second generation 2-pyridyl biphenyl amide inhibitors of the hedgehog pathway

Georgette Castanedo,Shumei Wang,Kirk Robarge,Elizabeth Blackwood,Daniel J. Burdick,Christine Chang,Gerrit J. P. Dijkgraaf,Stephen E. Gould,Janet L. Gunzner,Oivin Guichert,Jason Halladay,Cyrus Khojasteh,Leslie Lee,James C. Marsters,Lesley J. Murray,David A. Peterson,Emile Plise,Laurent Salphati,Frederic J. de Sauvage,Susan Wong,Daniel P. Sutherlin

Second generation 2-pyridyl biphenyl amide inhibitors of the hedgehog pathway

2010

Abstract Potent and efficacious inhibitors of the hedgehog pathway for the treatment of cancer have been prepared using the 2-pyridyl biphenyl amide scaffold common to the clinical lead GDC-0449. Analogs with polar groups in the para -position of the aryl amide ring optimized potency, had minimal CYP inhibition, and possessed good exposure in rats. Compounds 9d and 14f potently inhibited hedgehog signaling as measured by Gli1 mRNA and were found to be equivalent or more potent than GDC-0449, respectively, when studied in a Ptch +/− medulloblastoma allograft model, that is, highly dependent on hedgehog signaling.

Keywords:

Amide ring
Hedgehog signaling pathway
Aryl
GLI1
Stereochemistry
Medulloblastoma
Amide
Biochemistry
Structure–activity relationship
Organic chemistry
Messenger RNA
Chemistry

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