Mark Ian Lansdell
Pfizer
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Publication
Featured researches published by Mark Ian Lansdell.
Journal of Medicinal Chemistry | 2010
Mark Ian Lansdell; David Hepworth; Andrew Calabrese; Alan Daniel Brown; Julian Blagg; Denise J. Burring; Peter Wilson; David Sebastien Fradet; T. Bruce Brown; Faye Quinton; Neela Mistry; Kim Tang; Natalie M. Mount; Peter Stacey; Nick Edmunds; Cathryn Adams; Samantha Gaboardi; Stevie Neal-Morgan; Chris Wayman; Susan Cole; Joanne Phipps; Mark H. Lewis; Hugh Verrier; Val Gillon; Neil Feeder; Anne C. Heatherington; Stefan Sultana; Scott Haughie; Steven Martin; Maria Sudworth
The relevance of the melanocortin system to sexual activity is well established, and nonselective peptide agonists of the melanocortin receptors have shown evidence of efficacy in human sexual dysfunction. The role of the MC4 receptor subtype has received particular scrutiny, but the sufficiency of its selective activation in potentiating sexual response has remained uncertain owing to conflicting data from studies in preclinical species. We describe here the discovery of a novel series of small-molecule MC4 receptor agonists derived from library hit 2. The addition of methyl substituents at C3 and C5 of the 4-phenylpiperidin-4-ol ring was found to be markedly potency-enhancing, enabling the combination of low nanomolar potencies with full rule-of-five compliance. In general, the series shows only micromolar activity at other melanocortin receptors. Our preferred compound 40a provided significant systemic exposure in humans on both sublingual and oral administration and was safe and well tolerated up to the maximum tested dose. In a pilot clinical study of male erectile dysfunction, the highest dose of 40a tested (200 mg) provided a similar level of efficacy to sildenafil.
Chemical Communications | 2010
Donald Craig; Sophie J. Gore; Mark Ian Lansdell; Simon E. Lewis; Alexander V. Mayweg; Andrew J. P. White
Unsaturated epsilon-lactones bearing an alpha-arylsulfonyl or alpha-arylsulfoximinyl substituent undergo stereoselective transannular, decarboxylative Claisen rearrangement to give substituted vinylcyclopropanes.
Bioorganic & Medicinal Chemistry Letters | 2008
Mark Ian Lansdell; Denise J. Burring; David Hepworth; Matthew Strawbridge; Emily J. S. Graham; Thierry Guyot; Mark S. Betson; James Hart
The design and synthesis of the first fluorophore-conjugated SGLT2 inhibitors is described. The mode of linking the fluorophore to the SGLT2 pharmacophore was found to be crucial in achieving optimum potency. Superior potency to phlorizin was provided by examples containing TAMRA, BODIPY, Cy3B and NBD fluorophores.
Bioorganic & Medicinal Chemistry Letters | 2009
Mark David Andrews; Alan Daniel Brown; Jean-Yves Chiva; David Sebastien Fradet; David W. Gordon; Mark Ian Lansdell; Malcolm MacKenny
A second wave of potential SSRIs with high ease of synthetic accessibility were designed based on the reported selective serotonin re-uptake inhibitor litoxetine and our own previous work in this area. Preparation and subsequent optimisation yielded a range of potent and highly selective SSRIs.
Archive | 2004
Mark David Andrews; Alan Daniel Brown; David Sebastien Fradet; David W. Gordon; Mark Ian Lansdell; Malcolm MacKenny
Archive | 2006
Mark David Andrews; Alan Daniel Brown; David Sebastien Fradet; Mark Ian Lansdell
Tetrahedron Letters | 2007
Donald Craig; Mark Ian Lansdell; Simon E. Lewis
Archive | 2007
Mark David Andrews; Alan Daniel Brown; Mark Ian Lansdell; Nicholas William Summerhill
Archive | 2005
Mark David Andrews; Alan Daniel Brown; Paul Vincent Fish; Michael Jonathan Fray; Mark Ian Lansdell; Thomas Ryckmans; Alan Stobie; Florian Vakenhut; David L. Gray
Archive | 2007
Duncan Robert Armour; Sebastien Rene Gabriel Galan; Charlotte Alice Louise Lane; Mark Ian Lansdell; James E. J. Mills; Nunzio Sciammetta; Paul Anthony Stupple
