Identification and Optimization of Pyrrolo[3,2- d ]pyrimidine Toll-like Receptor 7 (TLR7) Selective Agonists for the Treatment of Hepatitis B

David C. Mcgowan,Florence Herschke,Frederik Pauwels,Bart Stoops,Ilham Smyej,Serge Maria Aloysius Pieters,Werner Constant Johan Embrechts,Mourad Daoubi Khamlichi,Tine Thoné,Bertrand Van Schoubroeck,Wendy Mostmans,Debbie Wuyts,Dorien Verstappen,Annick Scholliers,Dorien De Pooter,Deborah Dhuyvetter,Herman Borghys,Marianne Tuefferd,Eric Arnoult,Jin Hong,Gregory Fanning,Jacques Bollekens,Vijay Urmaliya,Ard Teisman,Helen Horton,Tim Hugo Maria Jonckers,Pierre Jean-Marie Bernard Raboisson

Identification and Optimization of Pyrrolo[3,2- d ]pyrimidine Toll-like Receptor 7 (TLR7) Selective Agonists for the Treatment of Hepatitis B

2017

Pyrrolo[3,2-d]pyrimidines were identified as a new series of potent and selective TLR7 agonists. Compounds were optimized for their activity and selectivity over TLR8. This presents an advantage over recently described scaffolds that have residual TLR8 activity, which may be detrimental to the tolerability of the candidate drug. Oral administration of the lead compound 54 effectively induced a transient interferon stimulated gene (ISG) response in mice and cynomolgus monkeys. We aimed for a high first pass effect, limiting cytokine induction systemically, and demonstrated the potential for the immunotherapy of viral hepatitis.

Keywords:

Hepatitis B
Lead compound
Biochemistry
Interferon-stimulated gene
Viral hepatitis
Toll-like receptor
TLR8
Immunology
Cytokine
Immunotherapy
Molecular biology
Biology
Chemistry
TLR7
Pharmacology

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