Richard Martyn Angell
GlaxoSmithKline
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Publication
Featured researches published by Richard Martyn Angell.
Bioorganic & Medicinal Chemistry Letters | 2008
Richard Martyn Angell; Tony D. Angell; Paul Bamborough; Mark J. Bamford; Chun-wa Chung; Stuart Cockerill; Stephen Flack; Katherine Louise Jones; Dramane I. Laine; Timothy Longstaff; Steve Ludbrook; Rosannah Pearson; Kathryn J. Smith; Penny A. Smee; Don O. Somers; Ann Louise Walker
The biphenyl amides (BPAs) are a series of p38alpha MAP kinase inhibitors. Compounds are able to bind to the kinase in either the DFG-in or DFG-out conformation, depending on substituents. X-ray, binding, kinetic and cellular data are shown, providing the most detailed comparison to date between potent compounds from the same chemical series that bind to different p38alpha conformations. DFG-out-binding compounds could be made more potent than DFG-in-binding compounds by increasing their size. Unexpectedly, compounds that bound to the DGF-out conformation showed diminished selectivity. The kinetics of binding to the isolated enzyme and the effects of compounds on cells were largely unaffected by the kinase conformation bound.
Bioorganic & Medicinal Chemistry Letters | 2008
Richard Martyn Angell; Nicola Mary Aston; Paul Bamborough; Jacky B. Buckton; Stuart Cockerill; Suzanne J. deBoeck; Chris D. Edwards; Duncan S. Holmes; Katherine Louise Jones; Dramane I. Laine; Shila Patel; Penny A. Smee; Kathryn J. Smith; Don O. Somers; Ann Louise Walker
The biphenyl amides (BPAs) are a novel series of p38alpha MAP kinase inhibitor. The optimisation of the series to give compounds that are potent in an in vivo disease model is discussed. SAR is presented and rationalised with reference to the crystallographic binding mode.
Journal of The Chemical Society-perkin Transactions 1 | 2002
Richard Martyn Angell; Keith Biggadike; Rosanne M. Farrell; Stephen Flack; Ashley Paul Hancock; Wendy R. Irving; Sean M. Lynn; Panayiotis A. Procopiou
A series of novel pregnane derivatives bearing γ-butyrolactones at C21 were prepared and tested as glucocorticoid agonists. The compounds were also tested for their lability in human plasma, and found to be rapidly hydrolysed by the enzyme paraoxonase to the respective hydroxyacids.
Journal of Medicinal Chemistry | 2000
Keith Biggadike; Richard Martyn Angell; Colin M. Burgess; Rosanne M. Farrell; Ashley Paul Hancock; Andy J. Harker; Wendy R. Irving; Chris Ioannou; Panayiotis A. Procopiou; Rupert E. Shaw; Yemisi E. Solanke; Onkar M. P. Singh; Michael A. Snowden; Rob J. Stubbs; Sarah Walton; Helen E. Weston
Archive | 2002
Richard Martyn Angell; Nicola Mary Aston; Paul Bamborough; Mark J. Bamford; George Stuart Cockerill; Suzanne Joy Merrick; Ann Louise Walker
Bioorganic & Medicinal Chemistry Letters | 2007
Paul Bamborough; Richard Martyn Angell; Inder Bhamra; David W. Brown; James A. Bull; John A. Christopher; Anthony William James Cooper; Lynsey H. Fazal; Ilaria Giordano; Lucy Hind; Vipulkumar Kantibhai Patel; Lisa E. Ranshaw; Martin J. Sims; Philip Alan Skone; Kathryn J. Smith; Emma Vickerstaff; Melanie Washington
Bioorganic & Medicinal Chemistry Letters | 2007
Richard Martyn Angell; Francis Louis Atkinson; Murray J.B. Brown; Tsu Tshen Chuang; John A. Christopher; Maria Cichy-Knight; Allison K. Dunn; Kendra E. Hightower; Susanna Malkakorpi; James R. Musgrave; Margarete Neu; Paul Rowland; Robyn L. Shea; Jeffery L. Smith; Donald O. Somers; Sonia Thomas; Gladstone Thompson; Ruolan Wang
Archive | 2002
Richard Martyn Angell; Nicola Mary Aston; Paul Bamborough; Mark J. Bamford; George Stuart Cockerill; Stephen Sean Flack; Dramane I. Laine; Ann Louise Walker
Archive | 2003
Richard Martyn Angell; Paul Bamborough; Ian Robert Baldwin; Anne-Marie Li-Kwai-Cheung; Timothy Longstaff; Suzanne Joy Merrick; Kathryn Jane Smith; Stephen Swanson; Ann Louise Walker
Archive | 2002
Richard Martyn Angell; Paul Bamborough; George Stuart Cockerill; Kathryn Jane Smith; Ann Louise Walker
