| Literature DB >> 25411473 |
Tom Y-H Wu1, Manmohan Singh2, Andrew T Miller1, Ennio De Gregorio3, Francesco Doro3, Ugo D'Oro3, David A G Skibinski3, M Lamine Mbow1, Simone Bufali3, Ann E Herman1, Alex Cortez1, Yongkai Li1, Bishnu P Nayak3, Elaine Tritto3, Christophe M Filippi1, Gillis R Otten2, Luis A Brito2, Elisabetta Monaci3, Chun Li1, Susanna Aprea3, Sara Valentini3, Samuele Calabrό3, Donatello Laera3, Brunella Brunelli3, Elena Caproni3, Padma Malyala2, Rekha G Panchal4, Travis K Warren4, Sina Bavari4, Derek T O'Hagan5, Michael P Cooke6, Nicholas M Valiante5.
Abstract
Adjuvants increase vaccine potency largely by activating innate immunity and promoting inflammation. Limiting the side effects of this inflammation is a major hurdle for adjuvant use in vaccines for humans. It has been difficult to improve on adjuvant safety because of a poor understanding of adjuvant mechanism and the empirical nature of adjuvant discovery and development historically. We describe new principles for the rational optimization of small-molecule immune potentiators (SMIPs) targeting Toll-like receptor 7 as adjuvants with a predicted increase in their therapeutic indices. Unlike traditional drugs, SMIP-based adjuvants need to have limited bioavailability and remain localized for optimal efficacy. These features also lead to temporally and spatially restricted inflammation that should decrease side effects. Through medicinal and formulation chemistry and extensive immunopharmacology, we show that in vivo potency can be increased with little to no systemic exposure, localized innate immune activation and short in vivo residence times of SMIP-based adjuvants. This work provides a systematic and generalizable approach to engineering small molecules for use as vaccine adjuvants.Entities:
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Year: 2014 PMID: 25411473 DOI: 10.1126/scitranslmed.3009980
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956