Lead identification of novel and selective TYK2 inhibitors

Authors :: Wade S. Blair
Sue Sohn
Stanley Mark S
Pawan Bir Kohli
Leo Berezhkovskiy
Lawren C. Wu
James P. Driscoll
Charles Eigenbrot
Adam R. Johnson
Vickie Tsui
Birong Zhang
Paul Gibbons
Nico Ghilardi
Yingjie Lai
Jun Liang
Marya Liimatta
Amy Sambrone
Jeremy Murray
Young G. Shin
Jason Halladay
Yisong Xiao
Kathy Barrett
Christine Chang
Maureen Beresini
Steven Shia
Mark Ultsch
Bao Liang
Kapil Menghrajani
Jan Smith
Priscilla Mantik
Anne van Abbema
Steven Magnuson
Source :: European Journal of Medicinal Chemistry. 67:175-187
Publication Year :: 2013
Publisher :: Elsevier BV, 2013.
Abstract: A therapeutic rationale is proposed for the treatment of inflammatory diseases, such as psoriasis and inflammatory bowel diseases (IBD), by selective targeting of TYK2. Hit triage, following a high-throughput screen for TYK2 inhibitors, revealed pyridine 1 as a promising starting point for lead identification. Initial expansion of 3 separate regions of the molecule led to eventual identification of cyclopropyl amide 46, a potent lead analog with good kinase selectivity, physicochemical properties, and pharmacokinetic profile. Analysis of the binding modes of the series in TYK2 and JAK2 crystal structures revealed key interactions leading to good TYK2 potency and design options for future optimization of selectivity.

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