Discovery of AZD-2098 and AZD-1678, Two Potent and Bioavailable CCR4 Receptor Antagonists

Nicholas Kindon,Glen Andrews,Andrew Douglas Baxter,David Cheshire,Paul Hemsley,Timothy Johnson,Yu-Zhen Liu,Dermot F. McGinnity,Mark McHale,Antonio Mete,James Reuberson,Bryan Roberts,John Steele,Barry Teobald,John Unitt,Deborah Vaughan,Iain Walters,Michael J. Stocks

Discovery of AZD-2098 and AZD-1678, Two Potent and Bioavailable CCR4 Receptor Antagonists

2017

Nicholas Kindon
Glen Andrews
Andrew Douglas Baxter
David Cheshire
Paul Hemsley
Timothy Johnson
Yu-Zhen Liu
Dermot F. McGinnity
Mark McHale
Antonio Mete
James Reuberson
Bryan Roberts
John Steele
Barry Teobald
John Unitt
Deborah Vaughan
Iain Walters
Michael J. Stocks

N-(5-Bromo-3-methoxypyrazin-2-yl)-5-chlorothiophene-2-sulfonamide 1 was identified as a hit in a CCR4 receptor antagonist high-throughput screen (HTS) of a subset of the AstraZeneca compound bank. As a hit with a lead-like profile, it was an excellent starting point for a CCR4 receptor antagonist program and enabled the rapid progression through the Lead Identification and Lead Optimization phases resulting in the discovery of two bioavailable CCR4 receptor antagonist candidate drugs.

Keywords:

Biology
Pharmacology
Antagonist
CCR4
CCR4 Receptor
Bioavailability

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