| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1391721 | Chemistry & Biology | 2014 | 11 Pages |
•Activated macrophages conditionally liberate a Cu-dependent fungicidal agent•Small molecule bypasses physiological copper import pathways in C. neoformans•Administration of masked agent reduces fungal burden in pulmonary infection•Antimicrobial agent targets Cu biology at the host-pathogen axis
SummaryRecalcitrant microbial infections demand new therapeutic options. Here we present an approach that exploits two prongs of the host immune cell antimicrobial response: the oxidative burst and the compartmentalization of copper (Cu) within phagolysosomes. The prochelator QBP is a nontoxic protected form of 8-hydroxyquinoline (8HQ) in which a pinanediol boronic ester blocks metal ion coordination by 8HQ. QBP is deprotected via reactive oxygen species produced by activated macrophages, creating 8HQ and eliciting Cu-dependent killing of the fungal pathogen Cryptococcus neoformans in vitro and in mouse pulmonary infection. 8HQ ionophoric activity increases intracellular Cu, overwhelming the Cu-resistance mechanisms of C. neoformans to elicit fungal killing. The Cu-dependent antimicrobial activity of 8HQ against a spectrum of microbial pathogens suggests that this strategy may have broad utility. The conditional activation of Cu ionophores by innate immune cells intensifies the hostile antimicrobial environment and represents a promising approach to combat infectious disease.
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