| Literature DB >> 26861551 |
Keith Biggadike1, Mahbub Ahmed1, Doug I Ball1, Diane M Coe1, Deidre A Dalmas Wilk2, Chris D Edwards1, Bob H Gibbon3, Charlotte J Hardy1, Stephen A Hermitage1, Joanne O Hessey1, Aimee E Hillegas2, Stephen C Hughes3, Linos Lazarides1, Xiao Q Lewell1, Amanda Lucas1, David N Mallett1, Mark A Price3, Fiona M Priest1, Diana J Quint1, Poonam Shah1, Anesh Sitaram3, Stephen A Smith1, Richard Stocker1, Naimisha A Trivedi1, Daphne C Tsitoura1, Victoria Weller1.
Abstract
Induction of IFNα in the upper airways via activation of TLR7 represents a novel immunomodulatory approach to the treatment of allergic asthma. Exploration of 8-oxoadenine derivatives bearing saturated oxygen or nitrogen heterocycles in the N-9 substituent has revealed a remarkable selective enhancement in IFNα inducing potency in the nitrogen series. Further potency enhancement was achieved with the novel (S)-pentyloxy substitution at C-2 leading to the selection of GSK2245035 (32) as an intranasal development candidate. In human cell cultures, compound 32 resulted in suppression of Th2 cytokine responses to allergens, while in vivo intranasal administration at very low doses led to local upregulation of TLR7-mediated cytokines (IP-10). Target engagement was confirmed in humans following single intranasal doses of 32 of ≥20 ng, and reproducible pharmacological response was demonstrated following repeat intranasal dosing at weekly intervals.Entities:
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Year: 2016 PMID: 26861551 DOI: 10.1021/acs.jmedchem.5b01647
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446