Publications by authors named "Simon Barber"
A lead generation and optimization program delivered the highly selective and potent CatC inhibitor 10 as an in vivo tool compound and potential development candidate. Structural studies were undertaken to generate SAR understanding.
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- - Two new series of formyl peptide receptor 1 (FPR1) antagonists have been identified, specifically methionine benzimidazole 6 and diamide 7
- - Both antagonists are effective at preventing the binding of a labeled peptide (fMLF) to hrFPR1, which indicates their potential in research applications
- - They selectively inhibit FPR1 function in human neutrophils, suggesting they could be valuable tools in laboratory experiments to validate FPR1 as a target
A novel series of small molecule C5a antagonists is reported. In particular, in vitro metabolic studies and solution based combinatorial synthesis are demonstrated as useful tools for the rapid identification of antagonists with low in vitro clearance. Members of this series specifically inhibited the binding of (125)I-labeled C5a to human recombinant C5a receptor (C5aR).
View Article and Find Full Text PDFThe design and synthesis of a new series of c-Jun N-terminal kinase inhibitors are reported. The novel series of substituted amino indazoles were designed based on a combination of hits from high-throughput screening and X-ray crystal structure information of the compounds crystallised into the JNK-1 ATP binding site.
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